Imatinib decreases germ cell survival and germline stem cell proliferation in rodent testis ex vivo and in vitro - UTU Research Portal

A1 Refereed original research article in a scientific journal

Imatinib decreases germ cell survival and germline stem cell proliferation in rodent testis ex vivo and in vitro

Authors: Eggert, Anna; Laasanen, Sini; Nurmio, Mirja; Wahlgren, Aida; Jahnukainen, Kirsi; Eerola, Kim; Nieminen, Miisael; Olotu, Opeyemi; Kotaja, Noora; Mäkelä, Juho‐Antti; Toppari, Jorma

Publisher: Wiley

Publication year: 2024

Journal: Andrology

Journal name in source: Andrology

ISSN: 2047-2919

eISSN: 2047-2927

DOI: https://doi.org/10.1111/andr.13777

Web address : https://doi.org/10.1111/andr.13777

Self-archived copy’s web address: https://research.utu.fi/converis/portal/detail/Publication/459052950

Abstract

Background

Imatinib and dasatinib are tyrosine kinase inhibitors (TKIs) increasingly used to treat several diseases in both children and adults at fertile age. We have previously shown that imatinib has adverse effects on developing testis, and imatinib-treated male patients have been reported to have reduced sperm counts. However, the cellular level effects of imatinib and dasatinib on adult male germ cells and germline stem cells (mGSCs) have not been thoroughly investigated.

Objectives

To analyze whether imatinib or dasatinib exposure ex vivo and in vitro is harmful to adult male rodent germ cells and mGSCs.

Materials and methods

Seminiferous tubule segments of adult male mouse or rat were cultured in the presence or the absence of imatinib or dasatinib. Stage-specific effects were monitored by ³H-thymidine incorporation assay (DNA synthesis), immunohistochemistry (cleaved Caspase-3; apoptosis), immunofluorescence (KI67, GFRα1, STRA8, c-KIT, LIN28A; proliferation and spermatogonial differentiation) and flow cytometry (Hoechst). Mouse mGSCs were exposed to imatinib and dasatinib to study proliferation, apoptosis, and differentiation.

Results

Imatinib decreased stage-specific DNA synthesis, and induced apoptosis in cultured rat seminiferous tubule segments. Imatinib also had an adverse effect on mGSC proliferation both in vitro and ex vivo, but did not induce cell death in cultured mGSCs. Imatinib did not impinge on induction of spermatogonial differentiation but suppressed c-KIT expression in nascent differentiating spermatogonia, providing a plausible mechanism for its pro-apoptotic function in spermatogenic cells. Clinically relevant doses of dasatinib did not induce apoptosis in seminiferous tubules but decreased mGSC colony growth in vitro.

Conclusions

Imatinib exposure ex vivo and in vitro impinges on male rodent germ cell proliferation and survival. The plausible mechanism in spermatogenic cells is the inhibition of SCF/c-KIT signaling, and reduced expression of c-KIT. Dasatinib did not show significant adverse effects with clinical doses ex vivo but inhibited mGSC colony growth in vitro.

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Funding information in the publication:
This study has been financially supported by University of Turku, Turku Doctoral Programme of Molecular Medicine, Academy of Finland, Sigrid Juselius Foundation, Emil Aaltonen Foundation, AAMU Pediatric Cancer Foundation, The Finnish Medical Foundation, Turunmaan Duodecim Society, Turku University Hospital, European Commission, Karolinska Institute, Swedish Childhood Cancer Foundation, Jane and Aatos Erkko Foundation, Novo Nordisk Foundation, Cancer Foundation Finland, the Finnish Foundation for Pediatric Research, the Birgitta and Carl-Axel Rydbeck's Research Grant for Paediatric Research.