Dopamine Beta-Hydroxylase Deficiency
Summary
Clinical characteristics.
Dopamine beta-hydroxylase (DBH) deficiency is characterized by lack of sympathetic noradrenergic function but normal parasympathetic and sympathetic cholinergic function. Affected individuals exhibit profound deficits in autonomic regulation of cardiovascular function that predispose to orthostatic hypotension. Although DBH deficiency appears to be present from birth, the diagnosis is not generally recognized until late childhood. The combination of ptosis of the eyelids in infants and children, together with hypotension, is suggestive of the disease. In the perinatal period, DBH deficiency has been complicated by vomiting, dehydration, hypotension, hypothermia, and hypoglycemia requiring repeated hospitalization; children have reduced exercise capacity. By early adulthood, individuals have profound orthostatic hypotension, greatly reduced exercise tolerance, ptosis of the eyelids, and nasal stuffiness. Presyncopal symptoms include dizziness, blurred vision, dyspnea, nuchal discomfort, and chest pain; symptoms may worsen in hot environments or after heavy meals or alcohol ingestion. Life expectancy is unknown, but some affected individuals have lived beyond age 60 years.
Diagnosis/testing.
The diagnosis of DBH is established in a proband with profound neurogenic orthostatic hypotension, minimal or absent plasma concentrations of norepinephrine and epinephrine, and a five- to tenfold elevation of plasma dopamine; it is confirmed with identification of biallelic pathogenic variants in DBH by molecular genetic testing.
Management.
Treatment of manifestations: Administration of L-threo-3,4-dihydroxyphenylserine (droxidopa) restores norepinephrine and alleviates the orthostatic hypotension and other symptoms. Affected individuals do not respond as well to standard therapeutic approaches for autonomic failure. Surgery can correct ptosis.
Surveillance: Renal function (measurement of plasma creatinine and BUN concentrations) is assessed every two years or more often if loss of renal function is evident; plasma magnesium and potassium should also be assessed. Yearly evaluation of efficacy of droxidopa against orthostatic hypotension as dosage adjustment may be required. Consultation with autonomic specialist prior to surgery or becoming pregnant.
Agents/circumstances to avoid: Untreated individuals should avoid hot environments, strenuous exercise, standing motionless, and dehydration.
Pregnancy management: Routine blood pressure monitoring during pregnancy and delivery, with adjustment of droxidopa dosage as needed; extra doses of droxidopa may be required during delivery and dose adjustment may be required post partum.
Genetic counseling.
DBH deficiency is inherited in an autosomal recessive manner. At conception, each sib of an affected individual has a 25% chance of being affected, a 50% chance of being an asymptomatic carrier, and a 25% chance of being unaffected and not a carrier. Carrier testing for at-risk relatives is possible if both pathogenic variants in the family are known. Once the DBH pathogenic variants have been identified in an affected family member, prenatal testing for a pregnancy at increased risk and preimplantation genetic diagnosis for DBH deficiency are possible.
Diagnosis
Individuals with dopamine beta-hydroxylase (DBH) deficiency are often first encountered during adolescence, complaining of lifelong difficulties with lightheadedness and fatigue and an inability to tolerate standing or exercise. Affected individuals and their parents will report behaviors (e.g., squatting) used to compensate for the problems with standing.
Suggestive Findings
No formal testing strategy has been presented for DBH deficiency; a clinical assessment including orthostatic vital signs and an ophthalmic exam should be the initial step and, if indicated, this should be followed by autonomic function testing and plasma catecholamine analysis.
DBH deficiency should be suspected in individuals with the following clinical, physiologic, and laboratory findings [Vincent & Robertson 2002, Timmers et al 2004]:
Clinical Findings
- Poor cardiovascular regulation evident from supine, seated, and standing vital signs:
- A low-to-normal supine blood pressure and low or normal supine heart rate
- Severely symptomatic orthostatic hypotension with systolic blood pressure falling below 80 mm Hg in the upright position
- A compensatory rise in heart rate with standing
- Inability to stand motionless for more than a few minutes
- Cardiovascular findings consistent with sympathetic failure but preserved parasympathetic function
- Other autonomic dysfunction evident from an ophthalmic examination:
- Ptosis in some individuals
- A marked decrease in intraocular pressure with standing [Phillips et al 2013]
- Somewhat small pupils that respond to light and accommodation but not to hydroxyamphetamine. Parasympatholytics dilate the pupils appropriately.
- A comprehensive history and physical examination (including neurologic exam) that typically reveal the following:
- Intact sweating consistent with intact sympathetic cholinergic function
- Skeletal and muscle findings in some affected individuals:
- Arched palate
- Hyperextensible joints
- Sluggish deep-tendon reflexes
- Mild facial-muscle weakness
- Hypotonic skeletal muscles
Findings on Physiologic Testing
Physiologic tests of autonomic function, when available, may provide diagnostic information of great specificity. Autonomic function test results (Table 1) indicate that complete DBH deficiency encompasses sympathetic noradrenergic failure and adrenomedullary failure but intact vagal and sympathetic cholinergic function [Biaggioni & Robertson 1987, van den Meiracker et al 1996, Bartoletti-Stella et al 2015].
- The Valsalva maneuver results in a profound fall in blood pressure together with an increase in heart rate reflecting parasympathetic withdrawal. The phase IV overshoot of the Valsalva maneuver does not occur.
- Hyperventilation causes a fall in blood pressure.
- Cold pressor testing causes either a fall or no change in blood pressure.
- Isometric handgrip exercise fails to significantly increase blood pressure.
Note: Click here for results of further physiologic tests of autonomic function.
Table 1.
DBHD 1 | Control 1 | Number: DBHD/Control | P Value | ||
---|---|---|---|---|---|
Age (years) | 26±14 | 34±10 | 0.033 | ||
Sinus arrhythmia ratio | 1.3±0.21 | 1.4±0.21 | 8/86 | 0.266 | |
Valsalva phase II | Delta SBP (mm Hg) | -41±25 | -7±22 | 7/55 | <0.001 |
Delta HR (bpm) | 29±11 | 30±16 | 7/53 | 0.828 | |
Valsalva phase IV | Delta SBP (mm Hg) | -22±18 | 23±16 | 8/84 | <0.001 |
Delta HR (bpm) | 5±9 | -8±11 | 8/82 | 0.001 | |
Valsalva ratio | 1.3±0.20 | 1.7±0.39 | 8/79 | <0.001 | |
Hyper- ventilation | Delta SBP (mm Hg) | -14±12 | -7±12 | 9/86 | 454 |
Delta HR (bpm) | 14±19 | 11±11 | 8/86 | 0.308 | |
Cold pressor | Delta SBP (mm Hg) | 4±10 | 21±14 | 8/83 | 0.001 |
Delta HR (bpm) | 16±11 | 10±11 | 7/83 | 0.183 | |
Handgrip | Delta SBP (mm Hg) | 2±6 | 17±13 | 7/83 | 0.003 |
Delta HR (bpm) | 15±11 | 10±10 | 7/83 | 0.230 |
EM Garland, unpublished data from Vanderbilt Autonomic Dysfunction Center
HR = heart rate; SBP = systolic blood pressure
- 1.
Mean ± SD
Specialized testing, such as a cardiac 123 I-metaiodobenzylguanidine scan, microneurography, and skin biopsies stained by the PGP pan neuronal marker and the DβH-specific adrenergic marker, can be used to confirm the selective loss of peripheral sympathetic noradrenergic function [Donadio et al 2016].
Laboratory Findings
Plasma catecholamines. Biochemical features unique to DBH deficiency:
- Minimal or absent plasma norepinephrine (NE) and epinephrine AND a five- to tenfold elevation of plasma dopamine (DA). This combination is probably pathognomonic of DBH deficiency.
- Plasma NE concentration should be below the limits of detection (<25 pg/mL or 0.15 nmol/L).
- Plasma DA concentration is frequently higher than 100 pg/mL (0.65 nmol/L). One atypical individual who was not diagnosed until age 73 years was reported to have a plasma DA concentration of 10,000 pg/mL (67 nmol/L) [Despas et al 2010].
- Although both baroreflex afferent and catecholamine release mechanisms are intact, DA is released in place of NE.
Note: (1) It is essential to assay both NE and DA and to use a procedure with high specificity for these catechols. (2) With some radioenzymatic methods for catecholamine determinations, a proportion of the DA may be erroneously measured as epinephrine [Robertson et al 1986]. (3) Very low (rather than undetectable) levels of NE can be reported in some assays and are also likely due to interference substances.
The plasma DA concentrations respond to various physiologic and pharmacologic stimuli in a way that mimics that of NE in normal individuals:
- A change from supine to upright posture doubles or triples the plasma DA concentration. This observation suggests that sympathetic nerves and reflex arcs are intact, but DA (rather than NE) is stored and released at the sympathetic synapse.
- Central sympatholytics lower plasma dopamine [Biaggioni & Robertson 1987].
Click here for information pertaining to pharmacologic findings that can be seen in individuals with DBH.
Establishing the Diagnosis
The diagnosis of DBH is established in a proband with profound neurogenic orthostatic hypotension, minimal or absent plasma concentrations of norepinephrine and epinephrine, and a five- to tenfold elevation of plasma dopamine; the diagnosis is confirmed with identification of biallelic pathogenic variants in DBH by molecular genetic testing (see Table 2).
Molecular genetic testing approaches can include a combination of gene-targeted testing (single-gene testing, multigene panel) and comprehensive genomic testing (exome sequencing, exome array, genome sequencing) depending on the phenotype.
Gene-targeted testing requires that the clinician determine which gene(s) are likely involved, whereas genomic testing does not. Because the phenotype of dopamine beta-hydroxylase deficiency is broad, individuals with the distinctive findings described in Suggestive Findings are likely to be diagnosed using gene-targeted testing (see Option 1), whereas those in whom the diagnosis of dopamine beta-hydroxylase deficiency has not been considered are more likely to be diagnosed using genomic testing (see Option 2).
Option 1
When the phenotypic and laboratory findings suggest the diagnosis of DBH deficiency, molecular genetic testing approaches can include single-gene testing or use of a multigene panel:
- Single-gene testing. Sequence analysis of DBH detects small intragenic deletions/insertions and missense, nonsense, and splice site variants; typically, exon or whole-gene deletions/duplications are not detected. Perform sequence analysis first. If only one or no pathogenic variant is found, perform gene-targeted deletion/duplication analysis to detect intragenic deletions or duplications.
- A multigene panel that includes DBH and other genes of interest (see Differential Diagnosis) is most likely to identify the genetic cause of the condition at the most reasonable cost while limiting identification of variants of uncertain significance and pathogenic variants in genes that do not explain the underlying phenotype. Note: (1) The genes included in the panel and the diagnostic sensitivity of the testing used for each gene vary by laboratory and are likely to change over time. (2) Some multigene panels may include genes not associated with the condition discussed in this GeneReview. (3) In some laboratories, panel options may include a custom laboratory-designed panel and/or custom phenotype-focused exome analysis that includes genes specified by the clinician. (4) Methods used in a panel may include sequence analysis, deletion/duplication analysis, and/or other non-sequencing-based tests. For this disorder a multigene panel that also includes deletion/duplication analysis is recommended (see Table 2).For an introduction to multigene panels click here. More detailed information for clinicians ordering genetic tests can be found here.
Option 2
When the diagnosis of DBH is not considered because an individual has atypical phenotypic features, comprehensive genomic testing (which does not require the clinician to determine which gene[s] are likely involved) is the best option. Exome sequencing is the most commonly used genomic testing method; genome sequencing is also possible.
Exome array (when clinically available) may be considered if exome sequencing is not diagnostic.
For an introduction to comprehensive genomic testing click here. More detailed information for clinicians ordering genomic testing can be found here.
Table 2.
Gene 1 | Method | Proportion of Pathogenic Variants 2 Detectable by Method |
---|---|---|
DBH | Sequence analysis 3 | 17/17 4 |
Gene-targeted deletion/duplication analysis 5 | Unknown 6 |
- 1.
See Table A. Genes and Databases for chromosome locus and protein.
- 2.
See Molecular Genetics for information on allelic variants detected in this gene.
- 3.
Sequence analysis detects variants that are benign, likely benign, of uncertain significance, likely pathogenic, or pathogenic. Pathogenic variants may include small intragenic deletions/insertions and missense, nonsense, and splice site variants; typically, exon or whole-gene deletions/duplications are not detected. For issues to consider in interpretation of sequence analysis results, click here.
- 4.
All variants reported to date
- 5.
Gene-targeted deletion/duplication analysis detects intragenic deletions or duplications. Methods used may include quantitative PCR, long-range PCR, multiplex ligation-dependent probe amplification (MLPA), and a gene-targeted microarray designed to detect single-exon deletions or duplications.
- 6.
No data on detection rate of gene-targeted deletion/duplication analysis are available.
Click here for information on the plasma DBH enzymatic assay.
Clinical Characteristics
Clinical Description
Dopamine beta-hydroxylase (DBH) deficiency is characterized by a lack of sympathetic noradrenergic function but normal parasympathetic and sympathetic cholinergic function. Affected individuals exhibit profound deficits in autonomic regulation of cardiovascular function, but apparently only subtle signs of central nervous system dysfunction [Robertson et al 1986, Man in 't Veld et al 1987, Timmers et al 2004, Jepma et al 2011].
Onset. Although DBH deficiency appears to be present from birth, the diagnosis is not generally recognized until late childhood, when orthostatic hypotension becomes more severe.
Features by age. The full clinical spectrum of DBH deficiency is not known because of the limited number of cases reported. Clinical features reported in 21 affected individuals (13 female, 8 male) are included in Table 3.
- Infancy:
- In the perinatal period, DBH deficiency has been complicated by vomiting, dehydration, hypotension, hypothermia, and hypoglycemia requiring repeated hospitalization.
- Delay in opening of the eyes has occurred and ptosis of the eyelids is seen in most affected infants.
- Childhood:
- Children with DBH deficiency have markedly reduced exercise capacity, perhaps because of hypotension engendered by physical exertion.
- The syncope associated with postural hypotension often suggests seizures and prompts trials of anticonvulsive medication despite lack of abnormalities on the electroencephalogram.
- Mental and physical development are normal.
- Adolescence and early adulthood:
- Symptoms generally worsen in late adolescence.
- By early adulthood, affected individuals demonstrate profound orthostatic hypotension, fatigue, greatly reduced exercise tolerance, ptosis of the eyelids, and nasal stuffiness. Insulin resistance has been reported in an affected female age 15 years [Arnold et al 2017].
- Males experience retrograde or prolonged ejaculation.
Clinical features of DBH deficiency are included in Table 3.
Table 3.
Feature | # of Individuals 1 |
---|---|
Severe orthostatic hypotension | 21/21 (100%) |
Anemia | 9/15 (60%) |
Ptosis of eyelids | 12/14 (86%) |
Hyperflexible or hypermobile joints | 6/10 (60%) |
ECG abnormalities 2 | 2/12 (17%) |
Epileptiform symptoms | 4/12 (33%) |
Nasal stuffiness | 10/10 (100%) |
Hypoglycemia | 4/12 (33%) |
Sluggish deep-tendon reflexes | 3/9 (33%) |
Increased plasma creatinine | 6/11 (54%) |
Polyuria/nocturia | 3/9 (33%) |
High palate | 9/10 (90%) |
Increased BUN | 6/9 (67%) |
Muscle hypotonia | 3/9 (33%) |
Postprandial hypotension | 3/7 (43%) |
Sleep irregularities | 5/7 (71%) |
Impaired ejaculation | 4/4 (100%) |
- 1.
Number of individuals with the finding/total number evaluated for the finding
- 2.
ECG = electrocardiogram
Presyncopal symptoms include dizziness, blurred vision, dyspnea, nuchal discomfort, and occasionally chest pain. Symptoms may worsen in hot environments or after heavy meals or alcohol ingestion. Occasional bouts of unexplained diarrhea occur.
Renal function. Elevated blood urea nitrogen has been noted in six affected individuals in the USA [Garland et al 2005a, Garland et al 2009]. This may be evidence of a loss of renal function. A nephrologist who evaluated an individual age 16 years with a disproportionately high BUN (32 mg/dL) and slightly elevated creatinine (1.09 mg/dL) proposed that renal perfusion was reduced and that a BUN/Cr ratio <25 should be targeted. Although droxidopa acutely improved the ratio, the BUN/Cr ratio was further increased after a year of droxidopa treatment. The estimated GFR of an affected female age 57 years was reduced to 18 mL/min/1.73 m2 [Emily Garland, personal observation]. Another patient with unexpectedly low eGFR and elevated creatinine was found, by electron microscopy, to have abnormal, fused mitochondria in the proximal, but not the distal, tubules. Associated problems with the glomerular-tubular balance can be at least partially reversed by treatment with droxidopa [Wassenberg et al 2017].
Cognitive function. Despite the lack of norepinephrine, persons with DBH deficiency apparently have relatively normal mental status. Five affected individuals and ten matched healthy unaffected participants underwent a comprehensive battery of neurocognitive testing in addition to brain MRI, pupillometry, and EEG. Performance of the affected individuals, whether on or off droxidopa treatment, was similar to that of the unaffected individuals in most respects, suggesting that other systems compensate for absent norepinephrine in affected individuals. Brain MRI studies revealed a smaller total brain volume in the affected individuals compared to unaffected individuals, although relative proportions of white and gray matter and cerebrospinal fluid were similar in the two groups. In addition, affected individuals had a temporal-attention deficit when they were not on treatment. During an attentional-blink task, participants were asked to identify two digits, separated by a variable number of letters. Attentional blink refers to the deficit in processing the second digit when it is presented within 200-400 msec of the first. Accuracy in identifying the second digit was impaired in affected individuals not on treatment but performance improved with droxidopa treatment [Jepma et al 2011].
Ptosis. Ptosis of the eyelids, defined as a reduction in the margin reflex distance, is common in individuals with DBH deficiency and can be noted at an early age. It was reported in the first descriptions of individuals with this disorder in the late 1980s and in more than 85% of all cases in the published literature. Levator function is intact. Some individuals undergo levator advancement surgery [Phillips et al 2013], which may mask this aspect of the phenotype.
Olfactory function is relatively unaffected in individuals with DBH deficiency, who have intact noradrenergic neurons, in contrast to the marked deficit in individuals with pure autonomic failure, who have peripheral neuronal degeneration [Garland et al 2011].
Hypoglycemia. Because so few individuals have been diagnosed with DBH deficiency, there has not been a clear explanation for the occurrence of hypoglycemic episodes in some of the individuals. It is not known if this is related to the absence of norepinephrine and epinephrine, or the elevated levels of dopamine. Investigators have speculated that it may result from loss of the counterregulatory actions of epinephrine that protect against hypoglycemia [Man in 't Veld et al 1987]. In contrast to the report of hypoglycemia during the perinatal period, a girl age 15 years studied with a hyperglycemic clamp had a normal fasting glucose level but insulin resistance [Shibao et al 2014]. Her hyperinsulinemia persisted after a year of droxidopa treatment, despite improved orthostatic tolerance and restoration of plasma norepinephrine [Arnold et al 2017].
High palate. Physicians who inspect the palate often report that patients with DBH deficiency have a high, arched palate [Man in 't Veld et al 1988, Cheshire et al 2006; Emily Garland, unpublished findings]. This, however, is generally a subjective determination; it is not known how frequently it is either not assessed or reported incorrectly.
Life span. Four persons with DBH deficiency are known to have died. A woman age 57 years had chronic kidney disease and was undergoing treatment for breast cancer. Her listed cause of death at an assisted living facility was cardiac arrhythmia. Autopsy of a male age 28 years reported "scattered pyknotic cerebral neurons, isolated microfoci of cortical gliosis, cardiac arteriolar smooth muscle hypertrophy, scattered fibrosis in the cardiac conduction system, and sclerotic renal glomeruli." Cardiac dysrhythmia, possibly related to fibrosis in the cardiac conduction system, may have contributed to the patient's sudden demise [Cheshire et al 2006]. One individual died at age 20 years, possibly by suicide. A person age 63 died of unknown causes. Other affected individuals are likely to be deceased, but there are no published reports of causes of death or of effects of the disorder on life span.
One individual was not diagnosed with DBH deficiency until age 73 years despite having long-lasting orthostatic hypotension [Despas et al 2010], suggesting that DBH deficiency may not necessarily shorten the life span.
Genotype-Phenotype Correlations
There are no known genotype-phenotype correlations.
Prevalence
The prevalence of DBH deficiency is unknown. Only 23 affected individuals, all of western European descent, have been reported in the literature, suggesting that it is a rare disorder.
Differential Diagnosis
The striking catecholamine abnormalities distinguish DBH deficiency from other disorders. Other catecholamine disorders described in the past, such as aromatic L-amino acid decarboxylase deficiency (OMIM 608643), have clinical presentations distinct from that of DBH deficiency [Swoboda et al 2003].
Pure autonomic failure / autonomic neuropathy. Pure autonomic failure or Bradbury-Eggleston syndrome is a degenerative disorder of the autonomic nervous system presenting in middle to late life. Like DBH deficiency, it is characterized by severe orthostatic hypotension. It differs from DBH deficiency in that it affects both the sympathetic and parasympathetic nervous systems. Hypohidrosis is common. Individuals with pure autonomic failure have marked hypersensitivity to all pressor and depressor stimuli. Plasma and urinary norepinephrine concentrations are greatly reduced, sometimes to 10% of normal; plasma dopamine concentrations are normal or low, rather than elevated as in DBH deficiency.
Systemic illness. Some dysautonomias result from well-characterized autonomic neuropathies secondary to systemic illnesses such as diabetes mellitus.
Other disorders with orthostatic hypotension to consider in the differential diagnosis of DBH deficiency are summarized in Table 4.
Table 4.
Disorder | Gene(s) | MOI | Clinical Description / Comments | Distinguishing Clinical Features |
---|---|---|---|---|
Familial dysautonomia (FD) | ELP1 1 | AR |
| In DBH deficiency:
|
ATP7A-related copper transport disorders (Menkes disease & Occipital horn syndrome) | ATP7A 4 | XL | DBH is a copper-dependent enzyme & thus DBH activity is depressed in individuals w/ATP7A |