The Proteolytic Activity of Separase in BCR-ABL-positive Cells is Increased by Imatinib

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2012 Aug 8

PMID 22870341

Citations 10

Authors

Wiltrud Haass

Michael Stehle

Stefanie Nittka

Michelle Giehl

Petra Schrotz-King

Alice Fabarius

Wolf-Karsten Hofmann

Wolfgang Seifarth

Affiliations

Soon will be listed here.

Abstract

Separase, an endopeptidase required for the separation of sister-chromatides in mitotic anaphase, triggers centriole disengagement during centrosome duplication. In cancer, separase is frequently overexpressed, pointing to a functional role as an aneuploidy promoter associated with centrosomal amplification and genomic instability. Recently, we have shown that centrosomal amplification and subsequent chromosomal aberrations are a hallmark of chronic myeloid leukemia (CML), increasing from chronic phase (CP) toward blast crisis (BC). Moreover, a functional linkage of p210BCR-ABL tyrosine kinase activity with centrosomal amplification and clonal evolution has been established in long-term cell culture experiments. Unexpectedly, therapeutic doses of imatinib (IM) did not counteract; instead induced similar centrosomal alterations in vitro. We investigated the influence of IM and p210BCR-ABL on Separase as a potential driver of centrosomal amplification in CML. Short-term cell cultures of p210BCR-ABL-negative (NHDF, UROtsa, HL-60, U937), positive (K562, LAMA-84) and inducible (U937p210BCR-ABL/c6 (Tet-ON)) human cell lines were treated with therapeutic doses of IM and analyzed by qRT-PCR, Western blot analysis and quantitative Separase activity assays. Decreased Separase protein levels were observed in all cells treated with IM in a dose dependent manner. Accordingly, in all p210BCR-ABL-negative cell lines, decreased proteolytic activity of Separase was found. In contrast, p210BCR-ABL-positive cells showed increased Separase proteolytic activity. This activation of Separase was consistent with changes in the expression levels of Separase regulators (Separase phosphorylation at serine residue 1126, Securin, CyclinB1 and PP2A). Our data suggest that regulation of Separase in IM-treated BCR-ABL-positive cells occurs on both the protein expression and the proteolytic activity levels. Activation of Separase proteolytic activity exclusively in p210BCR-ABL-positive cells during IM treatment may act as a driving force for centrosomal amplification, contributing to genomic instability, clonal evolution and resistance in CML.

Citing Articles

Gene Expression Pattern of , and Can Potentially Predict Response to TKI First-Line Treatment of Patients with Newly Diagnosed CML.

Christiani E, Naumann N, Weiss C, Spiess B, Kleiner H, Fabarius A Cancers (Basel). 2023; 15(9).

PMID: 37174118 PMC: 10177117. DOI: 10.3390/cancers15092652.

The Activity of Novel BCR-ABL Small-Molecule Degraders Containing Pyrimidine Rings and Their Role in Overcoming Drug Resistance.

Zhang X, Tu L, Chai H, Li Z, Fu Y, Zheng X J Oncol. 2022; 2022:4056398.

PMID: 36349200 PMC: 9637472. DOI: 10.1155/2022/4056398.

Separase activity distribution can be a marker of major molecular response and proliferation of CD34 cells in TKI-treated chronic myeloid leukemia patients.

Spiess B, Kleiner H, Flach J, Fabarius A, Saussele S, Hofmann W Ann Hematol. 2020; 99(5):991-1006.

PMID: 32253454 PMC: 7196950. DOI: 10.1007/s00277-020-04007-4.

Increased separase activity and occurrence of centrosome aberrations concur with transformation of MDS.

Ruppenthal S, Kleiner H, Nolte F, Fabarius A, Hofmann W, Nowak D PLoS One. 2018; 13(1):e0191734.

PMID: 29370237 PMC: 5784974. DOI: 10.1371/journal.pone.0191734.

Separase is a marker for prognosis and mitotic activity in breast cancer.

Gurvits N, Loyttyniemi E, Nykanen M, Kuopio T, Kronqvist P, Talvinen K Br J Cancer. 2017; 117(9):1383-1391.

PMID: 28859055 PMC: 5672940. DOI: 10.1038/bjc.2017.301.

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