AI Article Synopsis

  • Retinoblastoma (RB) is a childhood cancer linked to the loss of both RB1 alleles, with additional involvement of MDM2 and MDM4 genes in tumor development.
  • A study genotyped specific genetic variants in MDM2 and MDM4 among 104 RB patients and 104 controls, revealing that certain alleles may affect disease progression and survival rates.
  • Findings suggest that specific MDM2 and MDM4 genetic variations could influence both the likelihood of developing RB and the outcomes for affected patients.

Article Abstract

Background: Retinoblastoma (RB) accounts for 3% of all childhood malignancies, with different incidences around the world. This malignancy results from loss-of-function of both RB1 alleles although other genes, like MDM2 and MDM4, have been proposed to be involved in tumor development.

Procedure: We genotyped rs2279744T>G and rs937283A>G in MDM2, and rs4252668T>C and rs116197192G>A in MDM4, in 104 unrelated RB patients and 104 controls. Sixty-month survival Kaplan-Meier curves and χ(2)-tests were performed for estimating the putative effect of MDM2 and MDM4 alleles on disease progression and survival of RB patients.

Results: MDM2 rs2279744G was significantly more frequent in controls, indicating an apparently protective effect on RB development. However, survival of patients who carried a constitutional RB1 mutation was significantly lower with rs2279744TG or GG than with rs2279744TT. Presence of rs2279744G and a constitutional RB1 mutation was sixfold more frequent in the 0-12 month age group than other age groups at onset of symptoms (P = 0.0401). MDM4 rs4252668C was present at a significantly higher frequency in controls while the frequency of MDM4 rs116197192G was significantly higher in RB patients, suggesting that this allele might increase the risk of developing RB.

Conclusion: Our results indicate that MDM2 and MDM4 polymorphisms may influence development and/or survival in RB.

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Source
http://dx.doi.org/10.1002/pbc.24014DOI Listing

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