Erythrocyte PIG‐A mutant frequencies in cancer patients receiving cisplatin

Author:

Dobrovolsky Vasily N.1ORCID,Atiq Omar T.2,Heflich Robert H.1,Maisha Mackean3,McKinzie Page B.1,Pearce Mason G.1,Robison Timothy W.4

Affiliation:

1. Division of Genetic and Molecular Toxicology National Center for Toxicological Research (NCTR), US Food and Drug Administration (FDA) Jefferson Arkansas USA

2. University of Arkansas for Medical Sciences (UAMS) Winthrop P. Rockefeller Cancer Institute Little Rock Arkansas USA

3. Office of Scientific Coordination, NCTR, FDA Jefferson Arkansas USA

4. Office of New Drugs, OII, DPTII, Center for Drug Evaluation and Research (CDER), US FDA Silver Spring Maryland USA

Abstract

AbstractBackgroundCisplatin is a primary chemotherapy choice for various solid tumors. DNA damage caused by cisplatin results in apoptosis of tumor cells. Cisplatin‐induced DNA damage, however, may also result in mutations in normal cells and the initiation of secondary malignancies. In the current study, we have used the erythrocyte PIG‐A assay to evaluate mutagenesis in non‐tumor hematopoietic tissue of cancer patients receiving cisplatin chemotherapy.MethodsTwenty‐one head and neck cancer patients undergoing treatment with cisplatin were monitored for the presence of PIG‐A mutant total erythrocytes and the young erythrocytes, reticulocytes (RETs), in peripheral blood for up to five and a half months from the initiation of the anti‐neoplastic chemotherapy.ResultsPIG‐A mutant frequency (MF) in RETs increased at least two‐fold in 15 patients at some point of the monitoring, while the frequency of total mutant RBCs increased at least two‐fold in 6 patients. A general trend for an increase in the frequency of mutant RETs and total mutant RBCs was observed in 19 and 18 patients, respectively. Only in one patient did both RET and total RBC PIG‐A MFs did not increase at any time‐point over the monitoring period.ConclusionCisplatin chemotherapy induces moderate increases in the frequency of  PIG‐A mutant erythrocytes in head and neck cancer patients. Mutagenicity measured with the flow cytometric PIG‐A assay may serve as a tool for predicting adverse outcomes of genotoxic antineoplastic therapy.

Publisher

Wiley

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