Home
Search

Simple

Advanced

Syndromes

Chromosomal defects

Infertility phenotypes

Highthroughput dataset
Browse

Genes

Proteins

SNPs

References

GO

Diseases

Pathways

Tools

Orthologs

SNPs

Motif scan

STRING

CDART
BLAST

BLASTN

BLASTP
Analysis

Panther

Function

GO

Pathways

Diseases
  Help
Statistics
   About Us

Search Results



PMID 17437853
Gene Name INSL3
Condition Infertility
Association The study reports three mutations observer in INSL3 gene in patients and also infers that insulin-like factor 3 gene may contribute to other anomalies of male genital development, such as micropenis
PMID 17437853
Gene Name INSL3
Condition Cryptorchidism
Association The study identified 3 novel insulin-like factor 3 variants, including C-19G, V18M and R105H, in 3 of the 109 patients (2.75%) but in none of the 270 controls. The V18M mutation in the insulin-like factor 3 signal peptide had a significant deleterious eff
Mutation INSL3 variants (C-19G, V18M and R105H)
Population size 454
Population details 454 (184 patients (52 presented with unilateral cryptorchidism, 37 presented with bilateral cryptorchidism, 19 presented with cryptorchidism and hypospadias, 1 presented with bilateral cryptorchidism and micropenis, and 75 presented with isolated hypospad
Sex Male
Infertility type Male infertility
Associated genes INSL3, LGR8 receptor
Other associated phenotypes Cryptorchidism


Novel mutations involving the INSL3 gene associated with cryptorchidism

El Houate B, Rouba H, Sibai H, Barakat A, Chafik A, Chadli el B, Imken L, Bogatcheva NV, Feng S, Agoulnik AI, McElreavey K.

PURPOSE: Cryptorchidism affects 1% to 9% of full-term male neonates. Hypospadias is the second most frequent congenital anomaly seen in newborn males. These pathological conditions are part of the testicular dysgenesis syndrome. Insulin-like factor 3 and LGR8 (leucine-rich repeat-containing G protein-coupled receptor 8), acting as a hormone and a receptor, respectively, are involved in control of the first phase of testicular descent via gubernacular development. MATERIALS AND METHODS: The study group consisted of 184 patients, of whom 52 presented with unilateral cryptorchidism, 37 presented with bilateral cryptorchidism, 19 presented with cryptorchidism and hypospadias, 1 presented with bilateral cryptorchidism and micropenis, and 75 presented with isolated hypospadias. A control panel consisted of 270 controls, including 127 fertile, and 143 fertile noncryptorchid males. Insulin-like factor 3 mutations were analyzed by direct sequencing and restriction enzyme digestion. We analyzed the ability of the mutant insulin-like factor 3 peptides identified in this study to activate LGR8 receptor in an ex vivo assays. RESULTS: We identified 3 novel insulin-like factor 3 variants, including C-19G, V18M and R105H, in 3 of the 109 patients (2.75%) but in none of the 270 controls. The V18M mutation in the insulin-like factor 3 signal peptide had a significant deleterious effect in activating LGR8 receptor in ex vivo studies (p<0.05). To our knowledge we report the first variant in the promoter region of the insulin-like factor 3 gene in a patient with cryptorchidism in association with micropenis. CONCLUSIONS: Mutations involving the insulin-like factor 3 gene may contribute to other anomalies of male genital development, such as micropenis. FAU - El Houate, Brahim AU - El Houate B AD - Human Genetics Department, Institut Pasteur of Morocco, Casablanca, Morocco. FAU - Rouba, Hassan AU - Rouba H FAU - Sibai, Hicham AU - Sibai H FAU - Barakat, Abdelhamid AU - Barakat A FAU - Chafik, Abdelaziz AU - Chafik A FAU - Chadli, El Bekkay AU - Chadli el B FAU - Imken, Laila AU - Imken L FAU - Bogatcheva, Natalia V AU - Bogatcheva NV FAU - Feng, Shu AU - Feng S FAU - Agoulnik, Alexander I AU - Agoulnik AI