Mutation screening of SEMA3A and SEMA7A in patients with congenital hypogonadotropic hypogonadism.

[kallmann syndrome]

Congenital hypogonadotropic hypogonadism (HH ), a rare disorder characterized by absent , partial , or delayed puberty , can be caused by the lack or deficient number of hypothalamic gonadotropin-releasing hormone (GnRH ) neurons . SEMA 3 A was recently implicated in the etiology of the disorder , and Sema 7 A -deficient mice have a reduced number of GnRH neurons in their brains .S EMA 3 A and SEMA 7 A were screened by Sanger sequencing in altogether 50 Finnish HH patients (34 with Kallmann syndrome (KS ; HH with hyposmia /anosmia ) and 16 with normosmic HH (nHH )). In 20 patients , mutation (s ) had already been found in genes known to be implicated in congenital HH .Three heterozygous variants (c .458 A >G (p .Asn 153 Ser ), c .1253 A >G (p .Asn 418 S er ), and c .1303 G >A (p .Val 435 Ile )) were found in SEMA 3 A in three KS patients , two of which also had a mutation in FGFR 1 . Two rare heterozygous variants (c .442 C >T (p .Arg 148 Trp ) and c .1421 G >A (p .Arg 474 Gln )) in SEMA 7 A were found in one male nHH patient with a previously identified KISS 1 R nonsense variant and one male KS patient with a previously identified mutation in KAL 1 , respectively .Our results suggest that heterozygous missense variants in SEMA 3 A and SEMA 7 A may modify the phenotype of KS but most likely are not alone sufficient to cause the disorder .