UM171 suppresses breast cancer progression by inducing KLF2-Reference-Cited by-同舟云学术

UM171 suppresses breast cancer progression by inducing KLF2

Published:2024-02-12 Issue: Volume: Page:
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Author:

Ran Xiaojuan¹,Hu Anling²,Kuang Yi²,Wang Chunlin²,Liu Wuling²,Xiao Xiao²,Zacksenhaus Eldad³,Yu Xiangdi¹,Ben-David Yaacov²

Affiliation:

1. Guizhou University of Traditional Chinese Medicine

2. Guizhou Medical University

3. University of Toronto

Abstract

Purpose: Breast cancer is the most frequent cancer in women with significant death rate. Morbidity is associated with drug resistance and metastasis. Development of novel drugs is unmet need. The aim of this study is to show potent anti-neoplastic activity of the UM171 compound on breast cancer cells and its mechanism of action. Methods: The inhibitory effect of UM171 on several breast cancer (BC) cell lines was examined using MTT and colony forming assays. Cell cycle and apoptosis assays were utilized to determine the effect of UM171 on BC cell proliferation and survival. Wound healing scratch and transwell migration assays were used to examine the migration of BC cell lines in culture. Xenograft of mouse model with 4T1 cells was used to determine inhibitory effect of UM171 in vivo. Q-RT-PCR and western blotting were used to determine the expression level of genes effected by UM171. Lentivirus-mediated shRNA were used to knockdown the expression of KLF2 in BC cells. Results: UM171 was previously identified as a potent agonist of human hematopoietic stem cell renewal and inhibitor of leukemia. In this study, UM171 was shown to inhibit the growth of multiple breast cancer cell lines in culture. UM171-mediated growth inhibition was associated with the induction of apoptosis, G2/M cell cycle arrest, lower colony forming capacity and reduced motility. In a xenotransplantation model of mouse triple negative breast cancer 4T1 cells injected into syngeneic BALB/c mice, UM171 strongly inhibited tumor growth at a level comparable to paclitaxel. UM171 increased the expression of the three PIM genes (PIM1-3) in breast cancer cells. Moreover, UM171 strongly induced the expression of the tumor suppressor gene KLF2 and cell cycle inhibitor P21^CIP¹. Accordingly, knockdown of KLF2 using lentivirus-mediated shRNA significantly attenuated the growth suppressor activity of UM171. As PIM1-3 act as oncogenes and are involved in breast cancer progression, induction of these kinases likely impedes the inhibitory effect of KLF2 induction by UM171. Accordingly, combination of UM171 with a PAN-PIM inhibitor LGH447 significantly reduced tumor growth in culture. Conclusion: These results suggested that UM171 inhibited breast cancer progression in part through activation of KLF2 and P21. Combination of UM171 with a PAN-PIM inhibitor offer a novel therapy for aggressive forms of breast cancer.

Publisher

Research Square Platform LLC

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