TY - JOUR
T1 - Cdc42-dependent modulation of rigidity sensing and cell spreading in tumor repopulating cells
AU - Chowdhury, Farhan
AU - Doğanay, Sultan
AU - Leslie, Benjamin J.
AU - Singh, Rishi
AU - Amar, Kshitij
AU - Talluri, Bhavana
AU - Park, Seongjin
AU - Wang, Ning
AU - Ha, Taekjip
N1 - Publisher Copyright:
© 2018 Elsevier Inc.
PY - 2018/6/7
Y1 - 2018/6/7
N2 - Recently, a robust mechanical method has been established to isolate a small subpopulation of highly tumorigenic tumor repopulating cells (TRCs) from parental melanoma cells. In order to characterize the molecular and mechanical properties of TRCs, we utilized the tension gauge tether (TGT) single-molecule platform and investigated force requirements during early cell spreading events. TRCs required the peak single molecular tension of around 40 pN through integrins for initial adhesion like the parental control cells, but unlike the control cells, they did not spread and formed very few mature focal adhesions (FAs). Single molecule resolution RNA quantification of three Rho GTPases showed that downregulation of Cdc42, but not Rac1, is responsible for the unusual biophysical features of TRCs and that a threshold level of Cdc42 transcripts per unit cell area is required to initiate cell spreading. Cdc42 overexpression rescued TRC spreading through FA formation and restored the sensitivity to tension cues such that TRCs, like parental control cells, increase cell spreading with increasing single-molecular tension cues. Our single molecule studies identified an unusual biophysical feature of suppressed spreading of TRCs that may enable us to distinguish TRC population from a pool of heterogeneous tumor cell population.
AB - Recently, a robust mechanical method has been established to isolate a small subpopulation of highly tumorigenic tumor repopulating cells (TRCs) from parental melanoma cells. In order to characterize the molecular and mechanical properties of TRCs, we utilized the tension gauge tether (TGT) single-molecule platform and investigated force requirements during early cell spreading events. TRCs required the peak single molecular tension of around 40 pN through integrins for initial adhesion like the parental control cells, but unlike the control cells, they did not spread and formed very few mature focal adhesions (FAs). Single molecule resolution RNA quantification of three Rho GTPases showed that downregulation of Cdc42, but not Rac1, is responsible for the unusual biophysical features of TRCs and that a threshold level of Cdc42 transcripts per unit cell area is required to initiate cell spreading. Cdc42 overexpression rescued TRC spreading through FA formation and restored the sensitivity to tension cues such that TRCs, like parental control cells, increase cell spreading with increasing single-molecular tension cues. Our single molecule studies identified an unusual biophysical feature of suppressed spreading of TRCs that may enable us to distinguish TRC population from a pool of heterogeneous tumor cell population.
KW - Cell adhesion and spreading
KW - Focal adhesions
KW - Tension gauge tethers
KW - Tumor repopulating cells
KW - smFISH
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U2 - 10.1016/j.bbrc.2018.04.085
DO - 10.1016/j.bbrc.2018.04.085
M3 - Article
C2 - 29673588
AN - SCOPUS:85046130777
SN - 0006-291X
VL - 500
SP - 557
EP - 563
JO - Biochemical and Biophysical Research Communications
JF - Biochemical and Biophysical Research Communications
IS - 3
ER -