Microcephaly

• Prenatally, ultrasound

• Postnatally, physical examination, including measurement of head circumference and cranial imaging

• Genetic testing

Prenatally, the diagnosis of microcephaly sometimes is made with ultrasound done in the late second or early third trimester.

Postnatally, evaluation should include detailed prenatal history to identify risk factors, developmental and neurologic assessment, and brain MRI or CT. Primary isolated autosomal recessive microcephaly refers to microcephaly that is not associated with other extracerebral malformations. There are several different genes that can cause it.

A clinical geneticist should evaluate affected patients even in cases of apparent isolated congenital anomaly.

Chromosomal abnormalities can occur with microcephaly. Among the genetic syndromes to be considered are Seckel syndrome, Smith-Lemli-Opitz syndrome, syndromes due to defective DNA repair (eg, Fanconi and Cockayne syndromes), and Angelman syndrome. For parents of an affected child, risk of the disorder appearing in subsequent offspring may be as high as 25%, depending on which syndrome is present, and thus clinical genetic assessment is necessary. A gene panel test specific for microcephaly is available through several diagnostic laboratories. Chromosomal microarray analysis, or broader gene panel tests also should be considered in the evaluation of patients with microcephaly. If the results of these tests are nondiagnostic, whole exome sequencing analysis may be recommended.

• Symptomatic treatment

Symptoms resulting from brain damage are treated. Some disorders causing microcephaly can be treated.

In general, management is based on symptoms, and developmental services are maximized (1).