Clinical Description
Adams-Oliver syndrome (AOS) is characterized by aplasia cutis congenita (ACC) of the scalp and terminal transverse limb defects (TTLD). Additional major features frequently include cardiovascular malformations/dysfunction and less frequently, renal and brain anomalies (Table 2) [Snape et al 2009].
Table 2.
Frequency of Clinical Features Associated with Adams-Oliver Syndrome in Probands and Family Members
View in own window
| Finding | Frequency 1 |
|---|
| Cutis aplasia | ~80% |
| Transverse terminal limb defects | ~85% |
| Cardiac malformations | ~23% |
| Cutis marmorata telangiectatica congenita | ~20% |
| Neurologic abnormalities | Uncommon in AD & simplex AOS; ~30% in AR kindreds |
| Ophthalmologic abnormalities | <10% |
| Prenatal complications (intrauterine growth restriction or oligohydramnios) | <10% |
| Renal abnormalities | <5% |
- 1.
As reported in the literature
The severity of malformations ranges from subtle to disabling or life threatening; variability among family members is common. Although rare, severe morbidity and mortality in AOS usually results from hemorrhage or infection involving large and deep calvarial lesions, or from cardiovascular anomalies including severe heart malformations. At least five children with AOS have died from refractory pulmonary hypertension (~1% risk), all in the first three years of life.
Cutaneous/Cranial
Aplasia cutis congenita lesions usually occur in the midline of the parietal or occipital regions of the scalp, but can also occur on the abdomen or limbs, particularly in the setting of cutis marmorata telangiectatica congenita (CMTC). At birth, a lesion may already have the appearance of a healed scar (i.e., the absence of hair follicles).
Cutis aplasia lesions less than 5 cm often involve only the skin and almost always heal over a period of months into hairless, fibrotic patches with wound care measures only [Brzezinski et al 2015]. Scars may be either atrophic or hypertrophic.
Larger lesions are more likely to involve the skull and possibly the dura, and are at greater risk for complications, which can include infection, hemorrhage or thrombosis (especially of the sagittal sinus), brain herniation, CSF leakage, and seizures, and can result in death [Bernbeck et al 2005, Peralta-Calvo et al 2012, Udayakumaran et al 2013].
AOS-related ACC lesions – of the scalp and elsewhere – are generally non-membranous. Membranous ACC (appearing like a bulla) is hypothesized to arise from a different mechanism and may be associated with ectopic neural tissue and other findings such as a hair collar [Browning 2013].
Cutis aplasia lesions histologically show variable absence of epidermis, dermis, subcutaneous tissue, muscle, or bone.
Calvarial bone is affected in about half of reported individuals, which may reflect ascertainment and reporting biases toward more severely affected persons.
Cutis marmorata telangiectatica congenita (CMTC), one of the more clinically obvious findings, affects approximately 20% of individuals. CMTC is a network of superficial, persistently dilated small blood vessels, which creates a marbled or lattice-like appearance, also known as livedo reticularis. It usually becomes more prominent with strong emotions.
CMTC typically includes areas of phlebectasia, skin atrophy, or ulceration; when severe, CMTC is often associated with hypoplasia of the underlying structures (e.g., a smaller limb). Despite its name, telangiectasiae are only found in a minority of those with CMTC.
Cutis marmorata (CM), a milder vascular skin marbling phenomenon, is a normal physiologic finding in infants that shows marked enhancement with cold exposure or strong emotions and usually fades by age four months. Children with AOS may have more prominent CM than usual, but not have CMTC. A key distinction between CM and CMTC is that the vascular dilatation of CMTC does not fade markedly with local warming.
Limb
The term transverse terminal limb defect (TTLD), which is used to describe the types of anomalies seen in AOS, indicates involvement of all elements distal to a certain point. (In contrast, longitudinal defects [e.g., isolated radial or fibular aplasia] are not observed in AOS.) Although a few individuals with AOS have strictly transverse limb reduction defects, most have mild medial to lateral gradients in severity (or less commonly, the reverse) and others have a medial ray defect in the form of ectrodactyly.
The limb defects of AOS range from mild to severe. The mild end of the spectrum is unilateral or bilateral short distal phalanges, which may or may not affect all fingers or toes. Toes are almost always more severely affected than fingers. The nails may be dystrophic, shortened, or absent. Rarely, the distal phalanx may be present when the middle phalanx is absent [Isrie et al 2014].
Cutaneous or osseous syndactyly is often present. Occasionally, oligodactyly (entirely missing fingers or toes) or camptodactyly (fixed contracture of phalangeal joints) is observed.
The severe end of the spectrum can involve complete absence of all toes or fingers, feet or hands, or more. The appearance of a TTLD can often resemble an amputation.
Constriction rings and necrotic lesions have been observed [Keymolen et al 1999, Pereira-Da-Silva et al 2000].
Most individuals with AOS retain prehension of the thumb and fingers. Milder involvement, with fully preserved function, is much more common than severe involvement [Authors, personal observation].
Poland syndrome, the combination of unilateral aplasia of part of the pectoralis muscle and ipsilateral upper limb anomalies, has been reported convincingly in one family [Der Kaloustian et al 1991]. Of note, family 2 of this report most likely had scalp-ear-nipple syndrome (see Differential Diagnosis).
Radiographs can be helpful in delineating which bones are short; one would expect distal phalanges to be more severely affected than proximal phalanges, which in turn would be more affected than metacarpals.
Cardiovascular
Twenty-three percent of individuals with AOS have a major congenital cardiac malformation which can include left-sided obstructive lesions (bicuspid aortic valve, hypoplastic left ventricle, Shone's complex), septal defects, and conotruncal defects (tetralogy of Fallot, truncus arteriosus) [Snape et al 2009]. Although in some families the recurrences of a cardiac defect are very similar (e.g., tetralogy of Fallot or aortic valvulopathy), variability is more the norm.
Non-cirrhotic or idiopathic portal hypertension (also known as hepatoportal sclerosis), which is likely secondary to hepatic venulopathy or thrombosis, occurs in fewer than 10% of affected individuals [Swartz et al 1999]. Non-cirrhotic portal hypertension can initially be asymptomatic and only associated with mild thrombocytopenia, splenomegaly, or portal vein enlargement. However, eventually gastroesophageal varices can develop and affected individuals may experience variceal hemorrhage [Garcia-Tsao 2015]. Liver synthetic function would be expected to be normal. Liver fibrosis may be seen additionally or in isolation and massive steatosis has been reported in one individual.
Pulmonary hypertension occurs in fewer than 5% of individuals with AOS, but when present is associated with high mortality [Patel et al 2004]. It appears to be caused in most instances by primary abnormalities of the pulmonary vasculature, often on the venous side.
Other cardiovascular problems that may be present:
Neurologic
Although the majority of individuals with AOS have no neurologic deficits, a significant minority have a range of clinical and neuroimaging findings including the following [Sukalo et al 2015].
Possible clinical findings:
Cognitive disability, dyslexia, autism spectrum disorders
Spastic hemiplegia or diplegia
Seizures
Possible imaging findings:
Brain malformations and migration defects: microcephaly, cortical dysplasia, polymicrogyria, pachygyria, dysgenetic corpus callosum
Cortical atrophy with ventriculomegaly, cerebral hemorrhage, intracranial calcifications (often periventricular)
Delayed myelination
Brain involvement appears to associate with more severe vascular phenotypes, suggesting that impaired vascular supply to the developing brain may be a key component of pathogenesis for neurologic findings.
Although most individuals with brain involvement do not have an affected parent (suggesting either autosomal recessive inheritance or a de novo heterozygous pathogenic variant consistent with autosomal dominant inheritance), exceptions occur.
The severity of neurologic impairment can be such that central respiratory insufficiency can cause early death [Mempel et al 1999].
One individual has been reported with Tourette syndrome, which was not noted in two other sibs with AOS [Hassiem & Cavanna 2015].
Renal
Renal anomalies are rare and usually consist of small kidneys, hydronephrosis, or renal cortical vascular anomalies.
Ocular
The ophthalmologic complications of AOS can include the following [Fayol et al 2006, Temtamy et al 2007, Peralta-Calvo et al 2012]:
Microphthalmos
Peters anomaly-like findings
Cataracts
Retinal folds
Incomplete or abnormal retinal vasculature (including persistent fetal vasculature)
Esotropia
Optic nerve hypoplasia / optic atrophy
Rod dystrophy
Incomplete vascularization and fibrovascular proliferative ischemic retinopathy can appear similar to retinopathy of prematurity or certain cases of Norrie disease or Coats disease, and can lead to retinal hemorrhages or tractional retinal detachment, resulting in visual impairment [Lehman et al 2014].
Other
Other rarely reported, not necessarily associated findings include:
Possible Phenotype Correlations by Gene
While subtypes of AOS have not been established, emerging data suggest:
High risk for severe brain involvement in DOCK6-AOS (autosomal recessive inheritance) and less risk in ARHGAP31-AOS (autosomal dominant inheritance).
Increased risk for cardiac defects in NOTCH1-, DOCK6-, DLL4-, and EOGT-AOS and lower risk in RBPJ- and ARHGAP31-AOS.
ARHGAP31. The risk for cerebral involvement with this autosomal dominant form of AOS appears to be less than for the autosomal recessive forms, as to date neurologic abnormalities have not been reported in individuals with ARHGAP31-AOS.
DLL4. A significant minority of individuals have cardiovascular anomalies.
DOCK6. Approximately 15 families/probands with DOCK6-AOS have been reported. A cohort-based study yielded likely pathogenic DOCK6 variants in 29% (9/31) of families with suspected autosomal-recessive inheritance versus 2% (1/47) of simplex cases [Sukalo et al 2015]. To date, severe intellectual and neurologic impairments appear to be consistent findings in DOCK6-AOS, with findings in keeping with disturbed intracranial vasculogenesis. Ocular malformations and retinal issues are also seen more common in this subgroup; cardiac malformations have been reported as well.
EOGT. Periventricular calcifications and cardiovascular anomalies occurred in a significant minority [Shaheen et al 2013].
NOTCH1.
NOTCH1-AOS appears to show a particularly high rate of cardiac malformations and vasculopathy, occurring in at least half of affected individuals [Stittrich et al 2014, Southgate et al 2015]. Thrombotic occlusive or sclerotic portal venopathy leading to portal hypertension has been seen in several individuals, more commonly in simplex cases. Two children with NOTCH1-AOS have had pulmonary hypertension, which was mild in one [Southgate et al 2015] and transient in the other [Stittrich et al 2014]. At least one individual had neurologic deficits (spastic diplegia and intellectual disability) in the context of intracranial vascular lesions.
RBPJ. Intellectual impairment was a variable feature in both families reported with RPBJ-AOS [Hassed et al 2012].
