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 11182749
Gene Name INSL3
Condition Infertility
Association The evidence suggests that INSL3 mutations and polymorphisms are not a major cause of testicular maldescent with or without associated undermasculinisation
PMID 11182749
Gene Name INSL3
Condition Maldescent of the testis
Association The evidence suggests that INSL3 mutations and polymorphisms are not a major cause of testicular maldescent with or without associated undermasculinisation.
Mutation A-1G, V19L, P25S, A36T, R78H
Population size 211
Population details 211 (28 testicular maldescent, 24 patients with undermasculinised genitalia and intra-abdominal, 33 patients with inguinal gonads, 15 normal males, 29 males with undermasculinised genitalia and scrotal gonads, 82 females)
Sex Male, female
Infertility type Male infertility
Other associated phenotypes Maldescent of the testis


Genetic analysis of the INSL3 gene in patients with maldescent of the testis

Lim HN, Raipert-de Meyts E, Skakkebaek NE, Hawkins JR, Hughes IA.

OBJECTIVE: Testicular maldescent is important because it is a common congenital disorder that is associated with an increased risk of infertility and testicular cancer. Murine studies indicate that testicular maldescent can result from disruption of insulin-like factor 3 (INSL3) activity and that it may be more severe when there is concurrent undermasculinisation. Therefore, the INSL3 gene was screened for mutations and polymorphisms that may contribute to testicular maldescent in patients with undermasculinisation as well as those with isolated testicular maldescent. METHODS AND RESULTS: The patient groups consisted of individuals with isolated testicular maldescent (n=28) and patients with undermasculinised genitalia and intra-abdominal (n=24) or inguinal gonads (n=33). The three control groups were: normal males (n=15), males with undermasculinised genitalia and scrotal gonads (n=29) and females (n=82). SSCP/HA mutation screening detected eight variants, five of which were predicted to alter the protein sequence (A-1G, V19L, P25S, A36T, R78H). Three of the amino acid changes (A-1G, V19L, R78H) each occurred in a single control sample and one was identified in a male with undermasculinised genitalia and intra-abdominal testes (P25S). The A36T amino acid polymorphism was found in both patient and control groups at a similar frequency. CONCLUSIONS: The evidence suggests that INSL3 mutations and polymorphisms are not a major cause of testicular maldescent with or without associated undermasculinisation. FAU - Lim, H N AU - Lim HN AD - Department of Paediatrics, University of Cambridge, Box 116, Level 8, Addenbrooke's Hospital, Cambridge CB2 2QQ, UK. HL215@mole.bio.cam.ac.uk FAU - Raipert-de Meyts, E AU - Raipert-de Meyts E FAU - Skakkebaek, N E AU - Skakkebaek NE FAU - Hawkins, J R AU - Hawkins JR