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  • Nerve Injury Wikipedia
    Electrical stimulation with a motor response at < 0.2 mA only can occur with an intraneural/intrafasciular needle tip location. [28] See also [ edit ] Brain injury References [ edit ] ^ Seddon HJ (August 1942).
  • Melanocytic Nevus Wikipedia
    The letters stand for asymmetry, border, color, and diameter. [4] [28] Sometimes, the letter E (for elevation or evolving) is added.
    NRAS, BRAF, NF1, SUZ12, HRAS, PTEN, RAF1, FGFR3, RIT1, ERCC2, KRAS, TYR, AKT1, PTCH1, DDB2, RASA2, PIK3CA, PTPN11, RRAS, PRKAR1A, PDE4D, TNFRSF11B, SDHC, MPL, MC1R, ERCC3, ERCC4, ERCC5, ERF, IGF2, HPS1, SDHB, SOS2, SDHD, SOS1, KLLN, A2ML1, FKBP10, RBM28, SUFU, SMARCAL1, KAT6B, MRAS, SEC23B, SYNGAP1, TNFRSF11A, EED, PTCH2, TP63, CDH3, LZTR1, XPC, XPA, CDKN2A, LYST, CHRNA7, TP53, COL3A1, FGFR2, H3P10, BAP1, BCL2, CCND1, RREB1, KIT, IRF4, MITF, TERT, MYC, SLC2A1, GNAQ, KDM5B, NGFR, TRPM1, MYB, MTAP, PAX3, MKI67, KITLG, MCAM, MAP2, NID1, EIF4E, PRAME, PCNA, EDN1, PPARG, PRKCB, CTNND1, CTNNB1, BCAR1, CSE1L, SOCS1, TP73, CDKN2B, VDR, CDKN1A, MIB1, PLA2G6, ARHGAP24, MLANA, MIR21, NLRP7, HSDL1, TMX2-CTNND1, KHDC3L, UBE2C, METAP2, CLOCK, ZHX2, PHLDA1, MIR34A, GAB2, RBX1, KIF20A, TSPO, MRPL28, KHDRBS1, NES, MIR210, MIR373, MIR211, PPP1R13L, RASSF1, SUB1, SHCBP1, ABCG2, MIR510, MS4A1, RECK, NOP14, CDH1, CD44, H3P9, LOC110806263, MTCO2P12, CD34, NRP2, UCA1, CASP6, AD12, SQSTM1, MCM3AP, HSPB3, CD163, ADRB2, MAGED4, CARD8, SYNE1, PLXND1, ALCAM, DCTN4, SIRT6, IL23A, STS, KRT20, CKS1BP7, SLAMF9, ESPN, XAF1, AMN, AQP3, PAG1, SLC12A9, CTNNBIP1, PCBP4, SLURP1, MAGED4B, CLPTM1L, AQP1, LINC00328, NSDHL, MIR200C, LINC00032, BIRC7, DICER1, MIR155, BAD, MIR143, MIRLET7C, HAGLR, AMACR, RTL1, NUP62, CADM1, POT1, LRIT1, NXT1, PYCARD, ERVW-1, DPH3, ATP2A2, SASS6, FGF2, STK11, CDK4, ITGAX, IFNA2, IFNA13, IFNA17, ESR2, IGFBP7, IL1B, CXCL8, IL10, IL18, IRF6, KISS1, IFN1@, ERBB2, LGALS3, LGALS9, LRP2, MAGEA1, MAOA, EPHB2, MMP1, MMP9, ELAVL2, IFNA1, ICAM1, MIA, HCCS, G6PD, GABPA, GALK1, GH1, GJB2, GPC3, GLB1, GSN, GTF2H1, GZMB, HCL2, HSP90AA1, HDAC1, HIF1A, HLA-E, HLA-G, HOXA1, EZH2, ETS1, HSPA8, HSPB1, HSPB2, CITED1, MSH2, MT1A, CREBBP, DDIT3, RAG2, GADD45A, OPN1LW, RHCE, CYP24A1, CTSD, S100A6, VCAN, SHOX, SOX10, COX2, SPARC, PTK2B, TFAP2A, TGFBR2, TLR4, TSPAN8, CKS1B, CDK6, XRCC3, COIL, RAC1, PVT1, NQO1, PTGS2, NFE2L2, NME1, NOS2, EIF2S1, NRF1, OCA2, EGFR, PAM, PAX4, PAX9, DUSP3, PKD1, PKM, PLP2, PARP1, MAPK1, MAP2K7, HTRA1, PTAFR, DNM1, DMBT1, PLIN2
  • Complex Post-Traumatic Stress Disorder Wikipedia
    C-PTSD better describes the pervasive negative impact of chronic repetitive trauma than does PTSD alone. [20] PTSD can exist alongside C-PTSD, however a sole diagnosis of PTSD often does not sufficiently encapsulate the breadth of symptoms experienced by those who have experienced prolonged traumatic experience, and therefore C-PTSD extends beyond the PTSD parameters. [10] C-PTSD also differs from continuous traumatic stress disorder (CTSD), which was introduced into the trauma literature by Gill Straker (1987). [28] It was originally used by South African clinicians to describe the effects of exposure to frequent, high levels of violence usually associated with civil conflict and political repression . ... ISBN 978-1-56032-525-3 . Retrieved 28 October 2012 . ^ Rando TA (February 1993). ... ISBN 978-0-87822-329-9 . Retrieved 28 October 2012 . ^ Rando TA (1 January 1994). ... ISBN 978-0-86720-631-9 . Retrieved 28 October 2012 . ^ Green BL (2000).
  • Hemolytic Anemia Wikipedia
    Hemolytic anemia Other names Haemolytic anaemia Specialty Hematology Hemolytic anemia is a form of anemia due to hemolysis , the abnormal breakdown of red blood cells (RBCs), either in the blood vessels (intravascular hemolysis) or elsewhere in the human body (extravascular). [1] This most commonly occurs within the spleen, but also can occur in the reticuloendothelial system or mechanically (prosthetic valve damage). [1] Hemolytic anemia accounts for 5% of all existing anemias. [1] It has numerous possible consequences, ranging from general symptoms to life-threatening systemic effects. [1] The general classification of hemolytic anemia is either intrinsic or extrinsic. [2] Treatment depends on the type and cause of the hemolytic anemia. [1] Symptoms of hemolytic anemia are similar to other forms of anemia ( fatigue and shortness of breath ), but in addition, the breakdown of red cells leads to jaundice and increases the risk of particular long-term complications, such as gallstones [3] and pulmonary hypertension . [4] Contents 1 Signs and symptoms 2 Causes 2.1 Intrinsic causes 2.2 Extrinsic causes 3 Mechanism 3.1 Intravascular hemolysis 3.2 Extravascular hemolysis 4 Diagnosis 5 Treatment 6 Other animals 7 References 8 External links Signs and symptoms [ edit ] Symptoms of hemolytic anemia are similar to the general signs of anemia. [1] General signs and symptoms include: fatigue, pallor, shortness of breath, and tachycardia. [1] In small children, failure to thrive may occur in any form of anemia. [5] [6] In addition, symptoms related to hemolysis may be present such as chills, jaundice, dark urine, and an enlarged spleen. [1] Certain aspects of the medical history can suggest a cause for hemolysis, such as drugs , medication side effects, autoimmune disorders, blood transfusion reactions, the presence of prosthetic heart valve , or other medical illness. [1] Chronic hemolysis leads to an increased excretion of bilirubin into the biliary tract , which in turn may lead to gallstones. [7] The continuous release of free hemoglobin has been linked with the development of pulmonary hypertension (increased pressure over the pulmonary artery ); this, in turn, leads to episodes of syncope (fainting), chest pain , and progressive breathlessness. [8] Pulmonary hypertension eventually causes right ventricular heart failure, the symptoms of which are peripheral edema (fluid accumulation in the skin of the legs) and ascites (fluid accumulation in the abdominal cavity). [8] Causes [ edit ] Main articles: Congenital hemolytic anemia and Acquired hemolytic anemia They may be classified according to the means of hemolysis, being either intrinsic in cases where the cause is related to the red blood cell (RBC) itself, or extrinsic in cases where factors external to the RBC dominate. [9] Intrinsic effects may include problems with RBC proteins or oxidative stress handling, whereas external factors include immune attack and microvascular angiopathies (RBCs are mechanically damaged in circulation). [1] [2] Intrinsic causes [ edit ] Hereditary (inherited) hemolytic anemia can be due to : Defects of red blood cell membrane production (as in hereditary spherocytosis and hereditary elliptocytosis ). [1] Defects in hemoglobin production (as in thalassemia , sickle-cell disease and congenital dyserythropoietic anemia ). [1] Defective red cell metabolism (as in glucose-6-phosphate dehydrogenase deficiency and pyruvate kinase deficiency ). [10] [11] Paroxysmal nocturnal hemoglobinuria (PNH), sometimes referred to as Marchiafava-Micheli syndrome, is a rare, acquired, potentially life-threatening disease of the blood characterized by complement-induced intravascular hemolytic anemia. [12] Extrinsic causes [ edit ] Acquired hemolytic anemia may be caused by immune-mediated causes, drugs, and other miscellaneous causes. [1] Immune-mediated causes could include transient factors as in Mycoplasma pneumoniae infection ( cold agglutinin disease ) [13] or permanent factors as in autoimmune diseases like autoimmune hemolytic anemia [14] (itself more common in diseases such as systemic lupus erythematosus , rheumatoid arthritis , Hodgkin's lymphoma , and chronic lymphocytic leukemia ). [1] Spur cell hemolytic anemia [15] Any of the causes of hypersplenism (increased activity of the spleen), such as portal hypertension . [16] Acquired hemolytic anemia is also encountered in burns and as a result of certain infections (e.g. malaria ). [14] [17] Lead poisoning resulting from the environment causes non-immune hemolytic anemia. [18] Similarly, poisoning by arsine or stibine also causes hemolytic anemia. [19] Runners can suffer hemolytic anemia due to " footstrike hemolysis ", owing to the destruction of red blood cells in feet at foot impact. [20] [21] Low-grade hemolytic anemia occurs in 70% of prosthetic heart valve recipients, and severe hemolytic anemia occurs in 3%. [22] Mechanism [ edit ] In hemolytic anemia, there are two principal mechanisms of hemolysis; intravascular and extravascular. [23] Intravascular hemolysis [ edit ] Intravascular hemolysis describes hemolysis that happens mainly inside the vasculature . [24] As a result, the contents of the red blood cell are released into the general circulation, leading to hemoglobinemia [25] and increasing the risk of ensuing hyperbilirubinemia . [26] Intravascular hemolysis may occur when red blood cells are targeted by autoantibodies , leading to complement fixation, or by damage by parasites such as Babesia . [27] Extravascular hemolysis [ edit ] Extravascular hemolysis refers to hemolysis taking place in the liver , spleen , bone marrow , and lymph nodes . [24] In this case little hemoglobin escapes into blood plasma . [26] The macrophages of the reticuloendothelial system in these organs engulf and destroy structurally-defective red blood cells, or those with antibodies attached, and release unconjugated bilirubin into the blood plasma circulation. [28] [29] Typically, the spleen destroys mildly abnormal red blood cells or those coated with IgG-type antibodies , [30] [31] while severely abnormal red blood cells or those coated with IgM-type antibodies are destroyed in the circulation or in the liver. [30] If extravascular hemolysis is extensive, hemosiderin can be deposited in the spleen, bone marrow, kidney, liver, and other organs, resulting in hemosiderosis . [26] In a healthy person, a red blood cell survives 90 to 120 days in the circulation, so about 1% of human red blood cells break down each day. [32] [ unreliable medical source?
    G6PD, TPI1, SLC4A1, GCLC, COL4A1, HMOX1, ITPA, SPTB, GPI, EPO, IFNA2, GSR, EIF2AK1, ALAS2, A2M, UROS, ADAMTS13, NT5C3A, SPTA1, HBA2, HBA1, PGK1, CD59, ANK1, GSS, KRAS, CD40LG, RHAG, SLC2A1, HBB, PTPN22, TNFRSF13B, ATP7B, KCNN4, ATP11C, TNFRSF13C, LCAT, NFKB1, NFKB2, BTNL2, NRAS, PFKM, PGM3, PIGA, PRKCD, PIGT, ICOS, ALAD, HLA-DRB1, AK1, KDM6A, WAS, WIPF1, KMT2D, LAT, TNFSF12, TREX1, UROD, CD81, GP1BA, FCGR2B, CTLA4, FECH, GALT, DNASE1, CR2, GATA1, EPB42, CD19, MS4A1, EPB41, FCGR2A, CFH, PKLR, KLF1, HFE, UGT1A1, ADA, PRDX2, CP, HAMP, RN7SL263P, UBL4A, DHS, PIEZO1, H6PD, GCLM, ABCG8, HEPH, MIR451A, MIR144, GSTK1, BTG3, ADD2, IFNL3, IL27, SLEH1, SMUG1, C20orf194, SIRPA, MYDGF, ATN1, SLCO6A1, CRYZ, IL37, HPGDS, DECR1, KRT88P, FOXP3, ACR, RAB14, CD55, MED25, IL17D, ECB2, FUBP1, MTHFR, PTGS2, PSEN1, FOLR1, FOLR2, CD47, ABO, PRDX1, COX2, RPS19, CD247, C3, TNFRSF17, HP, BRCA2, HBG2, HK1, FLNA, S100A8, DMTN, UGT1A, SMARCA5, CDR3, F2, F3, FANCD2, VWF, FBP1, UGCG, SLC6A3, SLC35A2, TRV-AAC1-4, FCGR3A, TFRC, TRIM21, ALDH9A1, ALDOA, MTCO2P12
  • Executive Dysfunction Wikipedia
    The dopamine receptor D4 gene ( DRD4 ) with 7'-repeating polymorphism (7R) has been repeatedly shown to correlate strongly with impulsive response style on psychological tests of executive dysfunction, particularly in clinical ADHD. [27] The catechol-o-methyl transferase gene ( COMT ) codes for an enzyme that degrades catecholamine neurotransmitters (DA and NE), and its Val158Met polymorphism is linked with the modulation of task-oriented cognition and behavior (including set shifting [28] ) and the experience of reward, which are major aspects of executive functioning.
    FMR1, BDNF, COMT, APOE, SLC6A3, SNCA, SRPX, XPR1, TPSG1, CHD7, SPG11, CHD8, ZBP1, EBPL, SFXN1, STH, ANKK1, SLC6A4, PSEN2, SGCA, ARSD, PNN, NGF, CXCL8, ICAM1, ELK3, TOR1A, DRD4, DRD2, CSF1R, CHD2, CACNA1C, MCIDAS
  • Eosinophilic Myocarditis Wikipedia
    "Viral myocarditis" . Current Opinion in Rheumatology . 28 (4): 383–9. doi : 10.1097/BOR.0000000000000303 .
    CCR3, IL5, CCL11
  • Rumination Syndrome Wikipedia
    Involuntary rumination, similar to what is seen in humans, has been described in gorillas and other primates . [27] Macropods such as kangaroos also regurgitate, re-masticate, and re-swallow food, but these behaviors are not essential to their normal digestive process, are not observed as predictably as the ruminants', and hence were termed "merycism" in contrast with "true rumination". [28] See also [ edit ] Professional regurgitator References [ edit ] ^ Rumination Syndrome — Diagnosis and Treatment Options at Mayo Clinic ^ a b c d e f g h i j k l m n o p q r s t u Papadopoulos, Vassilios; Mimidis, Konstantinos (July–September 2007), "The rumination syndrome in adults: A review of the pathophysiology, diagnosis and treatment", Journal of Postgraduate Medicine , 53 (3): 203–206, doi : 10.4103/0022-3859.33868 , PMID 17699999 ^ a b c d e f g h i j k Chial, Heather J; Camilleri, Michael; Williams, Donald E; Litzinger, Kristi; Perrault, Jean (2003), "Rumination syndrome in children and adolescents: diagnosis, treatment, and prognosis" , Pediatrics , 111 (1): 158–162, doi : 10.1542/peds.111.1.158 , PMID 12509570 ^ a b c d e Camilleri, Michael; Seime, Richard J, Rumination Syndrome, symptoms , Rochester, Minnesota: Mayo Clinic , retrieved 2009-06-26 ^ Amarnath RP, Abell TL, Malagelada JR (October 1986), "The rumination syndrome in adults.
    BDNF, SLC6A4, CREB1, FLT4, PKD2L1, MIR620, MIR383, CACNA1G-AS1, KCTD12, ABHD14B, TAT, PPP1R3B, SETD5, REM1, MTHFD1L, CIB1, BCAR1, EBPL, PPP1R3C, COMT, MTHFR, LPP, LEP, KCNJ6, IL6, IL1B, IDS, FUT3, FKBP5, ELK3, DRD2, CRYGD, MIR1270
    • Rumination Disorder Gard
      Rumination disorder is the backward flow of recently eaten food from the stomach to the mouth. The food is then re-chewed and swallowed or spat out. A non-purposeful contraction of stomach muscles is involved in rumination. It may be initially triggered by a viral illness, emotional distress, or physical injury. In many cases, no underlying trigger is identified. Behavioral therapy is the mainstay of treatment. .
    • Rumination Syndrome Mayo_clinic
      Overview Rumination syndrome is a condition in which people repeatedly and unintentionally spit up (regurgitate) undigested or partially digested food from the stomach, rechew it, and then either reswallow it or spit it out. Because the food hasn't yet been digested, it reportedly tastes normal and isn't acidic, as vomit is. Rumination typically happens at every meal, soon after eating. It's not clear how many people have this disorder. Treatment may include behavioral therapy or medications. Behavioral therapy that involves teaching people to breathe from the diaphragm is the usual treatment of choice. Symptoms Effortless regurgitation, typically within 10 minutes of eating Abdominal pain or pressure relieved by regurgitation A feeling of fullness Bad breath Nausea Unintentional weight loss Rumination syndrome isn't usually associated with retching.
  • Psychological Trauma Wikipedia
    In children it is manifested as disorganized or agitative behaviors. [28] Trauma can be caused by a wide variety of events, but there are a few common aspects. ... Archived from the original on 2005-10-28. ^ a b c Frommberger, Ulrich (2014). ... Helping Abused and Traumatized Children: Integrating Directive and Nondirective Approaches . Guilford Press. pp. 28, 59. ISBN 978-1-60918-474-2 . ^ McNally, R.J. (2003) Remembering Trauma. ... International Journal of Risk & Safety in Medicine . 22 (4): 195–207. doi : 10.3233/JRS-2010-0508 . Archived from the original on 28 January 2013 . Retrieved 5 December 2012 . ^ Ramos, S.M., & Boyle, G.J. (2001).
    ADCYAP1R1, APOE, ERCC8, COMT, CSH1, CSH2, HSPA9, GAL
  • Central Serous Retinopathy Wikipedia
    In a retrospective study noted by Acta Ophthalmologica, spironolactone improved visual acuity in CSR patients over the course of 8 weeks. [28] Epleronone is another mineralocorticoid receptor antagonist that has been thought to reduce the subretinal fluid that is present with CSR.
    NR3C2, CD44, PROM1, PLXNA2, ALDH1A1, CTNNB1, SOX2, CD24, FOXM1, EGFR, ERBB2, POU5F1, POU5F1P3, POU5F1P4, BECN1, VEGFA, NOTCH1, TNF, CFH, DNMT1, STAT3, HES1, SLC22A3, DYNC2H1, HDAC2, MAPK1, IL6, YAP1, PLG, NFATC3, OSM, SERPINE1, PIK3CA, PIK3CB, PIK3CD, PIK3CG, AKT1, ALCAM, TP53, ZEB1, JAG1, LGR5, MIR145, MIR146A, MIR200C, NRP1, NMU, KAT7, STRAP, H4C8, H4C9, H4C3, RAD51AP1, H4C11, H4C12, H4C6, H4C4, H4C1, NES, H4C2, AHSA1, ATG7, TRAP1, ABCB6, TBPL1, ABCG2, GRAP2, KLF4, DCLK1, H4C5, OSMR, H4C13, H4C14, CLDN2, MBD2, ADM, KLF12, MIR155, CD109, RMDN2, SHISA3, DNAJB8, DNAJB1P1, ARMS2, MIR10B, MIR137, MIR150, MIR200B, CBX5, MIR203A, MIR21, MIR219A1, MIR23B, MIR31, MIR95, H4C15, MIR874, GATD3B, H4-16, ORAI1, FSD1L, AGBL2, CBX7, RNF19A, POLDIP2, SLC7A5, FBXO8, RMDN1, HDAC7, PINX1, RMDN3, FBXW7, SYBU, PAG1, KIF15, ACKR3, PCBP4, SPC25, WDR48, FBRS, FSD1, GATD3A, PRDX2, ADAM12, AIMP2, EIF4E, EZH2, F3, PTK2B, FGF5, FN1, GLI1, GSK3B, GSTM1, HDAC1, HMGB1, HOXB3, HSF1, HSPA4, DNAJB1, IFNB1, CXCL8, ITK, KIT, EGR3, DUSP5, DNMT3A, CAV1, AKT2, APC, AR, BAX, BMI1, BMP2, BMP7, BNIP3L, RUNX3, DDX3X, CDH5, CDK2, CREBBP, CRK, CRP, MAPK14, CSF2, DAB2, LAMC2, LGALS1, LOX, TGFB1, SMN2, SOX9, SOX15, SRF, AURKA, ADAM17, TEAD1, TERF2, TGM2, SLC16A1, TLR3, TRAF6, TWIST1, EZR, VIM, WIPF1, PCGF2, CXCR4, SMN1, SLC12A3, EPCAM, MAPK9, SMAD2, MMP11, COX2, NELL1, PECAM1, PLAT, MAPK3, MAPK8, MAP2K7, SLC3A2, PTEN, PTGS2, PTPRB, RAC1, OPN1LW, REN, SDC1, CXCL12, MTCO2P12
    • Central Serous Chorioretinopathy Orphanet
      A rare, acquired, choroidal disorder characterized by subretinal detachment in the macular área and leakage of fluid under the retina that accumulates under the central macula. Symptoms tend to include blurred or distorted vision (metamorphopsia), moderate dyschromatopsia, relative central scotoma, hypermetropization, micropsia and reduced contrast sensitivity. A blurred or gray spot in the central visual field is common when the retina is detached.
    • Central Serous Chorioretinopathy Gard
      Central serous chorioretinopathy (CSCR) occurs when fluid builds up under the retina , the back part of the inner eye that sends sight information to the brain. The fluid leaks from the choroid (the blood vessel layer under the retina), and can lead to retinal detachment. Signs and symptoms include dim and blurred vision, a blind spot in the center of vision, distortion of straight lines, and seeing objects as smaller or farther away. The cause of this condition is unknown, but it is thought to be due to a combination of genetic and environmental factors. Risk factors include steroid use, stress, certain infections, and sleep disorders.
  • Septic Shock Wikipedia
    Methylene blue has been found to work in cases resistant to the usual agents. [24] This effect was first reported in the early 1990s. [25] [26] Other [ edit ] While there is tentative evidence for β-Blocker therapy to help control heart rate , evidence is not significant enough for its routine use. [27] [28] There is tentative evidence that steroids may be useful in improving outcomes. [29] Tentative evidence exists that Polymyxin B-immobilized fiber column hemoperfusion may be beneficial in treatment of septic shock. [30] Trials are ongoing and it is currently being used in Japan and Western Europe. [31] Recombinant activated protein C ( drotrecogin alpha ) in a 2011 Cochrane review was found not to decrease mortality and to increase bleeding, and thus, was not recommended for use. [32] Drotrecogin alfa (Xigris), was withdrawn from the market in October 2011.
    TNF, NOS2, HLA-DRA, AQP1, C5AR1, GC, FER, IL10, ADM, CASP1, VWF, VEGFA, ADAMTS13, TNFRSF1A, NLRP1, DDAH2, PYCARD, TLR4, SLC5A1, SAA2, SAA1, TNFRSF1B, HSPD1, IL6, IL1B, ANGPT1, HMGB1, NR3C1, FCGR3B, F3, EDN1, CSF3, CRP, CPB2, CD6, ANGPT2, NLRP12
  • Ollier Disease Wikipedia
    Elastic stable intramedullary nailing system (ESIN) and flexible intramedullary nailing (FIN) are more recent surgical procedures that also utilize external fixation that has been shown to reduce the Healing Index and minimize complications. [28] [29] Similarly to the Ilizarov technique, the procedure is intended to correct deformities and elongate limb bones.
    IDH1, IDH2, PTPN11, OPN1SW, EP300, NPM1, TP53, CHEK2
    • Multiple Enchondromatosis, Maffucci Type Omim
      Description Enchondromas are common benign cartilage tumors of bone. They can occur as solitary lesions or as multiple lesions in enchondromatosis. When hemangiomata are associated, the condition is known as Maffucci syndrome. Clinical problems caused by enchondromas include skeletal deformity and the potential for malignant change to osteosarcoma (Schwartz et al., 1987). Classification of the Enchondromatoses In their classification of the enchondromatoses, Spranger et al. (1978) called Ollier disease (166000) and Maffucci syndrome types I and II enchondromatosis, respectively; metachondromatosis (156250), type III; and spondyloenchondrodysplasia (607944), type IV; enchondromatosis with irregular vertebral lesions, type V; and generalized enchondromatosis, type VI.
    • Maffucci Syndrome Wikipedia
      Maffucci syndrome Enchondromas are present in Maffucci syndrome Specialty Medical genetics Maffucci syndrome is a very rare disorder in which multiple benign tumors of cartilage develop within the bones (such tumors are known as enchondromas ). [1] The tumors most commonly appear in the bones of the hands, feet, and limbs, causing bone deformities and short limbs. [1] It is named for the Italian pathologist Angelo Maffucci who described it in 1881. [2] Fewer than 200 cases of this syndrome have been reported. [1] Contents 1 Signs and symptoms 2 Cause 3 Diagnosis 3.1 Differential diagnosis 4 Management 5 See also 6 References 7 External links Signs and symptoms [ edit ] Patients are normal at birth and the syndrome manifests during childhood and puberty. The enchondromas affect the extremities and their distribution is asymmetrical. The most common sites of enchondromas are the metacarpal bones and phalanges of the hands. The feet are less commonly afflicted. Disfigurations of the extremities are a result. Pathological fractures can arise in affected metaphyses and diaphyses of the long bones and are common (26%).
    • Maffucci Syndrome Gard
      Maffucci syndrome is a disorder that primarily affects the bones and skin. It is characterized by multiple enchondromas (benign enlargements of cartilage), bone deformities, and hemangiomas (tangles of abnormal of blood vessels). The abnormal growths associated with Maffucci syndrome may become cancerous (malignant). In particular, affected individuals may develop bone cancers called chondrosarcomas , especially in the skull. They also have an increased risk of other cancers, such as ovarian or liver cancer.
    • Maffucci Syndrome Orphanet
      Maffucci syndrome is a very rare genetic bone and skin disorder characterized by multiple enchondromas, leading to bone deformities, combined with multiple dark, irregularly shaped hemangiomas or less commonly lymphangiomas.
    • Maffucci Syndrome Medlineplus
      Maffucci syndrome is a disorder that primarily affects the bones and skin. It is characterized by multiple enchondromas, which are noncancerous (benign) growths of cartilage that develop within the bones. These growths most commonly occur in the limb bones, especially in the bones of the hands and feet; however, they may also occur in the skull, ribs, and bones of the spine (vertebrae). Enchondromas may result in severe bone deformities, shortening of the limbs, and fractures. The signs and symptoms of Maffucci syndrome may be detectable at birth, although they generally do not become apparent until around the age of 5.
  • Leukemia, Acute Lymphoblastic Omim
    By genotyping 1,384 cases of precursor B-cell childhood ALL and 1,877 controls from Germany and the United Kingdom, Prasad et al. (2010) found a significant association between ALL and the ARID5B SNP rs7089424 (OR of 1.80; p = 5.90 x 10(-28)). This finding replicated the independent susceptibility locus for ALL at chromosome 10q21.2 previously reported by Trevino et al. (2009) and Papaemmanuil et al. (2009).
    NOTCH1, IKZF1, CDKN2A, SH2B3, FBXW7, BLM, LIG4, KMT2A, PTEN, LMO2, EZH2, NOTCH3, FLT3, ETV6, NBN, NUDT15, CD6, TRBV20OR9-2, CD19, MS4A1, TCF3, CD33, TAL1, CD22, H3P10, SPG7, GNB1, KRT20, NR3C1, CRLF2, CSF2, RUNX1, PTPN11, GSTP1, GSTT1, CASR, PSMB6, PRKAR1A, ASRGL1, CD34, TNF, TRG, CD38, CSF3, MRPL28, CXADR, TBC1D9, CYP1A1, TRIM13, DHFR, NQO1, NR1I3, ATN1, ABCG2, HPGDS, CEBPE, DLL1, KIT, CNTNAP1, CDR3, CDKN2B, NXT1, CXCR4, YY1, ERG, EVPL, TYMS, TPMT, TP53, PIK3CG, FANCB, TRGC1, PMS2, GSTM1, PIK3CD, IL7, OPN1SW, BCL2, GSTK1, ASPG, MTTP, MTHFR, IGH, MPO, ARR3, MME, AFF1, MYC, ANPEP, MDM2, TARP, CXADRP1, ITPA, JAK1, ALL1, JAK2, ABL1, H3P9, BCR, ABCC1, SUB1, NRAS, HTC2, ABCB1, PIK3CA, PIK3CB, TMEM132D, ARID5B, PBX1, SLCO6A1, PAX5, HLF, IL3, FAS, IL2, GGH, AKT1, IL7R, WT1, CD44, NT5C2, CCND1, IFNG, RFC1, IL6, VEGFA, ASNS, ARHGAP24, CDK2, SLC19A1, IL3RA, CREBBP, CYP3A5, CCN2, IL10, CYP3A4, WLS, IL18R1, EBI3, IFNA1, CDKN1C, TP73, IFNA13, ZNF384, BCL6, FHIT, SAI1, S100A4, ATM, MSH3, MLLT10, HLA-DRB1, AICDA, MEF2D, RAG1, STAT5A, HRX, CTNNB1, STAT5B, MTX1, JAK3, GATA3, MTRR, ATG5, GEM, MLLT1, NRP1, IL15, PICALM, TLX1, HOXA9, EBF1, MCL1, KIR3DL1, ROPN1L, RBM45, ASPM, C3, CES1, ASPA, ASIP, MARCKSL1, CRYZ, DUX4, A1CF, MIR196B, LINC02605, MTOR, BTG1, HERPUD1, CALCA, HLA-A, BLNK, CD86, NUP214, CASP3, CDK4, RUNX1T1, SCT, SNAP25, EP300, ROR1, LEF1, MIR155, IGF2BP1, BCL2L11, MERTK, CYP2D6, IL2RA, MSH2, MTAP, MDM4, CCR7, MTR, KRAS, FOXO3, MLLT3, TGFB1, TG, SOAT1, TNFRSF9, CD40, FGFR1, FUT4, ADA, SPP1, TRD, CEP72, CD27, LRP1, FPGS, IDH1, CXCL12, BCRP2, NCAM1, HPRT1, IDH2, PDGFRB, P2RY8, HOXA@, BAX, TLX3, CALM1, GLS, CALM2, CALM3, PML, HLA-B, COL18A1, MIR146A, PTPRC, RB1, CSF1R, NAT2, ABCC3, CD52, CDKN1A, EPOR, CDKN1B, MVP, SNAP91, CYP2E1, FOXP1, PROM1, CDK6, EIF4E, HFE, PRKAA2, TRDJ1, NME1, MSI2, NPM1, PTPN6, TNFRSF13C, DERL1, SERPINE1, TSLP, CASP8, HDAC9, MAPK3, HDAC1, F2, ADIPOQ, HSP90AA1, PIP4K2A, HLA-DPB1, PRKAB1, PRKAA1, TCF7L1, BMI1, RALGAPB, A2ML1, KDR, AFF3, LAMC2, RPSA, LEP, CTCF, ISG20, BCRP3, COX8A, MEIS1, IL18, EIF2AK4, MLH1, MIR34B, MIR221, APAF1, CYP2B6, BIRC5, EFS, IL1B, SIRT1, MIRLET7B, IGFBP7, LINC01194, DCK, IGF1R, RMDN2, MYB, ZNF521, PTPRA, B3GAT1, PAG1, FANCL, WEE1, NLRP2, RTEL1, CD79A, CDKN2C, CD40LG, SHMT1, WNT5A, TRDC, ERCC2, ZAP70, GATA1, OPN1LW, ACKR3, CD7, PCBP4, RARA, TRDD3, SYK, FLT1, TAC1, PRAME, MIR203A, MIR181A2, SMUG1, SYNE1, ZNF197, MIR150, UHRF1, XPO1, UGT1A1, LAMTOR1, PPP1R13B, MMP9, TCF7L2, NSD2, MIR142, ABCC4, MIR126, TNFSF10, CIB1, MIR223, TERT, NUDC, KRT7, IGK, VDR, UBE2I, RMDN1, LCK, VWF, WT1-AS, H3P12, MIR1290, CXCR6, IL24, LMNA, LMO1, RASSF10, ATRAID, LPA, PTP4A3, SCLY, MDK, PACSIN2, MIR335, TLR4, MAP3K7, CD99, TFRC, RMDN3, AUTS2, LRPPRC, PGF, ABCB4, PHF2, PMEL, AFF4, GLS2, SET, DHX32, NR0B2, LPAR2, HAP1, CCNA1, S100A8, S100A6, SMYD2, PRDM9, IGHV1-12, EIF3A, PRKCB, MAPK1, MAP2K1, PSG2, BAALC, PTK7, TBL1XR1, PVT1, EEF1E1, HAVCR2, TOM1, TAM, MUC1, BTLA, PTPRG, STAT1, SSTR4, TES, CASP8AP2, NFKB1, NM, SYBU, NNMT, MAFK, DAZAP1, TPPP2, SOX4, SNX2, NT5E, OPRK1, PAEP, PRKN, WNT3A, PDGFRA, STIL, ZEB2, PECAM1, VPREB1, NAT1, GATA2, EPHA3, ETFA, BRAF, ERBB2, EPO, BMP4, HLA-C, CEACAM5, EPHX1, HLA-DQB1, CEACAM1, CFL1, HMMR, CEACAM3, HOXA5, CCN1, CEACAM8, ENO2, ENG, CHEK1, HOXB7, SERPINC1, HSPB1, ABCC2, EGF, ICAM1, IFNB1, IGF1, IGFBP2, MECOM, EXT1, BRS3, F3, FOLH1, FN1, FUS, G6PD, CCK, CBL, FLT3LG, CBFB, FOXO1, CD28, FGF2, CD80, FAT1, GFI1, CAT, CASP10, FANCC, CAMP, CXCR3, GPR42, GPT, CD58, DDR1, GSK3B, GSTM2, MSH6, BTK, IGFBP3, CEACAM7, FOS, CSF3R, CTLA4, AHR, EDNRA, E2F1, IRS1, CXCL8, DPYD, CTSG, ACTB, DCC, INPP5D, IL4, ADRA2B, ADRA1A, IL6ST, ABO, KIR2DS1, DPP4, TCFL5, DDX41, CD70, CD47, ERVW-1, IL23A, HDAC7, CST3, TRIM33, EMCN, CD72, WWOX, IGF2BP2, ZMYND11, ISYNA1, KDM5B, WNT16, WAC, TMED7, CD69, CD48, CD59, CSN2, MAP3K20, THEG, DCTN6, TNFSF13B, ZBTB7A, PLK4, DACT1, EBP, CD37, BCL11A, IGF2BP3, SEPTIN11, CD2, CD1D, PRDX4, CCND3, ATF7IP, ANP32B, CNDP2, ZNRD2, CCND2, CXCL13, CCNC, CYBB, ACSS2, CIB2, ZC4H2, MYDGF, CYLD, PRMT5, IMPACT, CD5, KDM3B, COLEC10, ARPP21, IL17D, TLR9, H2BS1, RIN2, PDLIM5, CD36, ADAMTSL4, TNFSF8, QRSL1, FBLIM1, GIPC2, WBP1L, TNFRSF8, MOCOS, MSTO1, ELP2, CD14, CD79B, RASSF1, GPR132, CKS1B, COBL, ATP11A, ARHGEF12, CCR5, DICER1, CKS2, SPIDR, CLCF1, CISH, CHI3L1, SSBP2, LY96, PLA2G15, TFIP11, FBXL2, LETMD1, CHRNA4, RIPK3, MLC1, CYFIP1, MPRIP, CNTFR, CREB1, CASC3, WDHD1, CILK1, CARD8, SACM1L, KLRK1, CRHR1, CORO1A, MAPRE1, CR1, CD160, ADAMTS13, USP33, WWP1, PIM2, SEPTIN6, CHRM3, NAT9, CDH11, TRBV7-9, CEL, CEBPA, HCST, CDX2, HPSE, PPP1R13L, CDKN2D, TRBV16, TRBC1, STAP1, TRAC, TRIB2, SETD2, CDK9, POLG2, CD274, CCR9, CDH13, IGHV3-69-1, NMU, IGHV3OR16-7, SMR3B, FBXL5, FBXO8, TSPAN16, CRKL, STEAP1, SLC27A4, CEACAM4, SLC27A5, DKK3, DKK2, PCDHA@, AGO2, NAAA, RAB40B, IL17C, CSF1, PCDH17, NEU3, KIR3DL2, RNF20, AREG, BIRC2, MIR15A, MIR16-1, MIR17, ANXA5, MIR185, MIR187, MIR192, MIR196A1, ANXA2, MIR206, MIR210, MIR181A1, MIR214, MIR22, ALPP, ALPI, MIR29B1, MIR29B2, MIR29C, MIR31, APRT, MIR144, ALK, MIR143, BCRP4, PGP, HOXA-AS2, BCL9, DDX51, CLEC4D, ADAMTSL5, ABCB5, H3P44, TICAM2, BAK1, B2M, ATRX, ATR, ATIC, MIR100, MIR125B1, MIR125B2, MIR128-2, MIR137, ASS1, MIR34A, MIR9-2, PCSK9, CDKN2B-AS1, SYCE1L, MFT2, ADM, ACTN4, TMED7-TICAM2, ACTG1, MIR3117, MIR2909, SNHG16, PPR1, KLRC4-KLRK1, COMMD3-BMI1, LOC102723407, LOC102724334, CBSL, LOC102724971, MTCO2P12, ABCA3, H3P13, H3P23, H3P47, MIR665, GGTLC4P, MIR9-3, GGT2, MIR99A, MIR17HG, BLID, AKR1B1, ALB, MIR339, AFM, MIR424, MIR425, H4C15, MIR499A, POU5F1P3, ADRB2, POU5F1P4, GGTLC5P, SNORD116@, MIR595, MIR625, MIR652, GGTLC3, POTEF, GCSAM, ZDHHC23, METTL3, SLC28A3, TNMD, CBFA2T3, FBRS, IKZF5, GORASP1, PLEKHG2, RANBP17, BCL11B, RUNX2, WNK1, CAV3, ZMAT4, CASP2, CAPG, TRABD, PNPLA3, TSGA10, PBX4, LBH, AMN, DOCK8, ELSPBP1, PRDM16, MXD3, HPSE2, FMN2, SPHK2, TCIM, CBS, SLC12A9, CBLB, KNL1, AVEN, ZNF695, GOPC, SALL4, RUNX3, SCYL1, BIRC6, DLEU1, PCDH10, KLHL1, METTL14, CCAR2, KMT2C, BACH2, CALR, CALCR, CERS6, EXOSC6, BRCA1, BMP6, UHMK1, SLX4IP, CMPK2, BLVRB, PRRC1, PACRG, CTCFL, CXCR5, PDIK1L, BHMT, CREBRF, CLEC12A, ZNF296, RASSF6, CFB, DLEU7, ZEB1-AS1, JMJD1C, IL27, H4-16, TWIST2, CHST9, TADA1, AIF1L, PARP9, SETDB2, MAGT1, BUB1, ZCCHC7, MAML2, ACCS, ATAD1, ZNF382, UBASH3B, ABCC11, ZFP36L2, LHX4, RCSD1, DNER, UBE2Q2, PRRT2, NLRP3, FCRL1, ZFP36L1, CYP1B1, DNMT1, LILRB2, PMAIP1, PNN, SEPTIN5, SEPTIN4, POLD1, POMC, POU5F1, PPARA, PTPA, PRF1, HIF1A, HIC1, HDC, HDAC2, PRKCA, HAL, H2AZ1, GZMB, MAPK8, GZMA, MAP2K2, MAP2K7, HK1, PLK1, CYP2C19, PLCG2, HOXB5, HOXB4, PAM, HOXB3, PARN, HOXB2, HOXB1, PCNA, PDE1A, PDGFB, HOXB@, HOXA10, SLC29A2, HNF4A, HMOX1, HMGB1, HLX, PIM1, HLA-DRA, HLA-DQA1, PLAT, EIF2AK2, PRPS1, PRSS1, GYPE, RPL22, GLI3, GLI2, GH1, S100A9, S100A10, GGT1, SCD, SRL, CCL2, CCL3, CCL4, CCL21, CCL22, XCL1, GFER, SELE, SELPLG, GDF10, SRSF2, SFTPD, BRD2, RMRP, RIT1, PVR, GYPB, PSMD9, PSMD12, GYPA, PTGS2, GSTM3, GRIK2, GRIA1, PTPRO, RAG2, GML, RAP1GDS1, GPER1, PLAAT4, KDM5A, RBBP4, GNG11, REG1A, GNA15, REN, P4HB, OTC, SIX6, MAP3K10, LYL1, LYN, MARCKS, SMAD7, MAOA, MAPT, MBL2, MBP, IRF3, MCM2, CD46, SMCP, IRF1, INSR, MEF2C, CXCL10, MEFV, ING2, MFAP1, KITLG, IL16, CYP4F3, LTB, LTA, LEPR, KIR2DL1, KCNH2, CD82, JUND, STMN1, LBR, JUNB, LCN2, JUN, LGALS1, LSS, LGALS3, ITPR1, LIPA, FADS1, ITGB1, ITGAM, ITGA4, LPL, IRF4, IL12B, IL12A, OPRM1, IL11, NELL1, NFATC2, NFIL3, NFKB2, NGFR, NKX3-1, HSPA5, HSPA4, PRMT1, NOS3, HRAS, NOTCH2, HPR, PNP, HOXD4, HOXB9, YBX1, HOXB8, NTRK1, NUP88, HOXB6, NEDD9, NEDD8, HSPB2, IGL, MMP1, IL1RN, MOS, CD200, MPL, IL1A, MPP1, MPST, MRE11, RBPJ, IAPP, MSR1, IGFBP4, COX2, MTHFD1, IGFBP1, IGF2, IFI27, MYH11, CEACAM6, KAT2A, SIAH2, GATA4, HSPB3, ELK3, AKR1C3, SOCS1, ELK1, BECN1, ELF3, TNFSF13, ELANE, FADD, TRIM24, EIF5A, EGR1, EGFR, CFLAR, HDAC3, NR1I2, PER3, SQSTM1, EFNB1, ENDOU, BCL10, PIK3R3, IRS4, ELN, GFI1B, EPHA1, KMT2D, HMGA2, TCL1A, TAF15, COIL, MLRL, H4C9, CTTN, H4C1, H4C14, H4C4, H4C6, H4C12, H4C11, H4C3, H4C8, H4C2, H4C5, H4C13, MBD2, NOL3, EPHB2, PHC1, DNM2, SARDH, DLX3, HDAC6, HDAC5, TIMM8A, DEFB1, DHX15, ABCC5, ABCB6, PPIF, RASGRP1, DDC, NAMPT, BRINP1, DAP, TRIB1, MSLN, SPRY1, CD55, NET1, P2RY14, DNMT3A, HDAC4, CD83, PKD2L1, SPAG9, PIAS2, ARHGEF1, EDNRB, IL1RL1, AURKB, MSC, PDLIM7, KLF4, KMT2B, SLIT2, NRXN1, DUSP7, PIGL, BAG4, CLOCK, NCOR1, TCL1B, DNTT, KAT6A, EPHB4, SLA, THY1, FLT4, TACR1, FLII, TAT, TCF4, FLI1, TCF7, ZEB1, TCF12, TCOF1, TRB, FOXM1, FH, FER, TERC, TERF1, FDXR, TFR2, FCGRT, FCGR2B, THBD, SYT1, AFF2, ABCC8, GAD1, SLC6A8, GAS6, SLC25A1, SLCO1A2, SMARCA1, SMARCB1, GART, FSCN1, GAPDH, SOD2, AURKA, SORL1, SOS1, SOX11, SPI1, FRAXE, SST, FOSB, STAT3, STC1, THPO, TIMP2, DEK, TLE1, F2R, VEGFC, VIS1, TRPV1, EWSR1, LAT2, ETS1, WNT7A, WNT10B, WNT2B, ESR1, ERCC1, XRCC1, XRCC3, XRCC5, ZBTB16, ZBTB17, MAP3K12, PRDM2, MOGS, USP7, VCP, NR1H2, UNG, TTC4, FAP, TMSB4X, PTK2B, TNFRSF1A, TOP2A, FABP3, TPM3, F10, NR2C2, TNFSF4, UCK2, TNFRSF4, TXN, TYK2, F9, TYRO3, F8, UCHL1, UCN, UMOD, RELA
    • Leukemia, Acute Lymphoblastic, Susceptibility To, 2 Omim
      For a discussion of genetic heterogeneity of susceptibility to acute lymphoblastic leukemia, see ALL1 (613065). Mapping In a genomewide association study of 317 patient with ALL and 17,958 controls, Trevino et al. (2009) found an association between ALL and 3 SNPs on chromosome 7p12.2. These were in linkage disequilibrium and located in the IKZF1 gene (603023) (rs11978267, p = 8.8 x 10(-11)) and the DDC gene (107930) (rs2167364, p = 2.8 x 10(-6) and rs2242041, p = 9.9 x 10(-7)). Trevino et al. (2009) concluded that germline variants can affect susceptibility to, and characteristics of, ALL and specific ALL subtypes. In a genomewide association study of 2 case-control series, totaling 907 ALL cases and 2,398 controls, Papaemmanuil et al. (2009) found a significant association between ALL and a SNP at chromosome 7p12.2 in the IKZF1 gene (rs4132601, OR of 1.69, p = 1.20 x 10(-19)).
    • Lymphoblastic Leukemia, Acute, With Lymphomatous Features Omim
      Patients with acute lymphoblastic leukemia (ALL) who present with bulky disease of the lymph nodes, spleen, and mediastinum, so-called lymphomatous ALL (LALL), appear clinically to represent a distinct category of ALL of T-cell lineage. The biologic basis of this distinction was pointed out by Chilcote et al. (1985) who found that 6 of 8 patients with clinical features of LALL had karyotypic abnormalities leading to loss of bands 9p22-p21. The mechanisms varied and included deletions, unbalanced translocations, and loss of the entire chromosome. Only 1 of 57 patients without LALL had an abnormality of chromosome 9 at diagnosis. Loss of a 'suppressor' gene (RB1; 614041) comparable to that in retinoblastoma (180200) was postulated.
    • Acute Lymphoblastic Leukemia Orphanet
      A rare disease characterized by malignant proliferation of lymphoid cells blocked at an early stage of differentiation and accounts for 75% of all cases of childhood leukaemia. Epidemiology About 3,000 children in the United States and 5,000 children in Europe are diagnosed with ALL per year. Clinical description The peak incidence occurs between 2 and 5 years of age. ALL may be either asymptomatic or acute with a life-threatening haemorrhage, infection, or episode of respiratory distress. Although ALL primarily affects the bone marrow and peripheral blood, any organ or tissue may be infiltrated by the abnormal cells.
    • Acute Lymphoblastic Leukemia Gard
      Acute lymphoblastic leukemia (ALL) is a type of cancer in which the bone marrow makes too many lymphocytes (a type of white blood cell). It may develop in children or adults. ALL spreads to the blood fairly quickly, and then may spread to other areas of the body such as the lymph nodes, liver, spleen, central nervous system, and testicles (in males). Signs and symptoms of ALL may include fever, easy bruising or bleeding, feeling tired, loss of appetite, pain in the bones or abdomen, and painless lumps in the neck, underarm, stomach, or groin. ALL is typically caused by random, non-inherited changes in the DNA of immature lymphocytes called lymphoblasts. However, some people may inherit a genetic susceptibility to developing ALL.
    • Acute Lymphoblastic Leukemia Wikipedia
      Medical imaging (such as ultrasound or CT scanning ) can find invasion of other organs commonly the lung , liver, spleen, lymph nodes, brain, kidneys, and reproductive organs. [28] acute lymphoblastic leukemia (ALL), peripheral blood of a child, Pappenheim stain, magnification x100 bone marrow smear (large magnification) from a person with acute lymphoblastic leukemia bone marrow smear from a person with acute lymphoblastic leukemia Immunophenotyping [ edit ] In addition to cell morphology and cytogenetics, immunophenotyping , a laboratory technique used to identify proteins that are expressed on their cell surface, is a key component in the diagnosis of ALL.
    • Acute Lymphocytic Leukemia Mayo_clinic
      Overview Acute lymphocytic leukemia (ALL) is a type of cancer of the blood and bone marrow — the spongy tissue inside bones where blood cells are made. The word "acute" in acute lymphocytic leukemia comes from the fact that the disease progresses rapidly and creates immature blood cells, rather than mature ones. The word "lymphocytic" in acute lymphocytic leukemia refers to the white blood cells called lymphocytes, which ALL affects. Acute lymphocytic leukemia is also known as acute lymphoblastic leukemia. Acute lymphocytic leukemia is the most common type of cancer in children, and treatments result in a good chance for a cure.
  • Plague (Disease) Wikipedia
    Members of the unit such as Shiro Ishii were exonerated from the Tokyo tribunal by Douglas MacArthur but 12 of them were prosecuted in the Khabarovsk War Crime Trials in 1949 during which some admitted having spread bubonic plague within a 36-kilometre (22 mi) radius around the city of Changde . [28] Ishii innovated bombs containing live mice and fleas, with very small explosive loads, to deliver the weaponized microbes, overcoming the problem of the explosive killing the infected animal and insect by the use of a ceramic, rather than metal, casing for the warhead.
    IL17A, ODC1, CCR5, FPR1
    • Plague Orphanet
      Plague is a severe bacterial infection caused by the Gram-negative bacterium Yersinia pestis . Epidemiology It is extremely rare in Europe but still spreads in Africa and, to a lesser degree, in Asia and Latin America. Clinical description There are two clinical forms of the disease: bubonic plague, characterized by painfully inflamed lymph nodes called "buboes'', an elevated temperature and an altered clinical state; and pulmonary plague which manifests itself as thoracic pain, a cough with bloody expectoration, an elevated temperature, an altered clinical state and consciousness disorders. Etiology Plague is transmitted from animals to humans by fleas. Rodents are the reservoir for the disease. Plague is also transmitted between humans via the respiratory route. Diagnostic methods Diagnosis is based on isolation of the bacterium in the bubo, blood or expectoration, or from serology.
    • Plague Mayo_clinic
      Overview Plague is a serious illness caused by a germ called Yersinia pestis. The germs mostly live in small rodents and their fleas. The most common way for humans to get plague is a flea bite. Plague is a rare disease. The illness mostly occurs in only a few countries around the world. In the United States, plague affects a few people each year in rural or semirural areas of western states. Plague usually can be treated with antibiotics. If not treated, the illness is often deadly.
  • Vertebral Subluxation Wikipedia
    However, it is not clear whether these afferent nerves are modulated during normal day-to-day activities of living and, if so, what segmental or whole-body reflex effects they may have." [27] Edzard Ernst has stated that the "core concepts of chiropractic, subluxation and spinal manipulation, are not based on sound science." [28] An area of debate among chiropractors is whether "vertebral subluxation" is a metaphysical concept (as posited in B.
  • Osteosarcoma Wikipedia
    Overall survival prognosis is about 30%. [28] Deaths due to malignant neoplasms of the bones and joints account for an unknown number of childhood cancer deaths.
    TP53, CHEK2, RB1, RECQL4, GRM4, SQSTM1, WRN, MMP2, EGFR, MET, RUNX2, MYC, EZH2, VEGFA, AKT1, GSTP1, SIRT1, PHLDA2, BMI1, DHFR, TNFRSF11A, KCNH1, JUN, MIR130B, MIR93, MIR328, RFC1, LOX, NR1I2, MIR106B, WT1, CCNB3, EXT1, ESRRA, CYP3A4, PRDX2, BCOR, EIF2S1, BRD4, FOLR1, EXT2, MIR302B, TOPORS, ZW10, TAF15, MST1R, RGS1, BRCA2, MDM2, IL3, CITED2, AKAP12, CDKN2A, LZIC, ATRX, MTAP, RPS19, LMNA, NFIB, TNF, SOX2, CXCR4, CD44, TNFSF11, TNFSF10, EZR, CDKN1A, GRAP2, CDK4, S100A4, PROM1, SPP1, STAT3, TBX5, ZEB1, CCK, TGFB1, AIMP2, PIK3CD, ROCK1, PTK2, IL1B, IGF1R, IGF1, HMGB1, HIF1A, GSK3B, GLI2, GLDC, MTOR, FOS, FN1, FOXM1, FGFR1, ESR1, ERCC2, ERCC1, EGF, ERBB2, EPHB2, IL6, CXCL8, STMN1, PIK3CB, PTGS2, PTH, PTEN, MAPK3, MAPK1, PLK1, PIK3CG, AHSA1, PIK3CA, CTNNB1, ABCB1, CRK, PCNA, TNFRSF11B, MAPK14, COX2, MMP9, CCN2, YAP1, H3P10, MIR27A, TUG1, WWOX, MIR133B, BMP2, MIR214, BGLAP, MIR21, CD274, APEX1, BCL2, CCND1, POLDIP2, RNF19A, ADAMTS17, MIR145, MALAT1, FBXW11, TBC1D9, MIR143, ADAMTS6, CASP3, ACTB, MTCO2P12, MIR34A, MIR19A, SOX9, MTDH, MIR144, MIR126, PTH1R, FGF2, E2F1, SETD2, COPS3, MEG3, CTLA4, SATB2, MIR183, FAS, GDF2, MIR20A, HPGDS, HSPA4, BECN1, SOX4, VDR, KIT, MIR17HG, CCN1, MAPK8, MIR335, MIR22, XIST, TGFA, ALB, ERCC5, MAPK7, MIR140, MIR142, POU5F1, PMP22, PARP1, HSP90AA1, MIR542, MMP13, MIR17, MIR451A, NOTCH1, NR3C1, MIR203A, MIR221, ANXA5, GH1, MCL1, MIR150, CXCL12, AURKB, FSD1, SEMA6A, TWIST1, ZNF395, FSD1L, WNT5A, SLC19A1, SLC2A1, NEAT1, THBS1, PTHLH, WIF1, RAC1, SMUG1, ZNRD2, H3P23, LOC110013312, MIR223, IGF2, MIR30A, CASR, IFI27, VIM, HSPA5, COMMD3-BMI1, GDE1, TIMM8A, UCA1, TMED7-TICAM2, GSTT1, MIR340, TMED7, CUL4B, MIR217, GLI1, TNKS, MIR503, POU5F1P3, POU5F1P4, FOXO1, FASN, MIR132, SLC12A9, DCTN6, MIR199A1, ROS1, CASP9, MIR206, MIR199A2, RAF1, SPARC, MIR210, MIR155, HMGN5, SMAD2, PSMD9, TICAM2, FOXO3, SERPINF1, MIR148A, BCAR4, CDK19, MIR100, MIR106A, RELA, MIR664A, SNHG1, SNHG16, ESR2, MICA, PPARG, FOXC2-AS1, ERBB4, PLAAT3, PVT1, MIR139, MIR491, TIMP2, FOXP1, MIR182, ITGB1, ACKR3, MIR29A, MIR29B1, MIR134, IGFBP5, CD276, COL18A1, ICAM1, CD99, MIR205, MMP3, HMGA1, EPAS1, MSN, HAS2, MIR135B, SKP2, LEF1, GSTM1, MIR195, MIR212, SDC2, MIR382, RECK, BAX, CDK6, CDC20, BMP7, CLU, XIAP, DNMT1, ATM, CASP8, CXADR, CHEK1, ALDH1A1, PDCD4, AKT2, ZEB2, MIR186, MKI67, NR1I3, MMP1, NANS, SIRT6, HLA-DOA, MIR375, OBP2A, MIR204, ABCC1, NOB1, MTX1, CAV1, DKK1, NME1, MIR29B2, MIR29C, MDM4, ABCB6, LILRB1, MIR31, TRIM13, MIR376C, PDPN, ZFAS1, NDRG1, PAEP, MIR184, MIR152, MIR15A, LIF, IGFBP3, KRAS, KIF22, IL1A, KISS1, KDR, HAVCR2, SNHG12, GSTK1, SOX2-OT, JAK2, IL11RA, SLCO6A1, IRS1, PTRH1, LDHA, FER1L4, ROCK2, MIR127, DANCR, HRAS, KMT2C, GAS5, ARR3, MIR141, HSF1, SMAD4, CCL2, HTC2, GORASP1, WNK1, ATF4, BGN, IDH1, MIR422A, EIF4E, YBX1, SRC, TP63, SYT1, DUSP1, E2F2, TAZ, PRKAR1A, CDK11B, MIR486-1, TGFB2, HOTAIR, CDKN2B-AS1, CD47, MIR765, EWSR1, MAP2K7, CXADRP1, FGFR2, FGFR3, HSP90B1, MIR33B, ECT2, VWF, MIR590, VCP, COL1A1, RNASE3, CDH11, CDKN1B, SATB1, SIX1, KLF4, ATG5, SNAI1, CCNB1, TSPAN31, CREB1, MIR497, RIPK1, CCNE1, SPG7, TNFRSF10B, TP73-AS1, MAP2K4, EBF2, TP73, SP7, SMAD7, RAD51, MED19, RAC2, UVRAG, TRAF6, ITGA2, TIMP3, POLD4, CDKN2B, NR1H2, RAB22A, SMAD1, AFAP1-AS1, ITGAV, SFRP2, RPAIN, TRIM27, CDK2, LGALS1, ARHGAP24, SP1, RPE65, LIMK1, PDCD1LG2, LPA, TERT, LRP5, LSAMP, TGFBR1, IL33, GGCT, CYC1, AURKA, CDH2, PAK5, GDF15, MEF2D, HSPB3, PTPA, IL24, NOTCH3, CKAP4, PLK2, ZEB1-AS1, ROR2, ABCC3, KHDRBS1, OXA1L, AGPAT2, SERPINE1, PAX3, CRP, MAP3K5, XPR1, RECQL5, PDGFA, PKM, PDGFRB, ABCG2, PECAM1, PIM1, TRIM14, PFKFB3, HDAC4, CDK14, HDAC9, RASSF1, FZD1, NFKB1, KLRK1, POLE4, CTBP1, MFAP1, BMP6, TRPV1, FBXW7, DCAF1, WNT1, MMP7, CDK1, DCTN4, MMP16, MNAT1, ING4, SOST, XRCC3, SENP1, MAP2K1, SGSM3, DKK3, LATS2, GNL3, HMGA2, NUP62, MXI1, PRAME, CA9, WEE1, MAD2L1, MIR449A, MIR130A, MIR200B, JAG1, HSPB1, HSPB2, MIR137, MIR136, TNC, MIR200C, MIR708, HES1, MIR506, HGF, MIR23B, ERG, HDAC2, MIR421, IFNA1, IFNA13, EDN1, RHOA, IFNG, OIP5-AS1, MIR301A, MIR191, MIR193A, FBN1, F3, APRT, FOXA1, MIR181A2, MIR18A, AGFG1, HOXA9, MIR320A, MIR26B, FLT1, AR, MIR199B, MIR34C, MIR25, ALK, MIR874, IL6R, IL11, GHR, MACC1, MIR410, MIR409, KLRC4-KLRK1, MIR361, IL10, MIR23A, MIR377, MIR370, ANXA2, GTF2H1, MIR381, MIR224, FHIT, ANPEP, FRZB, H3P5, EPHA2, MIR192, EGR1, MIR202, MIR493, MIR122, ADM, ERBB3, DCN, MIR107, MIR1908, MIR330, APC, MIR211, IL2, KMT5A, DDB1, AGTR1, MIR504, CD86, TAM, HAS2-AS1, HAT1, CD36, AXIN2, CUL4A, SNHG6, MLRL, BAP1, SNHG3, CLDN8, MIR499A, TNFRSF25, PDLIM7, SLC9A3R1, MIR146B, CCNA2, MIR490, MIR488, MIR485, MAPK8IP1, ADAMTS3, ADAMTS2, AHR, RAB3D, CLOCK, CBFB, TRAF4, PTTG1, MIR494, MIR495, CCN4, MIR522, ADAM9, MIR181D, TNFRSF10A, NRP1, CFLAR, CCNG1, CCNC, SPHK1, MBD2, MIR193B, MTA1, LATS1, PDCD5, MNX1-AS1, HOXA11-AS, FZD5, MIR210HG, CDK5, LINC01672, MIR466, SPINK1, MIR1301, STK11, MIR1247, ADAM17, MIR543, TBL1X, TCF7, TCF21, PPP1R11, MIR885, CDH4, SOX5, SOX3, CD63, CDK8, CDR1-AS, CCL18, CX3CL1, LSINCT5, PCAT1, SFRP1, NNT-AS1, SRSF3, FBXW4, SHOX, SPRY4-IT1, SLC1A3, CDK9, SNAI2, FSCN1, MIR300, TGFBI, TGM2, MIR671, MIR363, VEGFC, MIR618, MIR598, MIR564, MIR552, NSD2, MIR539, SNHG20, WNT7B, WNT10B, CD151, XBP1, PRB2, YY1, MIR645, KDM6A, USP1, POTEF, TIMP1, CDH1, LOC730101, TLR4, TNFAIP1, HULC, MIR663A, MIR646, TRPS1, TYMS, UBE2I, MIR92B, SUMO1, UCN, MIR638, ALOX5, MIR448, GOPC, PLXDC1, MIR15B, MIR149, MIR146A, MIB1, STS, ASS1, MMS19, ATF3, BHLHE41, BIRC7, SNRNP25, TBL1XR1, ATIC, MIR125A, MIR16-1, BMP4, MIR424, MIR181C, ZBTB7A, SIRT7, FXYD6, KLK3, SOX18, FBLIM1, TET2, BMPR2, FKBP14, IMP3, MIR187, MIR185, URGCP, FASLG, DIABLO, HAND2-AS1, PHC3, TET1, DCAF11, TP53INP1, PRRT2, CYTOR, FOXP4, TWIST2, LINC00161, TRIM59, DLX6-AS1, TUSC7, LYPD5, SPC24, SATB2-AS1, IRX2, EWSAT1, SKA1, FOXP2, LINC01116, NKD2, LINC01194, SRCIN1, MAP1LC3B, MIR10B, ZNRF3, MIRLET7G, ING5, HAGLR, NKD1, LINC00511, FENDRR, DICER1-AS1, FOXD2-AS1, SNHG7, SNHG5, PLEKHO1, MIR19B1, GAL, PPARGC1A, CASC2, ARPC1A, MIAT, CAT, PDLIM5, BLID, POSTN, MIR98, IGF2BP1, MIR95, USP39, MIR33A, NES, MIR30C2, FRS2, ATG7, CIB1, TACC3, BCL2L11, MIR384, MELK, MIR378A, TRIM66, MIR376A1, HDAC6, RANBP9, NDC80, MIR374A, MIR342, SPRY2, KLF2, TUBA1B, MIR338, MIR30C1, ALPP, BIRC3, MIR302A, PTTG1IP, SLC7A11, DCAF13, WWTR1, NOC2L, MIR216A, RNU1-1, HBP1, LAMP3, BTF3P11, MIR215, MIR208A, KLF5, BRD7, BIRC2, MIR222, ANGPTL2, SASH1, CAMK2A, FERMT2, RIPK3, NUDT21, CASP1, AMBN, MIR299, KLF8, CALCA, ATF6, NT5C2, CNOT1, KDM4C, CALR, MCF2L, CCL5, AADAC, HSD11B2, CSF3, KLF6, OXTR, MT2A, DPEP1, CHI3L1, ETS2, ATP6, TNFRSF9, CISH, LPAR1, ODC1, EDA, MTHFR, LIMK2, LGALS3, GFRA1, POU2F1, P2RX5, MST1, PRKN, PML, PRDX1, RET, PLD1, ERCC3, MSH3, IL12A, LUM, GRM5, ARHGAP35, RECQL, CXCR3, RDX, GPI, GNAS, GLS, P2RX7, PRKCG, NTRK1, ILK, PTN, CTSL, PRKCA, E2F3, EIF2AK2, PDGFRA, ATN1, PRKCB, FRA16D, FPR2, FPGS, FOSL2, FOSB, FOXF1, NFE2L2, CRYAB, FOXC2, NME2, FLI1, ITGA6, FGF5, NR5A2, GABPA, IMPDH2, ING1, COL11A2, EFEMP1, ING2, MUC4, NOVA1, PSMC2, FGF1, JUND, MYCN, CCN3, NOTCH2, NPY, FTL, JUNB, CAPRIN1, ERCC4, CXCR2, ATF2, MAP3K10, HMGCR, MECP2, MDK, RPS6KA3, EP300, IL2RA, MMP11, HLA-A, CEBPA, CEBPB, HK2, HIC1, PAX6, DAXX, IGF2R, S100A6, IDH2, IRF8, S100A9, HOXB7, GADD45A, MGMT, DDOST, HOXC10, MIF, MID1, DDX5, MICB, PDK1, PDGFB, VCAN, RBPJ, MMP14, CTSB, PLAU, H3-3B, H2AX, CXCR1, CYP19A1, GZMB, MSH6, H3-3A, HDAC1, PLA2G4A, FAM83H, PWAR4, AXL, SCAI, SCARA5, CCDC80, FEZF1-AS1, ATR, CYP2B6, CXCL10, IGFBP1, IFI16, CMTM8, AKR1C1, DCC, CILP2, PAQR3, DAB2IP, AMOT, BARD1, IL16, ATHS, IRF1, NMS, IL31RA, ISG20, CD109, LINC01139, IRF2, H3P44, DBH-AS1, DDX3X, LINC00028, STK35, WDR66, A2ML1, TMEM119, APCDD1, ILF3-DT, FFAR4, HTR2A, MIRLET7I, IAPP, FBXO39, CBLL2, IL17A, SNHG15, IL27, USP17L9P, IL18, HOXA-AS2, USP17L2, ADGRF1, SBF2-AS1, IL15, BAG1, FOXR1, MIR100HG, HNF1A-AS1, CYP27B1, LINC00323, FBXL19-AS1, IFITM5, LINC00324, METRNL, TMEM189-UBE2V1, TBPL2, TMEM189, IL12B, IL1R1, LAMA1, RTKN2, UBXN2A, RASSF6, LINC00858, BCHE, ASXL1, IGFBP7, PRSS55, NAIF1, MIRLET7D, ZNF699, MIRLET7B, CTAG1A, DAPK1, GASAL1, IGHG3, STING1, DAB2, FOXK1, SCUBE3, ZNRF2, ATP6V1C2, B2M, SLX4IP, CCL3, LINC00628, SCPEP1, TNMD, LRRC4, CLSTN2, UBE2O, SRR, MAGEA4, TGIF2, SENP2, IL21, LRP6, MAGEA10, OVOL2, CXCL16, ZNF410, RAP2C, MCAM, HES4, NCOA5, SMAD3, DCLRE1C, MXD1, DEPTOR, SUV39H2, LSS, COLGALT1, VTCN1, TNFAIP8L2, LTA, MUL1, LTBP2, BDNF, IRX1, TACSTD2, MAPKAP1, ASPSCR1, TRPM8, MARCKS, RAPH1, TUT1, FANCM, CIP2A, WDR48, CHPT1, SPHK2, GPR137, ZC3HAV1, RETN, MEN1, MELTF, RPRM, CTPS2, METTL3, MYDGF, ZC4H2, UBAP2, PAG1, CEP72, IPO9, KDM4D, RABL6, DPYSL5, RAB8A, BMP1, BMP3, CTNND1, HACE1, MTUS1, BIRC6, TMIGD3, MCM2, CD46, SMCP, SALL4, RALGAPB, CTBP2, CD248, LPAR5, PNPLA2, PCBP4, UTP3, PDXP, SLC25A22, ATAD5, TNFAIP8L1, LINC00473, TTYH2, JAK1, MYOCD, SHKBP1, BCL2A1, SPOCD1, PRMT9, TBL1Y, STARD13, DHDDS, GADD45GIP1, LMLN, WNT3A, BCL2L2, CD82, CYBB, KCNMA1, ORAI1, ITGB3, EGLN3, ITGB2, CYLD, TPPP2, H4-16, ITGA3, TMEM45B, CPXM2, PRAP1, ITGA4, ITGA5, PANX3, ITGAM, CTHRC1, TNFRSF13C, CYGB, HELQ, GLCCI1, LARP4, CDCA5, KCNQ1, KIF5B, KIF11, TAS1R1, FADS1, BCR, CTSK, TNKS2, LNPEP, ULBP1, ULBP2, CTSD, LPL, FBXO11, RUBCNL, ASRGL1, ZC3H12A, SEMA6D, NRSN2, LRP1, WLS, OPN1SW, WNT5B, CBX2, SLC38A1, MYO18B, KDM2B, SPZ1, HVCN1, BCL6, BRMS1L, KRT19, L1CAM, MAGT1, TMPRSS13, RASSF4, BCL9, ITCH, FERMT3, SOX7, RASSF5, NUF2, MYL12B, HLA-DQA1, HSD11B1, NBAT1, EEF1B2P2, ESD, EDNRB, MIR940, MIR935, MIR216B, MIR873, MIR744, MIR876, EDNRA, ETS1, TSL, ETV5, MIR802, MIR454, S1PR3, MIR758, MIR208B, MIR944, MIR889, LOXL1-AS1, MIR1248, MIR1182, MIR1286, MIR1200, MIR1284, H3C9P, DNAJC3-DT, ADPGK-AS1, MIR190B, CASC11, MFT2, MIR1225, MIR1224, CD24, TMPO-AS1, MIR939, CCR2, EYA2, MIR1205, CDK11A, FBP1, MIR635, MIR630, MIR628, MIR627, MIR625, MIR624, FCN2, MIR613, MIR610, MIR603, MIR599, FDPS, MIR596, FEN1, MIR586, MIR584, MIR641, MIR642A, MIR643, USP17L24, USP17L30, USP17L29, USP17L28, USP17L27, USP17L26, F2R, USP17L25, LINC00460, FAU, SSX2B, SNHG4, F8, MIR661, MIR660, MIG7, FAT1, MIR1296, MIR1258, MIR577, MIR499B, GHET1, LNCNEF, B4GALT1-AS1, CCAT2, BLACAT1, NPTN-IT1, CTTN, PANDAR, FOXP4-AS1, LINC-ROR, FALEC, HIF1A-AS2, ENDOG, H3P12, ENG, SLC29A1, MIR2682, CSAG2, WWOX-AS1, HAGLROS, LINC01705, ELF2, H3P47, ABCA1, H3P9, BTG3-AS1, LOC110351180, ACLY, ACTA2, ELK1, CCEPR, NKILA, CERNA3, UPK3B, MYOSLID, PACERR, ACTG2, MIR4443, MIR4695, MIR1269A, ACTN4, HOTTIP, MIR449C, MIR761, EFNB1, DLG2-AS1, EFNA1, EEF1D, MIR1972-1, MIR1304, MIR1281, ADORA3, MIR1238, MIR1253, MIR1271, MIR1228, MIR1294, MIR1270, MIR3200, MIR4262, EPS15, THORLNC, TMX2-CTNND1, LINC00968, RAB11B-AS1, ACTL6A, ACYP2, CCAT1, TTN-AS1, PCAT6, MIR3928, CBR3-AS1, EPHA7, LINC00963, LUCAT1, EGR2, ITGB2-AS1, LINC01133, MIR582, MIR570, ARL2, ANXA6, GLUL, FFAR1, GRM1, DNASE1L3, DMD, GSN, DLG2, AMPH, ANCR, GSTM3, DKC1, MIR24-1, SEPTIN1, ANGPT2, ANXA1, HSD17B10, HAL, ALPL, MIR34B, MIR7-1, GJA1, ALDH1B1, MIR326, MIR323A, ALDOA, MIR151A, GHRH, GHRHR, DPP4, MIR7-2, ALOX5AP, MIR99B, DNMT3B, MIR96, GLI3, ALPI, MIR7-3, ANXA3, GSDME, MIR337, APAF1, HMOX1, AQP1, HNF4A, HNRNPD, HOXA5, AQP3, MIR16-2, HOXA13, HOXB1, HOXB2, MIR154, HOXB8, AREG, HOXC8, ARG2, PRMT1, RHOB, DHX9, HMGN2, HMGN1, HLA-C, HAS3, AIRE, HDGF, HELLS, CFHR1, DES, BIRC5, APOD, MIR190A, CTAG1B, MIR198, MIR196A1, HLA-DQB1, HLA-DRB1, HLA-DRB4, DDX10, DPT, GFER, MIR569, FOLH1, FOXC1, FOXD1, MIR509-1, FOXL1, MIR505, DTYMK, MIR502, MIR501, FLII, MIR520D, MIR519D, MIR524, MIR520B, FLOT2, FLT3LG, FLT4, MIR496, MIR487A, AGT, CERNA2, NME1-NME2, MIR567, FGD1, MIR449B, E2F6, ADRB2, MIR544A, FGF13, FGFR4, CRNDE, FGR, AGER, LINC00273, FHL2, VEGFD, H3P16, BCRP1, DTX1, MIR432, MIR339, DSPP, GAK, GAPDH, MIR379, GAS1, GATA1, GATA3, GC, GCG, MIR196B, GCHFR, MIR373, MIR372, DPYD, GDF10, MIR346, GFAP, ALCAM, XRCC6, MIR423, FUT3, MIR323B, MIR492, FOLR2, DSG3, MIR511, APLNR, MIR489, MIR452, MIR433, MIR425, MIR20B, H4C15, FUS, MIR429, MIR31HG, MIR4435-2HG, DUXAP9, MFN1, MBTD1, FERMT1, SPARCL1, H4C14, H4C13, H4C5, H4C2, H4C8, H4C3, H4C11, H4C12, H4C6, H4C4, H4C1, H2BC21, FZD9, FZD8, FZD7, PRKDC, PRKG2, LOH19CR1, SPOP, H4C9, ULK1, PPP2R2B, RUVBL1, CD28, KHSRP, CBX4, PRKAA1, DGKZ, PRKAA2, PARG, PIK3R3, PPM1D, IRS4, CUL1, PRKAB1, RASAL1, AAVS1, NR0B2, AXIN1, ARID1A, QKI, SLBP, MAP2K3, DAP3, PRDM2, ZIC2, ZFX, YWHAZ, YWHAG, YWHAE, DNAJC3, XRCC5, PRL, XRCC1, XPO1, XPA, CD74, PRLR, CD81, USP7, DEK, NAA10, BAG6, USP9X, COL9A3, NCOA3, COL9A2, COIL, CD40, GPR68, ALX1, COL9A1, KMT2D, AD5, FOSL1, CSRP3, TUSC3, MAFK, COL4A3, TFEB, SOCS1, MS4A1, EIF3A, PLCL1, HACD1, BUB3, PLCG2, LPAR2, DYRK1B, NEURL1, ATG12, CCNB2, SLC16A3, SLC16A4, PLG, SLC31A1, TBX18, DIRAS3, CLDN2, PLXNA1, CLDN10, PLCG1, RAB11B, EIF3B, PLAUR, NCR1, NCR2, CHST2, MAP3K8, CBR3, PKD1, TSIX, ADIPOQ, PLAG1, PPIG, LHX2, SLIT2, TCEAL1, CD163, PLAT, SOCS6, MSC, CLDN12, SYT7, SOCS3, F2RL3, CD247, DLK1, TNFRSF18, FADD, TNFRSF6B, COMP, TNFSF9, CD6, CRADD, MED1, TRADD, PPP2R2A, PEA15, CD14, VAMP8, EIF3H, EIF3C, POU1F1, IL18R1, INPP4B, PER2, PMCH, KYNU, CPNE1, BUD31, CCND3, VNN2, IER3, POLA1, CES2, CDK5R1, KAT2B, POLD1, POLR2C, POMC, PON1, NRP2, PRNP, WNT2B, PROS1, STIM1, STAT5A, CDH15, STAT1, STAR, SSX2, SSR1, TRIM21, SREBF1, RNU1-4, CDH18, SPOCK1, ROBO1, RPA3, RPL7A, RPL10, RPL34, RPS3, SULT1E1, RNH1, TCF3, RLN2, TCF4, REV3L, TBX2, CFL1, RFC2, CNTN2, TAT, TAL1, MAP3K7, TAGLN, TACR1, CETN1, TAC1, RHAG, SYK, VAMP2, SULT1A3, SOD1, SOAT1, RPS6KB1, SNCA, S100A8, SH3GL1, SRSF1, S100A11, S100A12, S100B, SDHC, SDHA, SAA4, SDC4, CDKN2C, SDC1, SAI1, CXCL5, CXCL6, CCL24, MAPK12, CDKN2D, SIX3, CDKN1C, SLC20A1, RPS9, SMPD2, SMO, RPS15A, SLPI, SLC22A2, SLC20A2, CDKN3, SLC1A1, SLC18A2, SLC16A1, SLC12A1, SLC3A2, SLC2A4, S100A1, S100A2, HNF1A, CDH6, PSMA6, TPP1, UQCRC1, PTPN7, PTPRZ1, UCHL1, PVR, UBE2V1, PXN, UBC, TYS, RAB13, TXNRD1, CDC25A, TTR, TTN, CDC27, TSHR, RAB27B, PTPN6, VASP, TCF12, VCAM1, WNT6, WNT2, COL3A1, PSMD10, PSMD12, PTCH1, VRK1, COL1A2, BEST1, VIP, PTGER1, CDC5L, VHL, CNN1, CDC6, CCR5, CMA1, HSP90B2P, TRAF3, RAD21, NR2C2, RASGRF1, TH, FOXN3, TGFBR3, RBP2, OPN1LW, TGFB1I1, CDH3, TFRC, NR2F1, REG1A, TERF2, TERF1, TEAD1, CDH5, REN, RENBP, THBS3, THOP1, TIAM1, TOP1, CRISP2, TPT1, TPR, TPM1, TP53BP1, CDC34, TOP3A, TNNC1, RASA1, TNFRSF1A, RANBP1, CDC42, TMSB4X, RAP1A, RAP2B, RARA, MED27, EIF2AK3, SOX6, CKAP2, AATF, CSF1R, NUPR1, NUDT1, TINF2, SPAG8, PRPF31, BTK, ATRNL1, NGDN, ND1, CLIC4, POT1, BUB1, MTNR1A, BRMS1, ARMC8, GREM1, CSF2, BACE2, PELP1, MAT2B, CSN3, MCAT, STK39, KCNMB4, RABGEF1, BHLHE22, PGAP2, BTF3, PDLIM3, BBC3, SND1-IT1, MSX2, MTBP, TSPAN13, NSG1, SND1, TXN2, TNFAIP8, CRABP2, SF3B1, COTL1, SRGAP2, PUM2, WDR7, MYL2, USP22, TRIM2, MYO10, CALCR, CEACAM6, RRP12, RHOBTB2, ATG4B, CALML3, KDM6B, COLGALT2, NCL, DDR1, MYD88, QPCT, HEY1, IL17RA, CADM1, SGK3, TRIM29, TRIM37, LDOC1, MMUT, PRND, CORO1C, CLEC5A, CA8, CCNDBP1, LPAR3, CSE1L, NNT, SUZ12, ICMT, DLL1, GIT1, BZW2, SEMA4C, BNIP3, SCN8A, KMT2A, MME, P4HTM, KRT20, ANKIB1, XRN1, TERF2IP, CTAA1, TREM2, CSPG4, TLR9, FGFRL1, MMP8, IL17D, MAP3K20, NSD3, LAMTOR1, MCTS1, MARCHF1, CAMK2N1, LGR4, DRAM1, PACC1, KIRREL1, NAT10, RCBTB1, PRMT6, CEP55, MSTO1, CDCA8, WRAP53, ANO1, KIF26B, ATG16L1, MOCOS, MAP3K9, RSF1, CDK12, RTEL1, BPHL, MPP1, FOXP3, TRAT1, IL22, KCNIP3, EFEMP2, MPST, PSAT1, RMC1, MSH2, UHRF1, KLF9, TBK1, NXT1, UBE2T, MSI1, MSMB, MED31, BSG, NDUFA13, TNFRSF12A, RAB23, BRCA1, TDP2, TRIAP1, LIMA1, ATRAID, MMP12, PLAC8, MPO, NT5C3A, CSNK1G2, BRAF, LINC00328, SDF4, MNDA, ANGPTL4, PPRC1, NELL1, CLUAP1, APC2, RAMP2, ABCC4, PCK2, LRRC17, NBR2, CBFA2T3, PCYT1A, TNK2, ZNF197, EBI3, G3BP1, HIPK3, TSPAN1, ACTR2, PQBP1, PTPRU, HUWE1, EFS, DLEU1, NCOA2, NMUR1, CREB3, CAP1, PAWR, GPNMB, SPON1, CAV2, CPQ, PAX1, PIAS3, MYL9, PAX4, SEMA3A, RUNX1, PAX7, TFG, AKR1A1, IKZF1, NR1H3, ELAVL2, PDCD1, ABCC5, ESPL1, ISG15, ABCG1, PGF, CREBBP, SLC25A3, CXCL14, PHEX, TP53I3, EEF1E1, NPEPPS, SERPINB6, ADAMTS1, SERPINE2, PIGF, ADAMTS4, PIGR, PGC, DOCK4, PGAM1, TOX4, PDE4A, HDAC5, SRA1, AKT3, MVP, MFN2, DDX46, PDK4, PFN2, GAB2, CRIP1, PF4, PFKFB2, RB1CC1, PIEZO1, EIF4A3, CARM1, SEMA4D, PDZD2, NOS1, FSTL1, CORO1A, CASP6, EMILIN1, TOPBP1, CNMD, WWP1, NOS2, CRY2, RAB31, GLIPR1, COPS5, KCNQ1OT1, IFI44L, ERP29, BTG3, EHD1, STRAP, LZTS1, KAT5, PTENP1, KDM4B, NEU1, KDM2A, NF2, MMRN1, NFIC, ZHX2, ATG14, VASH1, PHLDA1, RRAS2, MGLL, CBX3, NGFR, POLG2, NKX2-2, CANX, SUB1, BLCAP, JTB, MALT1, ORC2, NPRL2, OXT, TXNIP, MYL12A, SLCO1B1, TXNRD2, SORBS1, MRPL28, SIVA1, SLC34A2, P2RY2, P4HB, DCTN2, UBD, PAFAH1B1, IPO8, IGF2BP3, CRY1, CXCR6, WASF3, RAB10, NMU, HCP5, NPM1, HPSE, CCL27, NPPB, ZMYND11, CTCF, NRAS, KDM5B, STAG2, PLK4, PTGES3, TNFSF13B, OLR1, DNM1L
    • Osteogenic Sarcoma Omim
      A number sign (#) is used with this entry because of evidence that many instances of osteogenic sarcoma occur in association with retinoblastoma (RB; 180200), which is caused by mutation in the RB1 gene (614041) on chromosome 13q14. Osteosarcoma occurs frequently in Paget disease of bone, which can be caused by mutation in the TNFRSF11A gene on chromosome 18q22. Mutation in another gene on chromosome 18q may be mutated in cases of osteosarcoma. Osteosarcoma is a feature of Li-Fraumeni syndrome-1 (LFS1; 151623), caused by mutation in the TP53 gene (191170), and of Li-Fraumeni syndrome-2 (LFS2; 609265), caused by mutation in the CHEK2 gene (604373). Sporadic osteosarcoma has also been associated with mutations in the CHEK2 gene (604373.0005).
    • Osteosarcoma Mayo_clinic
      Overview Osteosarcoma is a type of bone cancer that begins in the cells that form bones. Osteosarcoma is most often found in the long bones — more often the legs, but sometimes the arms — but it can start in any bone. In very rare instances, it occurs in soft tissue outside the bone. Osteosarcoma tends to occur in teenagers and young adults, but it can also occur in younger children and older adults. Treatment usually involves chemotherapy, surgery and, sometimes, radiation therapy. Doctors select treatment options based on where the osteosarcoma starts, the size of the cancer, the type and grade of the osteosarcoma, and whether the cancer has spread beyond the bone.
    • Osteosarcoma Orphanet
      Osteosarcoma is a primary malignant tumour of the skeleton characterised by the direct formation of immature bone or osteoid tissue by the tumour cells. Epidemiology Classic osteosarcoma is a rare (0.2% of all malignant tumours) highly malignant tumour, with an estimated incidence of 3 cases/million population/year. Clinical description Osteosarcoma arises predominantly in the long bones and rarely in the soft tissues. The age at presentation ranges from 10 to 25 years of age. Diagnostic methods Plain radiographs, computed tomography, magnetic resonance imaging, angiography and dynamic bone scintigraphy are used for diagnosis, evaluation the extent of tumour involvement and for making decisions about the type of operation and, if necessary, the type of reconstruction required. Management and treatment In the past, all patients with osteosarcoma were treated by amputation but the cure rate was under 10% and almost all patients died within a year from diagnosis.
    • Osteosarcoma Gard
      Osteosarcoma is the most common type of bone cancer. The average age at diagnosis is 15. Boys and girls have a similar incidence of this tumor until late adolescence, at which time boys are more commonly affected. In rare cases, osteosarcoma occurs in adults. Although osteosarcoma tends to occur in the larger bones, such as the shin (near the knee), thigh (near the knee) and upper arm (near the shoulder), it can occur in any bone. A number of variants of osteosarcoma exist, including conventional types (osteoblastic, chondroblastic, and fibroblastic), telangiectatic, multifocal, parosteal, and periosteal. The cause of osteosarcoma is not known. In some cases, it runs in families, and at least one gene has been linked to increased risk.
  • Hypokalemia Wikipedia
    Concomitant hypomagnesemia will inhibit potassium replacement, as magnesium is a cofactor for potassium uptake. [23] Popular culture [ edit ] The plot of the science fiction novel Destiny's Road by Larry Niven centers around the setting's scarcity of available potassium, and the resulting deficiency and its effects on the world's colonists and their society. [27] [28] [29] [30] See also [ edit ] Bartter syndrome Gitelman syndrome Hypokalemic acidosis Potassium deficiency (plant disorder) Superior mesenteric artery syndrome References [ edit ] ^ a b c d e f g h i j k l m n o p Soar, J; Perkins, GD; Abbas, G; Alfonzo, A; Barelli, A; Bierens, JJ; Brugger, H; Deakin, CD; Dunning, J; Georgiou, M; Handley, AJ; Lockey, DJ; Paal, P; Sandroni, C; Thies, KC; Zideman, DA; Nolan, JP (October 2010).
    NR3C1, ADRB2, SST, POMC, INS, NPPB, AGT, NOS1AP, USP8, OCRL, CDH23, SCN4A, SCN4B, SCN5A, SCN10A, MAGED2, SCNN1A, SCNN1B, TRDN, SCNN1G, SLC2A2, SLC4A1, SLC12A1, AKAP9, SNTA1, KCNE2, TP53, BSND, AIP, CLDN10, SLC12A3, KCNQ1, SMAD4, KCNJ10, ANK2, ATP1A1, FXYD2, BMPR1A, CACNA1D, CACNA1S, CALM1, CALM2, CAV3, CLCN2, CLCNKA, CLCNKB, COL3A1, CTNS, CYP11B1, CYP11B2, CYP17A1, SLC26A3, HMBS, HSD11B2, KCNE1, KCNH2, KCNJ1, KCNJ2, KCNJ5, KCNJ18, SLC26A7
  • Precocious Puberty Wikipedia
    The association between LIN28 and puberty timing was validated experimentally in vivo, when it was found that mice with ectopic over-expression of LIN28 show an extended period of pre-pubertal growth and a significant delay in puberty onset. [26] Mutations in the kisspeptin (KISS1) and its receptor, KISS1R (also known as GPR54), involved in GnRH secretion and puberty onset, are also thought to be the cause for ICPP [27] [28] However, this is still a controversial area of research, and some investigators found no association of mutations in the LIN28 and KISS1/KISS1R genes to be the common cause underlying ICPP. [29] The gene MKRN3, which is a maternally imprinted gene, was first cloned by Jong et al. in 1999.
    GNAS, KISS1R, MKRN3, GNRH1, IGF1, LHB, PTGS2, CYP19A1, LHCGR, NR0B1, NR3C1, SMAD4, CDKL5, RAP1B, RAP1A, STXBP1, MAGEL2, PTH1R, RFC2, TXNRD2, FGFRL1, SCN2A, PPARG, SMARCA2, MRAP, PLAGL1, PCNT, STAR, PIGP, RAB23, HYMAI, APC2, CNTNAP2, KMT2B, GTF2IRD1, H6PD, NRXN1, PIGQ, BAZ1B, BSCL2, CASK, KMT2D, ALMS1, NSD2, WHCR, CLIP2, TBL2, KDM6A, SLC35A2, SETD2, TSC2, TSC1, RAI1, IQSEC2, NEUROD2, GLI3, FOS, MC2R, FLII, FLI1, SLC25A22, ELN, TRIM8, DHCR7, DDX3X, NNT, CTBP1, SIK1, CAV1, ARX, CAVIN1, NSD1, PNKP, DEAF1, GNAO1, AGPAT2, GTF2I, IDH1, IDH2, IFNG, LMNA, LIMK1, LETM1, INSR, CPLX1, KCNA1, GH1, ESR1, CYP21A2, LEP, KISS1, CRP, COASY, CREBRF, CD44, POMC, ZBTB7A, LIN28B, AMH, QPCT, ACACA, CHDH, CUL9, KCNT1, PAPPA2, LIN28A, PROKR2, RETN, CCL18, PHB2, C1QL1, APOA1, APOB, AR, COL1A1, CRH, CYP3A4, CYP11B1, DMD, ESR2, ESRRG, FMR1, FSHR, IGFALS, IPP, NPY, NR4A2, POU1F1, PTEN, REN, BRD2, TAC3, TGFA, TRPC6, TSHR, BEST1, DLK1, BMS1, MIR664A
    • Precocious Puberty Mayo_clinic
      Overview Precocious puberty is when children's bodies begin to change into adult bodies too soon. This change is known as puberty. Most of the time, puberty occurs after age 8 in girls and after age 9 in boys. However, Black, Hispanic, and Native American children might naturally reach puberty earlier. Precocious puberty is when puberty begins too early for the child who's going through it. In puberty, muscles and bones grow quickly. Bodies change shape and size.
  • Folie À Deux Wikipedia
    Both had, in addition, other symptoms supporting a diagnosis of emotional contagion , which could be made independently in either case. [28] Psychiatrist Reginald Medlicott published an article about the Parker-Hulme murder case called “Paranoia of the Exalted Type in a Setting of Folie a Deux - A Study of Two Adolescent Homicides”, arguing that the intense relationship and shared fantasy world of the two teenaged friends reinforced and exacerbated the mental illness that led to the murder: “each acted on the other as a resonator increasing the pitch of their narcissism.” [29] In 2016, a case involving a family of five from Melbourne , Australia made headlines when they abruptly fled their home and travelled more than 1,600 km (1,000 mi) across the state of Victoria because some of the family had become convinced someone was out to kill and rob them.
    CALR, SIRT1, ESR1, GCLM, GSTP1, DTNBP1, AKT1, ACE2, HPGDS, SLC6A4, PVALB, HTR6, HTR2A, HTR1A, NRG1, ACHE, GRM2, GRIN2D, GABBR1, DRP2, DRD4, DRD1, DPYSL2, COMT, BDNF, APOE, GRIN1
  • Cervical Intraepithelial Neoplasia Wikipedia
    A case-control study found that there is an approximately two-fold increase in risk i. [22] The findings of low quality observational studies suggest that women receiving treatment for CIN during pregnancy may be at an increased risk of premature birth . [23] [24] People with HIV and CIN 2+ should be initially managed according to the recommendations for the general population according to the 2012 updated ASCCP consensus guidelines. [25] Outcomes [ edit ] It used to be thought that cases of CIN progressed through grades 1-3 toward cancer in a linear fashion. [26] [27] [28] However most CIN spontaneously regress.
    MTHFR, POU4F1, LCN2, TP53, CDKN2A, H3P10, PDXP, VEGFA, IL10, MYC, SEC14L2, CST3, IFNG, BCL2, TGFB1, TNF, NFE2L2, HLA-DQB1, PTGS2, CD274, ERBB2, MKI67, MAL, REG3A, ALB, STS, TERC, TLR4, PDAP1, GSTM1, GABPA, FHIT, PYCARD, HLA-DRB1, MIB1, HMGB1, SERPIND1, LINC01191, HLA-A, HIF1A, GSTT1, HRAS, ASAP2, MTPAP, LAMB2, ASAP1, EZR, MLH1, MTR, HPGDS, CADM1, PCNA, TUSC2, PAPOLA, UBE2B, MRPS30, ESR1, ACP3, NME1, CD44, HAVCR1, PTEN, APC, PSMA1, FOXP3, PIK3CA, PGR, ERAP1, MUC1, IL1B, APOBEC3G, MMP2, MDM2, LIPA, RBM45, TAFA4, IDO1, CYCSP38, CABIN1, SIRT1, EPB41L3, RASSF1, CFLAR, BMI1, XRCC1, HSPB3, VIP, CA9, SLIT2, TP53BP1, RAPGEF5, CAT, TLR2, SEC62, CTDSPL, TERT, TAP1, SLC2A1, SIX1, IL2, TP63, CCR2, FOXO1, CRP, MIR21, CTNNB1, MIR124-2, IFNA13, HSPB2, IFNA1, CYP1A1, HSPB1, ASCL1, SERPINC1, MIR27A, ATM, MIRLET7C, MIR29A, MIR34A, BAX, NES, MASP2, PDPN, PPARGC1A, KLRK1, NLRP1, NXF1, MIR20A, FGF21, PART1, APRT, MKRN1, AR, MIR218-2, MTREX, ANGPTL2, MIR22, SIRT3, SASH1, LPIN1, MIR25, KDM4B, LAMTOR5, LHX8, CFDP1, MIR99A, BECN1, NRP1, LINC02605, LOC110806263, CCNA1, MTCO2P12, MBD2, COMMD3-BMI1, KLRC4-KLRK1, LIMD1, SLC6A5, CACNA2D2, CD163, MICA, MIR466, PLAA, GDF15, EI24, MIR551B, PIEZO1, KIR2DL5B, KEAP1, MIR378A, MFN2, ABCB6, TSPAN1, ADAR, RABGEF1, NET1, APOB, SMARCAL1, XIAP, DCLK3, SMOC1, SEMA4A, CENPH, MLVI4, MUL1, VTCN1, PANK2, RUBCNL, PPP1R2C, PDCD1LG2, CD276, ST6GALNAC5, EMC6, HAVCR2, IL33, ADM, SLC52A3, KIR3DL3, TWIST2, ADSS1, CMPK2, MIR124-1, IDO2, NRK, ANKS4B, IS1, OR10A4, STING1, MIR10A, MIR100, SEMA6A, AGT, MIR15B, KLF13, MIR152, EFEMP2, VHLL, SYCP3, GEMIN4, ANXA2, MIR146A, GMNN, METTL9, ANGPTL4, TLR7, ATRAID, MIR145, MIR143, CMPK1, AKR1B10, MIR126, TLR9, TERF2IP, CPVL, PRPF38B, ALK, IMP3, PDE5A, FBXW7, LAPTM4B, AGK, DIABLO, MIR125A, ACKR3, ENPEP, VCP, NUMB, KRT7, LGALS9, LGALS3, CENPA, CHEK1, LAMA3, KRT19, KRT14, KIR3DL1, NELL1, KIR2DS4, KCNMA1, KCNH1, CD82, ITGA9, CCR5, IL9R, LTA, SMAD4, CDKN3, MCM5, MYBL2, MMUT, MTRR, CDC6, CDH1, COX2, MYO1B, MPO, MMP9, CDK2, CDKN1A, MIA2, MFAP1, MET, MEST, CXCL8, IL7, IL6, GNAO1, GEM, GATA3, DUT, FN1, FLNB, FOXM1, EEF1A1, FGFR2, FGF2, EFEMP1, FBN1, ACSL1, EXT1, ESR2, EGFR, GLP1R, SFN, IGFBP5, PDIA3, IGF2, IFNAR2, IFNAR1, TNC, CSF3, HLA-G, HLA-DQB2, CYP2D6, HLA-DQA1, DAPK1, DAXX, ACE, NQO1, GSTM2, DPH1, LRBA, NOTCH1, USO1, SNAI1, SERPINH1, TFPI, CD247, AURKA, STAT3, SOX2, SOD1, SLC22A2, YBX1, SLC22A1, SLC6A2, STIL, ACVR2A, SDHD, CXCL12, S100A11, TGFBR1, TIAM1, TLR3, CASP3, ARID1A, HMGA2, FGF23, ZIC1, XPNPEP2, XK, VIM, BUB1, VHL, VEGFC, EIF4G2, UBE3A, CALR, CANX, TNFRSF1B, S100A9, S100A7, RP9, PRL, MAPK1, PPP2R1B, PPBP, CD86, POU2F2, POU2F1, POLR2D, PLAUR, PEG3, CD34, SERPINA5, PAX1, ENTPD1, SERPINB2, NT5E, MAP2K5, PRLR, ROBO2, PSMB8, ROBO1, REN, RBP4, RBBP4, RB1, RARB, RAP1A, RAN, RAB5A, PTN, CD80, PTGER3, PTCH1, PSMD2, PSMB9, PMEL
  • Cerebrotendinous Xanthomatosis Gene_reviews
    Clinical features of 55 individuals with CTX (27 males, 28 females) [Mignarri et al 2014]; * refers to features that were assessed in only a subset of the 55 individuals (i.e., osteoporosis was seen in 20/30 affected individuals).
    CYP27A1, IL6, BGLAP, CYP2B6, SPG11, IL2, CFB, SPG7, TNF, TP53, UTRN, SSPN, MBD2, XPR1, SLC10A1, NR1H4, INSL6, SIRT1, FTO, B4GALNT2, MIR98, SLC22A2, PTGDS, SLC6A3, HSD11B2, CTSK, CYP3A4, CYP27B1, HLA-A, HNF4A, HSD11B1, IFNG, PTH, IL10, KRAS, LDLR, MTRR, SLC26A4, POU2F2, OCLN
    • Cerebrotendinous Xanthomatosis Omim
      A number sign (#) is used with this entry because cerebrotendinous xanthomatosis is caused by homozygous or compound heterozygous mutation in the CYP27A1 gene (606530), which encodes sterol 27-hydroxylase, on chromosome 2q35. Description Cerebrotendinous xanthomatosis is a rare inherited lipid-storage disease characterized clinically by progressive neurologic dysfunction (cerebellar ataxia beginning after puberty, systemic spinal cord involvement and a pseudobulbar phase leading to death), premature atherosclerosis, and cataracts. Large deposits of cholesterol and cholestanol are found in virtually every tissue, particularly the Achilles tendons, brain, and lungs. Cholestanol, the 5-alpha-dihydro derivative of cholesterol, is enriched relative to cholesterol in all tissues. The diagnosis can be made by demonstrating cholestanol in abnormal amounts in the serum and tendon of persons suspected of being affected.
    • Cerebrotendinous Xanthomatosis Medlineplus
      Cerebrotendinous xanthomatosis is a disorder characterized by abnormal storage of fats (lipids) in many areas of the body. People with this disorder cannot break down certain lipids effectively, specifically different forms of cholesterol, so these fats accumulate in the body in the form of fatty yellow nodules called xanthomas. These xanthomas are most commonly found in the brain and in connective tissue called tendons that attach muscle to bone, which is reflected in the condition name (cerebro- meaning brain and -tendinous referring to tendons). People with cerebrotendinous xanthomatosis often develop neurological problems in early adulthood that are thought to be caused by an abnormal accumulation of fats and an increasing number of xanthomas in the brain. These neurological problems include recurrent seizures (epilepsy), movement disorders, impaired speech (dysarthria), loss of sensation in the arms and legs (peripheral neuropathy), decline in intellectual function (dementia), hallucinations, and depression.
    • Cerebrotendinous Xanthomatosis Orphanet
      Cerebrotendinous xanthomatosis (CTX) is an anomaly of bile acid synthesis (see this term) characterized by neonatal cholestasis, childhood-onset cataract, adolescent to young adult-onset tendon xanthomata, and brain xanthomata with adult-onset neurologic dysfunction. Epidemiology More than 300 patients have been reported worldwide. Prevalence is estimated to be approximately 1/50,000 among Caucasians. Clinical description The initial clinical manifestation may be neonatal cholestasis or chronic diarrhea from infancy. In 75% of cases, cataract is the first finding, often appearing in childhood. Infants may present with cholestasis and liver dysfunction. Xanthomata may appear in the 2nd or 3rd decade of life, in the Achilles and other tendons (elbow, hand, patella, neck).
    • Cerebrotendinous Xanthomatosis Gard
      Cerebrotendinous xanthomatosis is a disorder characterized by abnormal storage of fats (lipids) in many areas of the body ( lipid storage disease ). People with this disorder cannot break down certain lipids effectively (such as cholesterol), so these fats form fatty yellow nodules called xanthomas, that accumulate in the body, especially in the brain and the tendons that attach muscle to bone, which is reflected in the condition name (cerebro- meaning brain and -tendinous referring to tendons). Symptoms may include diarrhea, clouding of the lens of the eyes (cataracts), tendon problems and progressive neurologic problems, such as epilepsy, movement disorders, impaired speech (dysarthria), loss of sensation in the arms and legs (peripheral neuropathy), dementia, hallucinations, and depression. Other symptoms may include brittle bones that are prone to fracture ( osteoporosis ) and an increased risk of developing heart or lung failure because of lipid buildup. It is caused by mutations in the CYP27A1 gene. Treatment may involve chenodeoxycholic acid (CDCA), inhibitors of HMG-CoA reductase, coenzyme Q 10 and surgery to remove cataracts.
    • Cerebrotendineous Xanthomatosis Wikipedia
      Cerebrotendinous xanthomatosis Other names Cerebrotendinous xanthomatosis Cerebrotendineous xanthomatosis has an autosomal recessive pattern of inheritance . Specialty Medical genetics , endocrinology Cerebrotendinous xanthomatosis also called cerebral cholesterosis , [1] is an autosomal recessive form of xanthomatosis . [2] [3] It falls within a group of genetic disorders called the leukodystrophies . Contents 1 Presentation 2 Genetics 3 Diagnosis 4 Treatment 5 Eponym 6 See also 7 References 8 External links Presentation [ edit ] An inherited disorder associated with the deposition of a steroid known as cholestanol in the brain and other tissues and with elevated levels of cholesterol in plasma but with normal total cholesterol level; it is characterized by progressive cerebellar ataxia beginning after puberty and by juvenile cataracts , juvenile or infantile onset chronic diarrhea, childhood neurological deficit, and tendineous or tuberous xanthomas . [ citation needed ] Genetics [ edit ] CTX is associated with mutations in the CYP27A1 gene, located on chromosome 2q33-qter . [1] [4] The disorder is inherited in an autosomal recessive manner. [2] This means the defective gene responsible for the disorder is located on an autosome (chromosome 2 is an autosome), and two copies of the defective gene (one inherited from each parent) are required in order to be born with the disorder. The parents of an individual with an autosomal recessive disorder both carry one copy of the defective gene, but usually do not experience any signs or symptoms of the disorder. [ citation needed ] Diagnosis [ edit ] Elevated levels of serum cholestanol are diagnostic of CTX. Alternatively analysis of 27-hydroxycholesterol and 7 alpha hydroxycholesterol can be used.
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