Sex and Circadian Timing Modulate Oxaliplatin Hematological and Hematopoietic Toxicities

Author:

Dulong SandrineORCID,de Souza Lucas Eduardo BotelhoORCID,Machowiak Jean,Peuteman Benoit,Duvallet Gaelle,Boyenval Déborah,Roth Elise,Asgarova Afag,Chang Yunhua,Li Xiao-Mei,Foudi AdlenORCID,Ballesta Annabelle

Abstract

Oxaliplatin was nearly twice as hematotoxic, with optimal circadian timing differing by 6 h, in women as compared to men with colorectal cancers. Hence, we investigated sex- and timing-related determinants of oxaliplatin hematopoietic toxicities in mice. Body-weight loss (BWL), blood cell counts, bone marrow cellularity (BMC) and seven flow-cytometry-monitored hematopoietic progenitor populations were evaluated 72 h after oxaliplatin chronotherapy administration (5 mg/kg). In control animals, circadian rhythms of circulating white blood cells showed a peak at ZT5 in both sexes, whereas BMC was maximum at ZT20 in males and ZT13h40 in females. All BM progenitor counts presented robust rhythms with phases around ZT3h30 in females, whereas only three of them rhythmically cycled in males with a ≈ −6 h phase shift. In treated females, chronotoxicity rhythms occurred in BWL, WBC, BMC and all BM progenitors with the best timing at ZT15, ZT21, ZT15h15 and ZT14h45, respectively. In males, almost no endpoints showed circadian rhythms, BWL and WBC toxicity being minimal, albeit with a substantial drop in BM progenitors. Increasing dose (10 mg/kg) in males induced circadian rhythms in BWL and WBC but not in BM endpoints. Our results suggest complex and sex-specific clock-controlled regulation of the hematopoietic system and its response to oxaliplatin.

Funder

French National Institute of Health and Medical Research

French Plan Cancer through the ATIP-Avenir young investigator program

Publisher

MDPI AG

Subject

Pharmaceutical Science

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