Differential effects of cisplatin on cybrid cells with varying mitochondrial DNA haplogroups

Author:

Abedi Sina1,Yung Gregory1,Atilano Shari R.1,Thaker Kunal1,Chang Steven1,Chwa Marilyn1,Schneider Kevin1,Udar Nitin1,Bota Daniela2,Kenney M. Cristina13

Affiliation:

1. Gavin Herbert Eye Institute, University of California, Irvine, Irvine, CA, United States of America

2. Department of Neurology, Neuro-Oncology Division, University of California, Irvine, CA, United States of America

3. Department of Pathology and Laboratory Medicine, University of California, Irvine, CA, United States of America

Abstract

Background Drug therapy yields different results depending on its recipient population. Cisplatin, a commonly used chemotherapeutic agent, causes different levels of resistance and side effects for different patients, but the mechanism(s) are presently unknown. It has been assumed that this variation is a consequence of differences in nuclear (n) DNA, epigenetics, or some external factor(s). There is accumulating evidence that an individual’s mitochondrial (mt) DNA may play a role in their response to medications. Variations within mtDNA can be observed, and an individual’s mtDNA can be categorized into haplogroups that are defined by accumulations of single nucleotide polymorphisms (SNPs) representing different ethnic populations. Methods The present study was conducted on transmitochondrial cytoplasmic hybrids (cybrids) that possess different maternal-origin haplogroup mtDNA from African (L), Hispanic [A+B], or Asian (D) backgrounds. Cybrids were created by fusing Rho0 ARPE-19 cells (lacking mtDNA) with platelets, which contain numerous mitochondria but no nuclei. These cybrid cells were cultured to passage five, treated with cisplatin, incubated for 48 h, then analyzed for cell metabolic activity (tetrazolium dye (MTT) assay), mitochondrial membrane potential (JC-1 assay), cytotoxicity (lactate dehydrogenase (LDH) assay), and gene expression levels for ALK, BRCA1, EGFR, and ERBB2/HER2. Results Results indicated that untreated cybrids with varying mtDNA haplogroups had similar relative metabolic activity before cisplatin treatment. When treated with cisplatin, (1) the decline in metabolic activity was greatest in L (27.4%, p < 0.012) < D (24.86%, p = 0.0001) and [A+B] cybrids (24.67%, p = 0.0285) compared to untreated cybrids; (2) mitochondrial membrane potential remained unchanged in all cybrids (3) LDH production varied between cybrids (L >[A+B], p = 0.0270). (4) The expression levels decreased for ALK in L (p < 0.0001) and [A+B] (p = 0.0001) cybrids but not in D cybrids (p = 0.285); and decreased for EGFR in [A+B] cybrids (p = 0.0246) compared to untreated cybrids. Conclusion Our findings suggest that an individual’s mtDNA background may be associated with variations in their response to cisplatin treatment, thereby affecting the efficiency and the severity of side effects from the treatment.

Funder

Discovery Eye Foundation, Polly and Michael Smith, Edith and Roy Carver, and NEI

Research to Prevent Blindness

Institute for Clinical and Translational Science (ICTS) at University of California Irvine

Publisher

PeerJ

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

Reference56 articles.

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4. A reason why the ERBB2 gene is amplified and not mutated in breast cancer;Birnbaum;Cancer Cell International,2009

5. Recent clinical trials using cisplatin, carboplatin and their combination chemotherapy drugs (review);Boulikas;Oncology Reports,2004

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