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25 May 2021 Polyploid giant cancer cells and ovarian cancer: new insights into mitotic regulators and polyploidy
JoAnne S. Richards, Nicholes R. Candelaria, Rainer B. Lanz
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Abstract

Current first-line treatment of patients with high-grade serous ovarian cancer (HGSOC) involves the use of cytotoxic drugs that frequently lead to recurrent tumors exhibiting increased resistance to the drugs and poor patient survival. Strong evidence is accumulating to show that HGSOC tumors and cell lines contain a subset of cells called polyploidy giant cancer cells (PGCCs) that act as stem-like, self-renewing cells. These PGCCs appear to play a key role in tumor progression by generating drug-resistant progeny produced, in part, as a consequence of utilizing a modified form of mitosis known as endoreplication. Thus, developing drugs to target PGCCs and endoreplication may be an important approach for reducing the appearance of drug-resistant progeny. In the review, we discuss newly identified regulatory factors that impact mitosis and which may be altered or repurposed during endoreplication in PGCCs. We also review recent papers showing that a single PGCC can give rise to tumors in vivo and spheroids in culture. To illustrate some of the specific features of PGCCs and factors that may impact their function and endoreplication compared to mitosis, we have included immunofluorescent images co-localizing p53 and specific mitotic regulatory, phosphoproteins in xenografts derived from commonly used HGSOC cell lines.

Summary sentence

Cytotoxic drugs frequently used in ovarian cancer treatment impact tumor cell cycle progression and the emergence of polyploid cells where genetic and epigenetic events ultimately lead to drug-resistant diploid progeny.

Graphical Abstract

© The Author(s) 2021. Published by Oxford University Press on behalf of Society for the Study of Reproduction. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com
JoAnne S. Richards, Nicholes R. Candelaria, and Rainer B. Lanz "Polyploid giant cancer cells and ovarian cancer: new insights into mitotic regulators and polyploidy," Biology of Reproduction 105(2), 305-316, (25 May 2021). https://doi.org/10.1093/biolre/ioab102
Received: 2 March 2021; Accepted: 22 May 2021; Published: 25 May 2021
KEYWORDS
cytotoxic stress
endoreplication
mitosis
ovarian cancer
p53
polyploid giant cancer cells
polyploidy
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