��28��-��- – FindZebra Search

Advanced

Abortion In Georgia (U.s. State) Wikipedia

Jones ruled in favor of the injunction to block enforcement in his decision in October 2019, stating "By banning pre-viability abortions, H.B. 481 violates the constitutional right to privacy, which, in turn, inflicts per se irreparable harm on Plaintiffs." [28] Statistics [ edit ] In the period between 1972 and 1974, the state had an illegal abortion mortality rate per million women aged 15 – 44 of between 0.1 and 0.9. [29] In 1990, 796,000 women in the state faced the risk of an unintended pregnancy. [30] In 2010, the state had eight publicly funded abortions, of which all eight were federally funded. [31] In 2014, 48% of adults said in a poll by the Pew Research Center that abortion should be legal in all or most cases. [1] According to a 2020 study, the 22-week law reduced the number of abortions after 21 weeks. [32] Number of reported abortions, abortion rate and percentage change in rate by geographic region and state in 1992, 1995 and 1996 [33] Census division and state Number Rate % change 1992–1996 1992 1995 1996 1992 1995 1996 South Atlantic 269,200 261,990 263,600 25.9 24.6 24.7 –5 Delaware 5,730 5,790 4,090 35.2 34.4 24.1 –32 District of Columbia 21,320 21,090 20,790 138.4 151.7 154.5 12 Florida 84,680 87,500 94,050 30 30 32 7 Georgia 39,680 36,940 37,320 24 21.2 21.1 –12 Maryland 31,260 30,520 31,310 26.4 25.6 26.3 0 North Carolina 36,180 34,600 33,550 22.4 21 20.2 –10 South Carolina 12,190 11,020 9,940 14.2 12.9 11.6 –19 Virginia 35,020 31,480 29,940 22.7 20 18.9 –16 West Virginia 3,140 3,050 2,610 7.7 7.6 6.6 –14 Number, rate, and ratio of reported abortions, by reporting area of residence and occurrence and by percentage of abortions obtained by out-of-state residents, US CDC estimates Location Residence Occurrence % obtained by out-of-state residents Year Ref No.
Binswanger's Disease Wikipedia

"Alterations in glia and axons in the brains of Binswanger's disease patients" . Stroke . 28 (7): 1423–9. doi : 10.1161/01.str.28.7.1423 .

SDHAF1, NOTCH3, APOE, L2HGDH
- Binswanger's Disease Gard
  
  Binswanger's disease is a type of dementia caused by widespread, microscopic areas of damage to the deep layers of white matter in the brain. Most affected people experience progressive memory loss and deterioration of intellectual abilities (dementia); urinary urgency or incontinence; and an abnormally slow, unsteady gait (style of walking). While there is no cure, the progression of Binswanger's disease can be slowed with healthy lifestyle choices. Treatment is based on the signs and symptoms present in each person.
Inflammatory Breast Cancer Wikipedia

Breast Cancer Research and Treatment . 95 (3): 219–28. doi : 10.1007/s10549-005-9002-1 .

ALK, RHOC, EGFR, ESR1, ERBB2, TP53, PGR, CCN6, EGF, PIK3CA, XIAP, CD274, ERBB3, CAV1, MTCO2P12, NFKB1, PTGS2, COX2, CTNNB1, EZH2, NOTCH3, TNFSF10, PIK3CG, MYC, EIF4G1, STAT3, PIK3CB, PIK3CD, IL13, RIPK2, CD68, AHR, AKT1, APC, SDC1, MUC1, CXCL8, PTK2, PTEN, COL1A1, GLI1, VEGFA, IL10, FOXP3, INPP4B, ARHGEF7, GPRC5A, SLIT2, ADM, TP63, LGR5, TFF1, TGFA, THBD, TNF, TP73, SUMO1, UVRAG, VDR, VIM, WNT1, WNT5A, CXCL14, CXCR4, H3-4, IFITM1, SLC9A3R1, B3GAT1, APOBEC3B, TAS2R64P, MIR126, MIR150, MIR155, MIR15A, MIR181C, MIR19A, MIR205, MIR21, MIR26B, MIR30B, MIR335, MIR337, MIR451A, HOTAIR, MIR1303, MIR210HG, TMX2-CTNND1, MIR10B, ARHGAP24, PUM1, FTO, KIAA0100, HDAC6, SCGB1D2, NES, CKAP4, KCNQ1OT1, UBE2C, TJP3, AGO2, REM1, ASCC1, PRLH, NUSAP1, MED15, WWOX, KRT20, DGCR8, STAT6, PMAIP1, ST14, IDH2, CST6, CTNND1, CTSB, CTSV, CYP1B1, DHCR24, DLX4, ECT2, ERBB4, F2R, FGFR1, GLO1, GPX3, HAGH, HGF, CSF1R, CSF1, CPB2, BRCA2, AGT, ALDH1A1, AREG, BAX, BCL2, BRCA1, CD1A, COL10A1, MS4A1, CD40, CD44, CDK2, CCR7, COL5A1, HHEX, IL6, SIAH2, IL13RA1, PAK1, PDGFRA, PDGFRB, PARP1, CTSA, PPP3CA, PRKCZ, MAP2K7, PSEN2, RARRES1, RBM3, RHO, RPE65, S100A7, SELE, TNFRSF11B, NOTCH1, NFKB2, MARCKS, IL13RA2, IL18, KDR, KRT18, KRT81, LMNA, MCL1, MYB, MMP1, MMP2, MMP3, MMP11, MMP12, MUC4, H3P40
- Inflammatory Breast Cancer Mayo_clinic
  
  Overview Inflammatory breast cancer is a rare type of breast cancer that develops rapidly, making the affected breast red, swollen and tender. Inflammatory breast cancer occurs when cancer cells block the lymphatic vessels in skin covering the breast, causing the characteristic red, swollen appearance of the breast. Inflammatory breast cancer is considered a locally advanced cancer — meaning it has spread from its point of origin to nearby tissue and possibly to nearby lymph nodes. Inflammatory breast cancer can easily be confused with a breast infection, which is a much more common cause of breast redness and swelling. Seek medical attention promptly if you notice skin changes on your breast.
- Inflammatory Breast Cancer Gard
  
  Inflammatory breast cancer (IBC) is a rare and aggressive type of breast cancer in which the cancer cells block the lymph vessels in the skin of the breast. This type of breast cancer is called “inflammatory” because the breast often looks swollen and red, or “inflamed.” The skin may also look dimpled like the skin of an orange. IBC can be difficult to diagnose because there is no lump to feel or detect on a mammogram. It is crucial to identify IBC right away because early diagnosis and treatment can greatly improve the outcome. Patients are often given a combination of treatments, including chemotherapy, surgery, and radiation therapy.
Achilles Tendon Rupture Wikipedia

. ^ Khan-Farooqi W, Anderson RB (April 28, 2010). "Achilles tendon evaluation and repair" .
- Achilles Tendon Rupture Mayo_clinic
  
  Overview Achilles (uh-KILL-eez) tendon rupture is an injury that affects the back of your lower leg. It mainly occurs in people playing recreational sports, but it can happen to anyone. The Achilles tendon is a strong fibrous cord that connects the muscles in the back of your calf to your heel bone. If you overstretch your Achilles tendon, it can tear (rupture) completely or just partially. If your Achilles tendon ruptures, you might hear a pop, followed by an immediate sharp pain in the back of your ankle and lower leg that is likely to affect your ability to walk properly.
Pulmonary Fibrosis Wikipedia

. ^ "www.spirXpert.com" . Archived from the original on 28 January 2010. ^ King TE Jr; Bradford WZ; Castro-Bernardini S; et al.

TGFB1, CCN2, EDN1, IL1B, MMP9, NFE2L2, IL4, CCL2, IL13, TIMP1, AGT, CSF2, HPS1, FAM13A, DSP, AP3B1, ABCA3, FN1, HGF, TNF, IL6, HMGB1, TGFA, STAT3, IGF1, FGF2, CXCL8, MTOR, MMP2, SOD1, CCL11, CCR2, SERPINA1, SPP1, AREG, MIR326, ADIPOQ, HMOX1, STAT6, MIR30A, MECP2, EGF, COL3A1, MIR29C, CAT, SOD3, BMP7, FGF1, ELN, CEBPB, FGF7, CCL5, GREM1, CCL4, CCR3, PARP1, SMAD7, ACTA2, LAMB1, PDGFA, IL1RN, IL5, CSF3, MIR140, MIR125A, CYSLTR2, CEBPA, MIR26B, CMA1, FYN, MIR200C, IL12B, MIR122, MIR345, CALCA, SKIL, MIR10A, PDGFB, PTX3, SERPINE1, MIR101-1, CXCL2, MIR425, MIR378A, CCL3, CFD, EGFR, IL17A, PTGS2, AGER, COL1A1, ACE, PLAU, SMAD4, MMP1, SCGB1A1, IL1A, ELANE, CD36, TGFBR2, COL1A2, PDGFRA, CCL17, CCL22, ANXA1, HSP90AB1, CDH1, HABP2, STAT1, ICAM1, MFN2, CYSLTR1, TERT, B3GAT1, HSPD1, MUC5B, CCR4, BAD, VWF, NKX2-5, CCR8, SFTPC, MUC5AC, CAV1, HPS4, RTEL1, TERC, PARN, IRF5, SFTPA2, SFTPA1, FAM111B, HLA-DRB1, TINF2, DKC1, HLA-DPB1, CTLA4, CFTR, DCTN4, PRTN3, PRKCD, FASLG, FAS, ACTB, BTNL2, HIF1A, IL10, MRPS22, PIK3CD, PIK3CG, PIK3CB, PIK3CA, RNF168, SMAD2, NLRP3, STN1, SP110, BMP15, NHP2, HLA-DPA1, KIAA0319L, DPP9, RCBTB1, SMAD3, NOP10, NR5A1, NUP107, FSHR, THOC2, NOX4, PLEC, PSMC3IP, RASGRP1, ALMS1, ASAH1, POSTN, NKX2-1, CASP10, CLCA4, STX1A, CCR6, ATP11A, SMN2, SMN1, SPIDR, CTNNB1, PTPN22, MIR21, F2R, VEGFA, TP53, LOX, AKT1, GABPA, CXCR4, TLR4, FOSL2, PLG, COPD, ACE2, THY1, ANGPT1, TNC, SIRT3, MMRN1, GLI1, DECR1, BLM, LPAR1, CXCL12, VIM, CEL, FSTL1, LOXL2, SLC27A5, PARP9, PRKAB1, IL33, JAK2, PRKAA1, PRKAA2, TM7SF2, IFNG, MTCO2P12, SIRT1, SFTPD, COX2, LGALS3, MMP12, CCL18, MMP7, REN, S100A4, HSPA4, NR1I2, PTEN, MUC1, MIRLET7D, ZEB1, MIR34A, OGG1, ADAM17, MSC, VTN, CCN4, YY1, PPARG, SPHK1, SEMA7A, NT5E, DNM1L, SMUG1, TOP1, BRD4, SLC52A2, HSPB3, PINK1, TMED7, SPARC, PDGFRB, TGFB3, GDF15, PHEX, MAPK3, KLF4, HSP90AA1, DNER, MAPK14, MARK2, TMED7-TICAM2, F2RL1, TICAM2, BLMH, TSLP, GLB1, PWAR1, GSK3B, FOXO3, EGR1, CD44, DDIT3, DCN, DNMT1, ING4, MAPK1, ELK1, MAPK7, MAPK8, PSMD9, TLR2, LILRB1, PTK2, PTPN11, DCTN6, IL7, TSC1, CXCR6, FOLR2, PDCD1, LCLAT1, ZNRD2, FOXM1, WNT1, SLC52A1, PF4, ATF3, SSRP1, AHSA1, BDNF, STING1, UTRN, SIRT6, TXN, FASN, TWIST1, PTPRC, MIR145, HPGDS, MIR154, CD274, CST3, CHI3L1, NLRP1, CSF1R, CSF1, SLC2A1, CRYAB, CRMP1, SNAI1, CRK, SOAT1, MIR29A, SOD2, CREBBP, MIR29B1, MIR29B2, STAT4, CNR2, LTB4R, DAPK2, SDC2, SDC1, TGFBI, MOK, THBD, PRKN, METAP2, IL37, MIR155, MIR15A, MIR18A, DPP4, CX3CL1, SERPINH1, RIPK3, POLDIP2, RNF19A, TFF1, MIR200B, NUDT21, CDH11, FOS, BACH1, SOCS1, ANXA2, LGALS1, SQSTM1, JAG1, LOXL1, PERCC1, TNFSF14, HDAC4, MARCO, CTHRC1, BECN1, DENR, MIP, RBM45, HAS2, CXCL16, ANPEP, MMP13, ROCK2, LDHA, HSPB1, SETD7, S1PR2, IL9, MAPKAPK2, H3P23, CCN1, MAP1LC3B, IL18, IRAK1, HSPB2, KL, IGFBP3, GRAP2, MCU, IFI27, ITGB6, ADORA2B, LTBP4, ST2, MYD88, MPO, FST, GLI2, GPX4, P2RX7, ANXA5, TSPAN1, YAP1, CBLIF, AIMP2, GLRX, TFEB, GAS6, IL18BP, OSM, NTN1, MIR323A, RAPGEF3, MIR542, MIR1224, CHP1, TMPRSS11D, ABCG2, AIM2, GGPS1, DUSP10, TRIM16, MIR328, MIR96, LINC02605, KLF2, MIR34B, P2RX2, MIR31, MERTK, FBLN5, KAT5, CXCL13, ATG7, SLIT2, H3P11, TRIP10, MIR30D, P2RX5-TAX1BP3, ATG5, MIR541, RAMP2, ATP6AP2, MIR506, PPARGC1A, TNFSF13B, GAB2, MIR5100, MIR486-1, MIR454, MIR455, DNM3OS, CAPN9, FAM72A, NEU3, FAM72B, MIR627, HDAC6, SPATA2, RPL17-C18orf32, JTB, KHDRBS1, PLF, MIR448, PLXNC1, MIR4516, MIR449A, SIRT1-AS, CDR1-AS, PCLAF, ABCG1, H4C15, RGS6, LRPPRC, MIR503, CD226, TMX2-CTNND1, B3GAT3, ATG4B, ACKR3, TRPV4, GER, H4-16, SLCO6A1, ROMO1, TRIB3, PRX, MRTFA, RCN3, RMDN2, ASPRV1, KMT5AP1, PCBP4, TCIM, SULF1, SPHK2, RHOV, TMPRSS4, PARD3, PGAM5, MYDGF, SULF2, HDAC8, PAG1, IL26, MFN1, PRSS55, ZEB1-AS1, RXFP1, FKBP10, SCGB3A2, SMOC2, SPZ1, RETNLB, ING5, CRISPLD2, LOXL3, HAVCR2, CD276, ADAM33, WNT10A, ZC3H12A, GRHL2, NAF1, MMP28, ELOVL6, TRPM8, WNK1, CDCP1, IL25, MUC16, PRRT2, DEPTOR, NREP, SEMA4A, IFIH1, IL17F, UCN3, FBXO32, SYBU, EBF3, ELMOD2, ADGRE2, TBK1, SETD2, IL17B, BBC3, LATS2, FGF21, KISS1R, PHGDH, MIR185, PART1, MIR193A, MIR19A, MIR19B1, MIR205, MIR210, PRDX5, NUP62, MIR221, DDAH1, PIGN, MIR27A, TRAM1, MIR27B, CBX5, HEY1, PPP1R13B, MIR301A, MIR146A, DELEC1, RMDN3, MIR144, SARS2, EGLN1, ROBO4, NPNT, IFNL3, POLE3, LAMA1, PWAR4, GSTK1, SIRT7, GTSE1, MALAT1, FENDRR, SNX9, CSAD, CHST15, CRNKL1, TNFRSF12A, MIR126, MIR130A, MIR130B, MIR139, RMDN1, ADIPOR1, MIR141, MIR142, FOXP3, GORASP1, SFRP4, CRLF1, GRP, FUT8, GAB1, GATA3, GLS, CCR10, CXCR3, GPT, GTF2H1, HPGD, HDAC2, CFHR1, NRG1, HLA-A, HLA-B, HLA-C, HLF, FOSB, FLT3LG, FLT3, FLT1, ESR1, ETS2, F2, F2RL2, F3, F10, FAP, FCGR3A, FCGR3B, FGF13, FGFR2, FGL1, VEGFD, FOXF1, FOXD1, NR4A1, HSPA1A, ERN1, JUNB, ITGAE, ITGAX, ITGB3, EIF6, IVD, JAK1, JUN, JUND, HSPA1B, KCNMB1, LEP, LMNA, LRP6, LTBR, LUM, MARCKS, ITGA9, ISG20, ITGA6, INPP5D, HTR2A, ID1, IFNB1, IGF2, IGFBP2, IGFBP5, IL2, IL2RA, IL4R, IL6ST, IL7R, IL11, IL11RA, IL15, TNFRSF9, FBL, ERBB3, MEN1, CAST, KLF9, TSPO, C3, C3AR1, C5AR1, VPS51, DDR1, CASP1, CDKN2A, RUNX2, RUNX3, CBS, CD28, CD59, ADGRE5, CD151, BSG, BMPR2, BMP3, BGN, ADA, ADAM10, ADM, AEBP1, AGTR1, AIF1, AKT2, ALB, ANGPT2, ANXA11, APOA1, APRT, ARG1, BARD1, BCL2, CDH5, CDKN2B, ERBB2, E2F4, CYP27B1, DES, NQO1, DIO2, DNAH8, ARID3A, E2F1, ECE1, CHAT, ECT2, S1PR3, EFNB2, EPHA2, EIF4E, EP300, STX2, CYP2E1, CYLD, CX3CR1, CTSK, CHIT1, CHRM3, CHRNA4, CLU, ACKR2, CNR1, COL11A2, COX8A, CREB1, ATF2, CRIP1, CRYZ, CSNK1D, CSRP1, CTNND1, MCAM, MFAP1, XPR1, TNFRSF1A, TGFB2, TGFBR1, THAS, THBS1, TIAM1, TIMP3, TLR3, TNNC1, WT1, TPH1, CRISP2, TRPC6, TSC2, TNFSF4, VCAM1, VDR, TMBIM6, PPP1R11, TRBV20OR9-2, TAZ, SHH, SIX1, SKI, SKP2, SNAI2, SNCA, SOX2, SPINT1, SRC, SREBF1, SRF, STC1, STK11, SYT1, TAGLN, TRPV1, XIST, SFRP1, MBD2, AOC3, EIF3A, MBTPS1, TNFSF10, CCN6, CCN5, SGPL1, TRPA1, FOSL1, F2RL3, TM4SF5, SYT7, P2RX6, ATG12, LPAR2, IL1RL1, BHLHE40, ENC1, RASAL1, ULK1, HMGA2, H3-4, H4C9, FZD7, H4C1, H4C4, H4C6, H4C12, H4C11, H4C3, H4C8, H4C2, H4C5, H4C13, H4C14, ACO2, SELPLG, MID1, PAWR, P2RX3, P2RX4, P2RX5, P2RY1, P2RY2, P4HB, FURIN, PCNA, PIP, PDE1A, PDK1, PECAM1, ATP8B1, ABCB1, PHB, SERPINE2, P2RX1, DDR2, NTF3, NOTCH4, MAP3K11, MMP3, MMP10, MMP14, MMP19, MPG, MRC1, MSR1, MST1, NEDD8, NEU1, NFKB1, NINJ1, NM, NOTCH1, PIN1, PLA2G4A, SELE, ROCK1, RASA1, RBP2, OPN1LW, RELA, RGS2, BRD2, RNH1, ROS1, PLAUR, RPL17, S100A6, S100A9, SARS1, SERPINB3, CCL24, SDC4, RARRES2, RAG2, RAF1, RAC2, PLK1, POU2AF1, PPL, PRH1, PRH2, PRKCA, PRKCB, PRKDC, EIF2AK2, PTCH1, PTGER4, PTHLH, PTPN13, PTPRJ, RAC1, H3P10
- Pulmonary Fibrosis Mayo_clinic
  
  Overview Pulmonary fibrosis is a lung disease that occurs when lung tissue becomes damaged and scarred. This thickened, stiff tissue makes it more difficult for your lungs to work properly. As pulmonary fibrosis worsens, you become progressively more short of breath. The scarring associated with pulmonary fibrosis can be caused by a multitude of factors. But in most cases, doctors can't pinpoint what's causing the problem.
Anemia In Pregnancy Wikipedia

Transfusion Medicine (Oxford, England) . 28 (2): 107–116. doi : 10.1111/tme.12532 .

G6PD, WDHD1
Central Pontine Myelinolysis Wikipedia

Imaging by MRI typically demonstrates areas of hyperintensity on T2-weighted images. [ citation needed ] Treatment [ edit ] To minimise the risk of this condition developing from its most common cause, overly rapid reversal of hyponatremia, the hyponatremia should be corrected at a rate not exceeding 10 mmol/L/24 h or 0.5 mEq/L/h; or 18 mEq/L/48hrs; thus avoiding demyelination. [27] No large clinical trials have been performed to examine the efficacy of therapeutic re-lowering of serum sodium, or other interventions sometimes advocated such as steroids or plasma exchange. [27] Alcoholic patients should receive vitamin supplementation and a formal evaluation of their nutritional status. [28] [29] Once osmotic demyelination has begun, there is no cure or specific treatment.
Salicylate Poisoning Wikipedia

.; Rutka, John A. (2004). Ototoxicity . PMPH-USA. p. 28. ISBN 9781550092639 . Archived from the original on 10 September 2017 .
Hiatal Hernia Wikipedia

PubMed Health . Archived from the original on 28 April 2017 . Retrieved 6 May 2017 . ^ Chang SW, Lee HC, Yeung CY, Chan WT, Hsu CH, Kao HA, Hung HY, Chang JH, Sheu JC, Wang NL (2010).

ATP7A, COL1A1, GPHN, WDR4, AFG3L2, SPECC1L, NIPBL, TPRKB, OSGEP, NUP133, NUP107, PORCN, SLC2A10, TUBB6, ATAD1, WDR73, TP53RK, ADAMTS2, SLC6A5, LAGE3, PTCH1, COL5A1, COL5A2, TNXB, GLRB, GLRA1, ALDH18A1, SMARCB1, TCF4, TGFB3, CHST14, IL12B, HLA-DMA, GER, FUT3, ECI1, ADGRV1, CYP2C19, COL3A1
- Hiatal Hernia Mayo_clinic
  
  Overview A hiatal hernia occurs when the upper part of your stomach bulges through the large muscle separating your abdomen and chest (diaphragm). Your diaphragm has a small opening (hiatus) through which your food tube (esophagus) passes before connecting to your stomach. In a hiatal hernia, the stomach pushes up through that opening and into your chest. A small hiatal hernia usually doesn't cause problems. You may never know you have one unless your doctor discovers it when checking for another condition. But a large hiatal hernia can allow food and acid to back up into your esophagus, leading to heartburn.
- Hernia, Hiatus Omim
  
  Goodman et al. (1969) observed 6 affected persons in 2 generations. Five of the 6 were female. This disorder is sometimes called congenital short esophagus (Myles, 1939) or partial thoracic stomach. Carre and Froggatt (1970) described 8 definite cases in 3 successive generations of a family. Others were equivocally affected. Sidd et al. (1966) observed a sliding hiatal hernia in 4 brothers, aged 42 to 44 years, 2 of whom were monozygotic twins. Carre et al. (1999) described a 5-generation family in which 23 of 38 individuals had a radiologically proven hiatus hernia.
Reactive Hypoglycemia Wikipedia

It might be an " adrenergic postprandial syndrome" — blood glucose levels are normal, but the symptoms are caused through autonomic adrenergic counterregulation. [28] Often, this syndrome is associated with emotional distress and anxious behaviour of the patient. [13] This is often seen in dysautonomic disorders as well.

TNF, HNF1A, SOD2, PPARA, GSR, IGF2, IL1B, INS, SERPINA1, CACNA1C, ALDOB, PCSK1, MEN1, GLUD1, GCG, GLP1R, EHMT1, ZGLP1, INSR, SLC5A2, CRIP1, FGF19, ZC4H2
Agrammatism Wikipedia

"Linguistic complexity and frequency in agrammatic speech production" (PDF) . Brain and Language . 109 : 18–28. doi : 10.1016/j.bandl.2008.12.004 .
Brainstem Death Wikipedia

No testing of testable brain stem functions such as oesophageal and cardiovascular regulation is specified in the UK Code of Practice for the diagnosis of death on neurological grounds. There is published evidence [28] [29] [30] strongly suggestive of the persistence of brainstem blood pressure control in organ donors .
Reduced Affect Display Wikipedia

They seem to lack feelings altogether, although this may actually be because of their inability to express emotion rather than from an absence of emotion altogether". [28] Alexithymic patients however can provide clues via assessment presentation which may be indicative of emotional arousal . [29] "If the amygdala is severed from the rest of the brain, the result is a striking inability to gauge the emotional significance of events; this condition is sometimes called 'affective blindness'". [30] In some cases, blunted affect can fade, but there is no conclusive evidence of why this can occur.
Cataplexy Wikipedia

"Emerging Therapies in Narcolepsy-Cataplexy" . Sleep . 28 (6): 754–763. doi : 10.1093/sleep/28.6.754 .

HCRT, HLA-DQB1, HLA-DRB1, P2RY11, KCNMA1, REM1, ZNF365, NPC2, TNFSF4, TBCD, NPC1, MOG, KCNMA1-AS1, CTSH, DNMT1, GNAO1, HLA-DQB2, RBM45, TAAR1, PSG5, HRH3, KCNA1, UBXN2B, TRIB2, SLC17A5, MCHR1, UGCG, LAMC2, TG, TEAD4, HLA-DQA1, SNAP25, CSF2, HLA-DRB5, ATXN3, CHAT
- Narcolepsy Medlineplus
  
  Narcolepsy is a chronic sleep disorder that disrupts the normal sleep-wake cycle. Although this condition can appear at any age, it most often begins in adolescence. Narcolepsy is characterized by excessive daytime sleepiness. Affected individuals feel tired during the day, and several times a day they may experience an overwhelming urge to sleep. "Sleep attacks" can occur at unusual times, such as during a meal or in the middle of a conversation. They last from a few seconds to a few minutes and often lead to a longer nap, after which affected individuals wake up feeling refreshed.
Blepharitis Wikipedia

In this study, researchers provide a diagnosis of the disease and propose diagnostic criteria of Demodex blepharitis. [28] References [ edit ] ^ a b c d Emmett T.

APOE, UROS, WIPF1, XPA, XPC, SMC1A, TP63, SMC3, TBX4, TRAF3IP2, GJB6, PLXND1, PIGN, NIPBL, TINF2, MBTPS2, RTEL1, WRAP53, SETD5, NOP10, SLC39A4, NHP2, HDAC8, USB1, CTC1, WAS, TERT, MMP1, ERCC2, ERCC4, ERCC5, GATA1, GNAQ, DKC1, KMT2A, TERC, DDB2, CST6, PARN, PKP1, PLCD1, RAD21, REV3L, MSMO1, COL7A1, ST14, STAT1, ADAM17, ERCC3, LTB4R, IL4, MMP9, PSIP1, CX3CL1, LACRT
- Blepharitis Mayo_clinic
  
  Overview Blepharitis (blef-uh-RYE-tis) is inflammation of the eyelids. Blepharitis usually affects both eyes along the edges of the eyelids. Blepharitis commonly occurs when tiny oil glands near the base of the eyelashes become clogged, causing irritation and redness. Several diseases and conditions can cause blepharitis. Blepharitis is often a chronic condition that's difficult to treat. Blepharitis can be uncomfortable and unsightly. But it usually doesn't cause permanent damage to your eyesight, and it's not contagious.
Focal Segmental Glomerulosclerosis Wikipedia

These include: NPHS1 , which encodes the protein nephrin that contributes to the filtration barrier; [25] NPHS2 , which encodes the protein podocin found in podocytes; [26] and INF2 , which encodes the actin-binding protein formin . [27] Diagnosis [ edit ] Diagnosis of FSGS is made by renal biopsy that includes at least 15 serial cuts with at least 8 glomeruli. [28] [29] Histologic features include sclerosis (scarring) of a portion (average: 15%) of the glomerular space, with only a portion of glomeruli manifesting any sclerosis. [30] Other tests helpful in the diagnosis include urine protein, urinalysis, serum albumin, and serum lipids. [2] A clinical picture of proteinuria, low blood protein levels (albumin, antibodies), and high blood cholesterol would support a diagnosis of FSGS, although these do not help to distinguish between FSGS and other causes of proteinuria . [5] [9] Classification [ edit ] Micrograph of the collapsing variant of FSGS (collapsing glomerulopathy).

TRPC6, INF2, AGT, NPHS2, ACTN4, CD2AP, APOL1, SERPINE1, PAX2, CRB2, MYO1E, ANLN, MYH9, SGPL1, NPHS1, SYNPO, TGFB1, EDN1, ZMPSTE24, COL4A5, NXF5, LMX1B, ARHGAP24, CCN2, LMNA, MPV17, NOS2, PCNA, FN1, E2F3, ACTA2, GNAQ, HAVCR1, SPP1, MYH10, COL4A1, AGTR1, MMP9, MMP2, LIPC, AGTR2, CASP9, ANGPT2, VLDLR, LPL, ACTR3, PIAS1, WT1, REN, PLCE1, SMARCAL1, COQ6, NUP107, PTPRO, TBC1D8B, ITGA3, COQ8B, SCARB2, CLCNKB, NARS2, NUP160, NUP205, WDR73, SLC12A3, NUP133, COL4A4, NUP93, ACTB, SEC61A1, VPS33A, CLCN5, IGAN1, TRIM8, G6PC, SLC37A4, ACE, NUP85, COL4A3, CD44, VEGFA, TNF, TRPC5, CCL2, POMC, PODXL, TBPL1, TYRP1, ALB, RAC1, NFE2L2, BAX, CAMK4, CCR2, APOE, KRT20, MAPK1, MS4A1, PON1, PLG, CD80, TLR4, MAPK3, IL10, MTOR, MIR193A, CYP11B2, LAMB2, HLA-A, IL1A, IL1B, UBD, HPSE, C1QL1, NES, CHP1, GDF15, POLDIP2, MAFB, AHSA1, SIRT1, YAP1, RAPGEF5, BMS1, RNF19A, PLA2R1, MLYCD, DDN, KEAP1, PTPRU, MMRN1, SERPINA3, SMPDL3B, SIRPA, CNKSR3, RHOV, SDK1, THSD7A, NPNT, NPHP4, LINC01193, MIR106A, MIR150, MIR155, MIR19B1, MIR200C, MIR30A, MIR34C, HNP1, MIR451A, MIR490, MIR663A, KTWS, MIR1225, MIR1915, PLB1, HT, IGKV3-7, PLEKHH2, IL22, DERL2, ATL1, ZDHHC2, WT1-AS, SNX9, NBAS, ADA2, KIRREL1, FBXW7, PLXNA3, RPL23, PDSS2, TMEM63C, VANGL2, RBPJP4, PDLIM2, HHIP, TTC21B, ALG13, STRIP1, GRAP2, CCL19, KLF4, CFH, DMPK, ECT2, EGF, ENPEP, EPHB2, EYA1, F2RL1, GABPA, GH1, CXCL1, HLA-DQA1, MAGI1, HMOX1, HP, HTC2, IL1R1, IL6, IL18, ILK, ITGAE, ITGB1, LAMA5, CTLA4, VCAN, CSF2, MAPK14, ANK3, FASLG, B2M, BAK1, BCL2, BCL2L1, BSG, C3AR1, CALB2, CD9, CD40, CD40LG, CDC42, COL1A1, COL8A1, COL8A2, KLF6, COX10, CP, CRH, CRK, LAMC2, LCN2, LPA, ACACA, SLC5A2, SLC12A1, SNRPB, TAGLN, HNF1B, TGFBR2, TIMP1, TLR2, TYRO3, UBA52, KDM6A, VASP, YWHAZ, PAX8, CXCR4, MANF, AIMP2, CUBN, CASK, NRP2, PDLIM1, SELP, SCN7A, SMAD7, S100A4, MMP14, MTHFR, TRNL1, MUC1, MYH1, NAGLU, RPL10A, NEFH, NOS1, NOTCH1, NPHP1, PKD1, PKD2, PLA2G1B, PLAU, PLCG1, PPARG, PTPRC, RAP1GAP, RARA, RPL17, LOC105374325
- Focal Segmental Glomerulosclerosis (Fsgs) Mayo_clinic
  
  Overview Focal segmental glomerulosclerosis (FSGS) is a disease in which scar tissue develops on the glomeruli, the small parts of the kidneys that filter waste from the blood. FSGS can be caused by a variety of conditions. FSGS is a serious condition that can lead to kidney failure, which can only be treated with dialysis or kidney transplant. Treatment options for FSGS depend on the type you have. Types of FSGS include: Primary FSGS . Many people diagnosed with FSGS have no known cause for their condition. This is called primary (idiopathic) FSGS . Secondary FSGS . Several factors, such as infection, drug toxicity, diseases including diabetes or sickle cell disease, obesity, and even other kidney diseases can cause secondary FSGS .
- Focal Segmental Glomerulosclerosis Gard
  
  Focal segmental glomerulosclerosis (FSGS) is a type of kidney disorder. It is characterized by scar tissue that forms in some of the glomeruli in the kidney. FSGS may cause non-specific signs and symptoms, including protein in the urine, elevated levels of creatinine , and swelling. In many cases the cause of FSGS can not be determined. Some cases are thought to be associated with congenital kidney defects, urine backing up into the kidneys, obesity, obstructive sleep apnea , sickle cell anemia , or viruses (e.g., HIV ). The goal of treatment is to control symptoms and prevent chronic kidney failure .
Abortion In Virginia Wikipedia

That year, 78% of women in the state aged 15 – 44 lived in a county without an abortion clinic. [24] In 2017, there were five Planned Parenthood clinics in a state with a population of 1,971,590 women aged 15 – 49 of which four offered abortion services. [25] Statistics [ edit ] In the period between 1972 and 1974, the state had an illegal abortion mortality rate per million women aged 15 – 44 of between 0.1 and 0.9. [26] In 1990, 745,000 women in the state faced the risk of an unintended pregnancy. [22] In 2010, the state had two federally funded abortions. [27] In 2013, among white women aged 15–19, there were abortions 1090, 1280 abortions for black women aged 15–19, 250 abortions for Hispanic women aged 15–19, and 190 abortions for women of all other races. [28] In 2014, 55% of adults said in a poll by the Pew Research Center that abortion should be legal in all or most cases. [29] In 2017, the state had an infant mortality rate of 5.9 deaths per 1,000 live births. [9] Number of reported abortions, abortion rate and percentage change in rate by geographic region and state in 1992, 1995 and 1996 [30] Census division and state Number Rate % change 1992–1996 1992 1995 1996 1992 1995 1996 South Atlantic 269,200 261,990 263,600 25.9 24.6 24.7 –5 Delaware 5,730 5,790 4,090 35.2 34.4 24.1 –32 District of Columbia 21,320 21,090 20,790 138.4 151.7 154.5 12 Florida 84,680 87,500 94,050 30 30 32 7 Georgia 39,680 36,940 37,320 24 21.2 21.1 –12 Maryland 31,260 30,520 31,310 26.4 25.6 26.3 0 North Carolina 36,180 34,600 33,550 22.4 21 20.2 –10 South Carolina 12,190 11,020 9,940 14.2 12.9 11.6 –19 Virginia 35,020 31,480 29,940 22.7 20 18.9 –16 West Virginia 3,140 3,050 2,610 7.7 7.6 6.6 –14 Number, rate, and ratio of reported abortions, by reporting area of residence and occurrence and by percentage of abortions obtained by out-of-state residents, US CDC estimates Location Residence Occurrence % obtained by out-of-state residents Year Ref No.
Lactic Acidosis Wikipedia

Both L and D isomers of lactic acid are produced in the rumen; [21] these isomers are metabolized by different metabolic pathways, and activity of the principal enzyme involved in metabolism of the D isomer declines greatly with lower pH, tending to result in an increased ratio of D:L isomers as acidosis progresses. [25] Measures for preventing lactic acidosis in ruminants include avoidance of excessive amounts of grain in the diet, and gradual introduction of grain over a period of several days, to develop a rumen population capable of safely dealing with a relatively high grain intake. [21] [22] [23] Administration of lasalocid or monensin in feed can reduce risk of lactic acidosis in ruminants, [27] inhibiting most of the lactate-producing bacterial species without inhibiting the major lactate fermenters. [28] Also, using a higher feeding frequency to provide the daily grain ration can allow higher grain intake without reducing the pH of the rumen fluid. [29] Treatment of lactic acidosis in ruminants may involve intravenous administration of dilute sodium bicarbonate, oral administration of magnesium hydroxide, and/or repeated removal of rumen fluids and replacement with water (followed by reinoculation with rumen organisms, if necessary). [21] [22] [23] References [ edit ] ^ Woods, Hubert Frank; Cohen, Robert (1976).

PDHA1, TRNL1, DNM1L, RRM2B, ND6, ATAD3A, PLAT, CYTB, ACAD9, MTO1, PDP1, POLG, BCS1L, PC, ISCU, COX1, ND1, ATP5F1E, SCO2, RMND1, TMEM70, COQ9, ND4, KARS1, FBXL4, TRMT10C, NDUFB11, LIPT1, MRPS14, NDUFS4, SLC25A3, EXOSC9, WARS2, SUCLA2, ELAC2, SURF1, TUFM, HADHA, IBA57, SLC37A4, DLD, EARS2, NDUFAF3, MICOS13, NDUFA11, NDUFAF6, NAXE, MLYCD, LARS2, FASTKD2, SFXN4, TANGO2, USP18, TPK1, ETHE1, FARS2, LIAS, NFU1, SLC25A42, NDUFS7, LIPT2, SLC25A13, LRPPRC, TSFM, COA6, BOLA3, PREPL, UQCC3, SUCLG1, PDHX, UQCRFS1, COQ2, MRPS34, COX20, SLC25A19, NDUFAF5, AARS2, LYRM4, COQ8A, TMEM126B, CAMKMT, AGK, TRMU, NUBPL, PUS1, FOXRED1, COA8, TK2, GTPBP3, SERAC1, COX14, LYRM7, ATPAF2, MPC1, NDUFAF2, LARS1, TIMMDC1, TACO1, NDUFAF1, MRPS7, YARS2, MRPS16, PNPLA8, TIMM50, NDUFAF4, PET100, TRNN, TRNS1, NDUFS2, NDUFS1, NDUFB10, NDUFB9, NDUFB3, NDUFA10, NDUFA6, GFER, NDUFA1, TRNW, TRNV, TRNT, TRNS2, TRNQ, NDUFS3, HSD17B10, HADHB, TRNK, TRNH, TRNF, ND5, ND3, HADH, ND2, COX3, COX2, TRNC, MPV17, G6PC, NDUFV1, CYC1, NDUFS6, SLC25A4, ALDOB, ATP5F1D, BCKDHA, SLC3A1, BCKDHB, CA5A, CHAT, COX6B1, SDHA, SCO1, COX8A, COX10, COX15, MIPEP, DBT, PPM1B, DGUOK, PHKG2, DLAT, PHKA2, PDHB, PCK1, PCCB, PCCA, TYMP, FH, NDUFV2, NDUFS8, HSPA5, MB, TFAM, TXNIP, VARS2, CA2, PTGS1, RPS6KA3, ABCB6, MGAM, SRSF2, SI, MEHMO, MAP2K7, SLC5A2, UQCRB, ALDH7A1, ATF4, AQP9, LINC01194, TTR, PTBP1, ARRDC4, MET, GSTZ1, IL10, IL6, MRPS22, SLC47A1, TNF, ZDHHC13, NDUFA5, RNPS1, UQCC2, UQCRQ, OPA1, FBP1, ECHS1, TRS-AGA2-3, ALB
Dysphagia Wikipedia

Journal of Neurology, Neurosurgery, and Psychiatry . 75 Suppl 3: iii22–28. doi : 10.1136/jnnp.2004.045906 .

MEGF10, TSEN2, TSEN54, TSEN34, KIT, ATXN3, MATR3, ATXN1, PANK2, TWNK, SLC52A2, PSEN1, TP63, DYSF, AR, DNAJB6, ATXN2, ATXN8OS, SCN4A, PABPN1, CACNA1A, SLC9A6, KLHL41, TUBB4A, NOP56, SON, IKZF1, STUB1, HUWE1, DNM1L, SCO2, KMT2B, SEMA3E, SNCAIP, OPTN, ERLIN2, NPC2, AFG3L2, PIK3R5, KAT6B, MACF1, TARDBP, ATP13A2, SPECC1L, DNAJC13, AGTPBP1, DDHD2, VPS13A, PLXND1, SPART, SETX, DKK1, PUF60, POLG2, POLR3A, MYOT, CACNA1G, MED17, SURF1, TPM3, TPM2, TOP3A, TK2, TBP, TBCD, VAMP1, SPG7, VARS1, SOX4, ACOX1, SNCA, SNAP25, SLC25A1, SLC18A3, SLC6A9, UBTF, VCP, CYP7B1, SYNJ1, PEX16, NRXN1, PLAA, TRIP4, PIGQ, NUP62, SQSTM1, PDE8B, WFS1, PRKRA, KCNAB2, CNTNAP1, PLA2G6, COLQ, SMC1A, XRCC1, PIGN, CHMP2B, FBXO7, PYROXD1, REPS1, LINGO1, TUBB6, C19orf12, SLC19A3, FLAD1, SPG11, KIAA0319L, SLC25A22, MGME1, RHBDF2, CARS2, CDC73, FA2H, REEP1, IRF2BPL, PRDM16, SLC5A7, NDUFAF2, SLC52A3, ATXN10, RNASEH1, CHCHD10, MYMK, AGRN, KY, CAVIN1, KANSL1, SYT14, EBF3, C9orf72, LRRK2, ARX, KCTD7, SIK1, CARMIL2, TTBK2, HGSNAT, KLHL40, SYT2, GBA2, ALS2, ARID1B, TBK1, YARS2, ASCC1, GEMIN4, RRM2B, UBQLN2, LRP12, GMPPA, ANKRD11, SACS, MYORG, FBXL4, TOR1AIP1, GIGYF2, CNTNAP2, SETBP1, SDHD, PNKD, NDUFAF3, MECR, TRAPPC12, COQ4, RLIM, SELENON, MFF, LMOD3, KLHL7, VPS11, TBC1D23, VPS35, POLR3B, VAC14, CHD7, FERMT1, NCAPG2, GDAP2, PDP1, MAGEL2, SPG21, KCNK9, SKI, ATXN8, KCNC3, KCND3, ITGB4, CACNA1C, IRF6, IRF5, CAV1, IDH2, IDH1, HPRT1, HOXB1, HPCA, HLA-DRB1, HLA-B, HTT, H3-3A, GUCY1A1, SDHC, KIF5A, CHAT, LAMA2, ATP6, MRE11, MPZ, MMP1, KMT2A, MID1, MECP2, MCL1, MAPT, BRAF, LMNB1, LIFR, LBR, SERPING1, LAMB2, SCARB2, GRM1, ND2, EPRS1, CHRNE, ECM1, TYMP, ATN1, CLCN1, CCR6, DYNC1H1, DMPK, COL7A1, DGUOK, TIMM8A, COL13A1, CYP27A1, CTNS, CCN2, EIF4G1, FMR1, GRIN2D, FXN, GRIN2B, GNS, GNAQ, GNAO1, GLUD2, GJB1, GFPT1, GCH1, CHN1, CHRNA1, GBA, GABRD, CHRND, FUS, FTL, ND1, MSX1, ND3, OPA1, ADH1C, PRNP, MAP2K2, PRKCG, POLG, SLC25A4, EXOSC9, PLP1, PLEC, PIGA, PFN1, APP, PDGFRA, ND4, ASPA, PRPS1, PSAP, ADD3, ATXN7, SDHB, ACTA1, SDHA, SCN8A, ACTB, SCN3A, RYR1, PTCH1, REV3L, ACTG2, ADAR, QDPR, NECTIN1, PTS, RERE, PCNA, NR4A2, NDUFA9, ATP7B, ND5, ND6, TRNK, TRNL1, TRNV, TRNW, ATP7A, MYH7, MYH8, MYO9A, NDUFA6, ATP1A3, NEB, CRYAB, NDUFS3, NDUFS1, NPC1, NF1, NEUROD2, NEK1, NDUFS2, NDUFB8, SOD1, BDNF, TAC1, CRP, ALB, MORC3, NPNT, ATP4A, ATP12A, COPD, IGFALS, BMP2, ARSA, CRYGD, ASXL1, UCN2, MALAT1, APOE, CA3, IS1, OTULIN, SGCA, CSF2, NBN, NT5E, PAFAH1B1, CDK13, PAX9, ELP1, SRPX, EPX, ZP3, YWHAE, PNN, TRI-AAT9-1, TRNAG1, TPO, PSMA7, RAD51, TRIM21, RPS20, SLN, SLC10A1, PCYT1B, SAE1, CTBS, CCL26, ECI1, DMD, DPP4, MRS2, EGF, FUT3, GCG, TET2, GSS, GSTP1, IL5, PART1, KRAS, TNFRSF13B, SF3B1, LAMC2, LY6E, MMP8, KDELR2, ACR
- Dysphagia Mayo_clinic
  
  Overview Dysphagia is difficulty swallowing — taking more time and effort to move food or liquid from your mouth to your stomach. Dysphagia can be painful. In some cases, swallowing is impossible. Occasional difficulty swallowing, such as when you eat too fast or don't chew your food well enough, usually isn't cause for concern. But persistent dysphagia can be a serious medical condition requiring treatment. Dysphagia can occur at any age, but it's more common in older adults. The causes of swallowing problems vary, and treatment depends on the cause.
Neurofibromatosis Wikipedia

However, radiotherapy is not recommended in children who present with this disorder. [28] It is recommended that children diagnosed with NF1 at an early age have an examination each year, which allows any potential growths or changes related to the disorder to be monitored. [29] Prognosis [ edit ] In most cases, symptoms of NF1 are mild, and individuals live normal and productive lives.

NF1, NF2
- Neurofibromatosis, Type Iv, Of Riccardi Omim
  
  Riccardi (1982) described cases of neurofibromatosis that are sufficiently variant that they seem to warrant separation from the classic von Recklinghausen NF I (162200), the acoustic neuroma type, NF II (101000), and the mixed type, NF III (162260). The group still is undoubtedly heterogeneous. Iris Lisch nodules, one of the most specific features of NF I, are usually absent in NF IV. The importance of a separate category for these cases is related to the probable difference in prognosis and genetic counseling and the desirability of avoiding confusion of studies of the natural history and pathogenesis of NF I. Eyes - Iris Lisch nodules usually absent Inheritance - Autosomal dominant - heterogeneous Skin - Atypical neurofibromatosis ▲ Close