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Series GSE5822

Query DataSets for GSE5822

Status

Public on Sep 14, 2006

Title

Rapamycin treated CEM-C1 cells 3 hours

Organism

Homo sapiens

Experiment type

Expression profiling by array

Summary

Drug resistance remains a major obstacle to successful cancer treatment. Here we use a novel approach to identify rapamycin as a glucocorticoid resistance reversal agent. A database of drug-associated gene expression profiles was screened for molecules whose profile overlapped with a gene expression signature of glucocorticoid (GC) sensitivity/resistance in Acute Lymphoblastic Leukemia (ALL) cells. The screen indicated the mTOR inhibitor rapamycin profile matched the signature of GC-sensitivity. We thus tested the hypothesis that rapamycin would induce GC sensitivity in lymphoid malignancy cells, and found that it sensitized cells to glucocorticoid induced apoptosis via modulation of antiapoptotic MCL1. These data indicate that MCL1 is an important regulator of GC-induced apoptosis, and that the combination of rapamycin and glucocorticoids has potential utility in ALL. Furthermore this approach represents a novel strategy for identification of promising combination therapies for cancer.
Keywords: drug treatment

Overall design

CEM-C1 cells were treated with 10 nM rapamycin for 3 hours and compared to DMSO treated cells

Citation(s)

17010674

Submission date

Sep 13, 2006

Last update date

Aug 10, 2018

Contact name

Scott A. Armstrong

E-mail(s)

scott.armstrong@childrens.harvard.edu