@article {Kapoor099655, author = {Aastha Kapoor and Bhushan Thakur and Melissa Monteiro and Alakesh Das and Sejal Desai and Snehal Gaikwad and Amirali B. Bukhari and Pankaj Mogha and Abhijit Majumder and Abhijit De and Pritha Ray and Shamik Sen}, title = {Soft drug-resistant ovarian cancer cells invade via two distinct mechanisms utilizing myosin IIB}, elocation-id = {099655}, year = {2017}, doi = {10.1101/099655}, publisher = {Cold Spring Harbor Laboratory}, abstract = {The failure of chemotherapeutic drugs in treatment of various cancers is attributed to the acquisition of drug resistance. However, the invasion mechanisms of drug-resistant cancer cells remains incompletely understood. Here we address this question from a biophysical perspective by mapping the phenotypic alterations in ovarian cancer cells (OCCs) resistant to cisplatin and paclitaxel. We show that cisplatin-resistant (CisR), paclitaxel-resistant (PacR) and dual drug-resistant (i.e., resistant to both drugs) OCCs are softer and more contractile than drug-sensitive cells. Protease inhibition suppresses invasion of CisR cells but not of PacR and dual cells, suggesting protease-dependent mode of invasion in CisR cells and protease-independent mode in PacR and dual cells. Despite these differences, actomyosin contractility, mediated by the RhoA-ROCK2-Myosin IIB signaling pathway regulates both modes of invasion. Myosin IIB modulates matrix metalloproteinase-9 (MMP-9) secretion in CisR cells and nuclear squeezing in PacR and dual cells, thereby highlighting its importance as a potential therapeutic target for treatment of drug-resistant ovarian cancer cells.Financial Support Authors acknowledge financial support from IIT Bombay Healthcare Initiative, CSIR andDepartment of Biotechnology (Govt. of India) (Grant $\#$ BT/PR14658/MED/31/107/2010).AK and BTwere supported by fellowships from UGC and CSIR respectively (Govt. of India).Authors declare no competing financial interestsAuthor contributions: AK, PR and SS designed the experiments. AK performed most of the experiments and analyzed the data.BT and SG developed drug resistant cell lines and did RT-PCR. MM performed western blot. AD performed AFM experiments. SD performed gelatin zymography. ABB, PM, AM and AD helped with live cell imaging experiments. AK and SS wrote the manuscript. All authors read and approved the final manuscript.Summary statement: This study identifies drug-specific differences in the modes of invasion utilized by ovarian cancer cells, and demonstrates the role of myosin IIB in regulating both modes of invasion.}, URL = {https://www.biorxiv.org/content/early/2017/01/11/099655}, eprint = {https://www.biorxiv.org/content/early/2017/01/11/099655.full.pdf}, journal = {bioRxiv} }