Abstract
The role of the prokineticin 2 pathway in human reproduction, olfactory bulb morphogenesis, and gonadotropin-releasing hormone secretion is well established. Recent studies have highlighted the implication of di/oligogenic inheritance in this disorder. In the present study, we aimed to identify the genetic mechanisms that could explain incomplete penetrance in hypogonadotropic hypogonadism (HH). This study involved two unrelated Tunisian patients with HH, which was triggered by identifying a homozygous p.(Pro290Ser) mutation in the PROKR2 gene in a girl (HH1) with Kallmann syndrome (KS). The functional effect of this variant has previously been well demonstrated. Unexpectedly, her unaffected father (HH1P) and brother (HH1F) also carried this genetic variation at a homozygous state. In the second family, we identified a heterozygous p.(Lys205del) mutation in PROKR2, both in a male patient with normosmic idiopathic IHH (HH12) and his asymptomatic mother. Whole-exome sequencing in the three HH1 family members allowed the identification of additional variants in the prioritized genes. We then carried out digenic combination predictions using the oligogenic resource for variant analysis (ORVAL) software. For HH1, we found the highest number of disease-causing variant pairs. Notably, a CCDC141 variant (c.2803C > T) was involved in 18 pathogenic digenic combinations. The CCDC141 variant acts in an autosomal recessive inheritance mode, based on the digenic effect prediction data. For the second patient (HH12), prediction by ORVAL allowed the identification of an interesting pathogenic digenic combination between DUSP6 and SEMA7A genes, predicted as “dual molecular diagnosis.” The SEMA7A variant p.(Glu436Lys) is novel and predicted as a VUS by Varsome. Sanger validation revealed the absence of this variant in the healthy mother. We hypothesize that disease expression in HH12 could be induced by the digenic transmission of the SEMA7A and DUSP6 variants or a monogenic inheritance involving only the SEMA7A VUS if further functional assays allow its reclassification into pathogenic. Our findings confirm that homozygous loss-of-function genetic variations are insufficient to cause KS, and that oligogenism is most likely the main transmission mode involved in Congenital Hypogonadotropic Hypogonadism.
Highlights
Idiopathic hypogonadotropic hypogonadism (IHH) (MIM ID #146110) is defined as the absence of sex steroid synthesis associated with the lack of appropriate gonadotropin secretion
Her basal and stimulated gonadotropin-releasing hormone (GnRH)–gonadotropin levels were flat, and her magnetic resonance imaging (MRI) of the hypothalamic–pituitary region showed an aplasia of the olfactory bulbs (Table 1)
His GnRH response showed a normal response of follicle-stimulating hormone and luteinizing hormone
Summary
Idiopathic hypogonadotropic hypogonadism (IHH) (MIM ID #146110) is defined as the absence of sex steroid synthesis associated with the lack of appropriate gonadotropin secretion. This leads to a variable degree of impuberism, often diagnosed during childhood or adolescence. Normosmic idiopathic hypogonadotropic hypogonadism (nIHH), which is not associated with anosmia, and results from the dysfunction of the GnRH neurons that successfully completed their embryonic migration to the hypothalamus. Molecular alterations have been identified for several neuropeptides or their corresponding receptors, which are involved in the physiology of the gonadotropic axis: GNRHR/GNRH1, KISS1R/GPR54, TAC3/TACR3, and PROK2/PROKR2 (Brioude et al, 2010; Topaloglu and Kotan, 2010). IHH has been predominantly detected in sporadic cases (Quaynor et al, 2011; Gach et al, 2020)
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