The clinical spectrum of nodular heterotopias in children: report of 31 patients.

[pyruvate dehydrogenase deficiency]

The phenotypic and etiologic spectrum in adults with nodular heterotopias (NHs ) has been well characterized . However , there are no large pediatric case series . We , therefore , wanted to review the clinical features of NHs in our population .Hospital records of 31 patients with pathology or imaging-confirmed NHs were reviewed . Two -sided Fisher 's exact t-test was used to assess associations between distribution of NHs and specific clinical features .NHs were distributed as follows : 8 (26 %) unilateral focal subependymal , 3 (10 %) unilateral diffuse subependymal , 5 (16 %) bilateral focal subependymal , 12 (39 %) bilateral diffuse subependymal , and 3 (10 %) isolated subcortical . The phenotypic spectrum in our population differs from that described in adults . Significant morbidity and mortality are associated with presentation in childhood . Twenty -two of 31 patients (71 %) died in the neonatal period or in childhood . Additional cerebral malformations were found in 80 % and systemic malformations in 74 %. The majority of patients had developmental delay , intellectual deficit , and intractable epilepsy . Patients with unilateral focal NHs were more likely to have ventriculomegaly (p = 0 .027 ), and those with bilateral diffuse NHs more likely to have cerebellar abnormalities (p = 0 .007 ). Isolated subcortical NHs were associated with multiple malformations (p = 0 .049 ) and cardiac abnormalities (p = 0 .027 ). Underlying etiology was heterogeneous and determined in only six cases (19 %): del chr 1 p 36 , del chr 15 q 11 , pyruvate dehydrogenase deficiency , sialic acidosis type 1 , Aicardi syndrome , and FLNA mutation .NHs are present in childhood as part of multiple cerebral and systemic malformations ; developmental delay and refractory seizures are the rule rather than the exception . Milder forms go unrecognized until seizure onset in adulthood .