PROK2/PROKR2 Signaling and Kallmann Syndrome.

[kallmann syndrome]

Kallmann syndrome (KS ) is a developmental disease that associates hypogonadism and a deficiency of the sense of smell . The reproductive phenotype of KS results from the primary interruption of the olfactory , vomeronasal , and terminal nerve fibers in the frontonasal region , which in turn disrupts the embryonic migration of neuroendocrine gonadotropin-releasing hormone (GnRH ) synthesizing cells from the nose to the brain . This is a highly heterogeneous genetic disease , and mutations in any of the nine genes identified so far have been found in approximately 30 % of the KS patients . PROKR 2 and PROK 2 , which encode the G protein-coupled prokineticin receptor-2 and its ligand prokineticin-2 , respectively , are two of these genes . Homozygous knockout mice for the orthologous genes exhibit a phenotype reminiscent of the KS features , but biallelic mutations in PROKR 2 or PROK 2 (autosomal recessive mode of disease transmission ) have been found only in a minority of the patients , whereas most patients carrying mutations in these genes are heterozygotes . The mutations , mainly missense mutations , have deleterious effects on PROKR 2 signaling in transfected cells , ranging from defective cell surface-targeting of the receptor to defective coupling to G proteins or impaired receptor-ligand interaction , but the same mutations have also been found in apparently unaffected individuals , which suggests a digenic /oligogenic mode of inheritance of the disease in heterozygous patients . This non-Mendelian mode of inheritance has so far been confirmed only in a few patients . However , it may account for the unusually high proportion of KS sporadic cases compared to familial cases .