Enhancing carboplatin sensitivity in ovarian cancer cells by blocking the mercapturic acid pathway transporter

Author:

Krishna B Madhu1,Ramisetty Sravani K1,Garg Pankaj2,Mohanty Atish1,Wang Edward1,Horne David3,Awasthi Sanjay4,Kulkarni Prakash1,Salgia Ravi1,Singhal Sharad S1ORCID

Affiliation:

1. Department of Medical Oncology, Beckman Research Institute, City of Hope Comprehensive Cancer Center and National Medical Center , Duarte, CA 91010, United States

2. Department of Chemistry, GLA University , Mathura, Uttar Pradesh 281406, India

3. Department of Molecular Medicine, Beckman Research Institute, City of Hope Comprehensive Cancer Center and National Medical Center , Duarte, CA 91010, United States

4. Cayman Health, CTMH Doctors Hospital in Cayman Islands , George Town, Grand Cayman

Abstract

Abstract Ral-binding/interacting protein (RLIP) acts as a transporter that responds to stress and provides protection, specifically against glutathione–electrophile conjugates and xenobiotic toxins. Its increased presence in malignant cells, especially in cancer, emphasizes its crucial antiapoptotic function. This is achieved by selectively regulating the cellular levels of proapoptotic oxidized lipid byproducts. Suppressing the progression of tumors in human xenografts can be achieved by effectively inhibiting RLIP, a transporter in the mercapturic acid pathway, without involving chemotherapy. Utilizing ovarian cancer (OC) cell lines (MDAH2774, OVCAR4, and OVCAR8), we observed that agents targeting RLIP, such as RLIP antisense and RLIP antibodies, not only substantially impeded the viability of OC cells but also remarkably increased their sensitivity to carboplatin. To delve further into the cytotoxic synergy between RLIP antisense, RLIP antibodies, and carboplatin, we conducted investigations in both cell culture and xenografts of OC cells. The outcomes revealed that RLIP depletion via phosphorothioate antisense led to rapid and sustained remissions in established subcutaneous human ovary xenografts. Furthermore, RLIP inhibition by RLIP antibodies exhibited comparable efficacy to antisense and enhanced the effectiveness of carboplatin in MDAH2774 OC xenografts. These investigations underscore RLIP as a central carrier crucial for supporting the survival of cancer cells, positioning it as a suitable focus for cancer treatment.

Funder

National Cancer Institute of the National Institutes of Health

United States Department of Defense

Publisher

Oxford University Press (OUP)

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