Paradoxical Risk of Reduced Fertility After Exposure of Prepubertal Mice to Vincristine or Cyclophosphamide at Low Gonadotoxic Doses in Humans

Overview

Journal Sci Rep

Specialty Science

Date 2020 Oct 21

PMID 33082498

Citations 8

Authors

Marion Delessard

Justine Saulnier

Ludovic Dumont

Aurelie Rives-Feraille

Nathalie Rives

Christine Rondanino

Affiliations

Soon will be listed here.

Abstract

Cancer treatment can have long-term side effects in cured patients and infertility is one of them. Given the urgency of diagnosis in children with cancer, the toxicity of treatments on the gonad was overshadowed for a long time. In the present study, prepubertal mice were treated by vincristine or cyclophosphamide commonly used in acute leukaemia treatment. The prepubertal exposure to cyclophosphamide, at a low gonadotoxic dose in humans (< 3.5 g/m), led to morphological alterations of prepubertal testicular tissue. An increased proportion of spermatozoa with hypocondensed chromatin and oxidized DNA associated with decreased fertility were uncovered at adulthood. Short- and long-term morphological alterations of the testicular tissue, disturbed progression of spermatogenesis along with increased proportions of isolated flagella and spermatozoa with fragmented DNA were evidenced in vincristine-treated mice. Moreover, the fertility of mice exposed to vincristine was severely affected despite being considered low-risk for fertility in humans. Paternal exposure to vincristine or cyclophosphamide before puberty had no impact on offspring development. Contrary to the current gonadotoxic risk classification, our results using a mouse model show that vincristine and cyclophosphamide (< 3.5 g/m) present a high gonadotoxic risk when administered before the initiation of spermatogenesis.

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