Islamabad, 
Jan 18: A small slice of RNA inhibits prostate cancer metastasis by 
suppressing a surface protein commonly found on prostate cancer stem cells. 
miR-34a targets a surface protein common to cancer stem cells and associated 
with tumor development and metastasis.
When the micro RNA stifles CD44, 
it inhibits formation of prostate stem cells. Researchers blocked tumor 
formation, shrunk tumors and inhibited metastasis in mouse models.
A 
research team led by scientists at The University of Texas MD Anderson Cancer 
Center reported January 16 in an advance online publication at Nature 
Medicine.
"Our findings are the first to profile a microRNA expression 
pattern in prostate cancer stem cells and also establish a strong rationale for 
developing the microRNA miR-34a as a new treatment option for prostate cancer," 
said senior author Dean Tang, Ph.D., professor in MD Anderson's Department of 
Molecular Carcinogenesis.
MicroRNAs, or miRNAs, are short, 
single-stranded bits of RNA that regulate the messenger RNA expressed by genes 
to create a protein.
Cancer stem cells are capable of self-renewal, have 
enhanced tumor-initiating ability and are generally more resistant to treatment 
than other cancer cells. They are associated with tumor recurrence and 
metastasis, the lethal spreading of cancer to other organs. These capacities are 
more prevalent in cancer cells that feature a specific cell surface protein 
called CD44, Tang said.
"CD44 has long been linked to promotion of tumor 
development and, especially, to cancer metastasis," Tang said. "Many cancer stem 
cells overexpress this surface adhesion molecule. Another significant finding 
from our study is identifying CD44 itself as a direct and functional target of 
miR-34a."
MicroRNA goes up, CD44 and cancer stem cells fall.
In a 
series of lab experiments with cell lines, human xenograft tumors in mice and 
primary human prostate cancer samples, the researchers demonstrated that miR-34a 
inhibits prostate cancer stem cells by suppressing CD44.
miR-34a is 
greatly reduced in prostate cancer cells that express high levels of CD44 on the 
cell surface. In 18 human prostate tumors, the microRNA was expressed at 25 to 
70 percent of the levels found in cells without CD44. 
Prostate tumors in 
mice that also received miR-34a treatment were one third to half the average 
size of those in control group mice. 
In CD44-positive prostate cancer cell 
lines, treatment with miR-34a resulted in greatly reduced tumor incidence. Most 
dramatically, in one cell line, tumor regeneration was blocked in all 10 treated 
animals, while tumors formed in all 10 animals treated with the control miRNAs. 
Many characteristics of cancer stem cells -- formation of self-renewing 
cells, clonal growth capacity and formation of spheres -- were suppressed when 
miR-34a was overexpressed in prostate cancer cell lines. 
Most 
significantly, intravenous treatment of tumor-bearing mice with synthetic 
miR-34a reduced tumor burden by half in one tumor type. It also steeply reduced 
lung metastases in another tumor type, resulting in increased animal survival. 
Interestingly, the researchers observed a consistent, inverse 
relationship between miR-34a levels and CD44, the surface marker used to enrich 
prostate cancer stem cells. For example, the CD44 protein and CD44-expressing 
cancer cells were reduced in tumors treated with the microRNA. Tumors with 
miR-34a blocked had higher levels of CD44 protein and messenger RNA. 
Finally, knocking down CD44 with a short hairpin RNA produced the same 
results as treating cells with miR-34a did -- reduced tumor development, tumor 
burden and metastases. 
"There are many companies developing 
microRNA-based drugs," Tang said. "Delivery of miRNAs is a challenge, but the 
field is moving fast through the preclinical stage."
Scientists from 
Austin-based Mirna Therapeutics collaborated on the study. Mirna has eight 
microRNAs in preclinical development, including 
miR-34a.
Ends
SA/EN
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MicroRNA suppresses prostate cancer stem cells and metastasis
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