TY - JOUR
T1 - Premalignant PTEN-deficient thymocytes activate microRNAs miR-146a and miR-146b as a cellular defense against malignant transformation
AU - Burger, Megan L.
AU - Xue, Ling
AU - Sun, Yuefang
AU - Kang, Chulho
AU - Winoto, Astar
PY - 2014/6/26
Y1 - 2014/6/26
N2 - Cancer develops by a multistep process during which cells acquire characteristics that allow them to evade apoptosis and proliferate unchecked. Sequential acquisition of genetic alterations drives this processbut alsocauses cellular stress, frequently prompting cells to enter a premalignant period during which they mount a defense against transformation. T cell-specific deletion of the tumor suppressor PTEN in mice induces premalignancy in the thymus and development of CD4+ T-cell lymphomas in the periphery. Here we sought to identify factors mediating the cellular defense against transformation during the premalignant period. We identified several microRNAs upregulated specifically inpremalignant thymocytes, including miR-146a,miR-146b,andthemiR-183/96/182 cluster. CD4-driven T cell-specific transgenic overexpression of mir-146a and mir-146b significantly delayed PTEN-deficient lymphomagenesis and delayed c-myc oncogene induction, a key driver of transformation in PTEN-deficient T-cell malignancies. We found that miR- 146a and miR-146b targeting of Traf6 attenuates TCR signaling in the thymus and inhibits downstream NF-ΚB-dependent induction of c-myc. Additionally, c-myc repression in mature CD4 T cells by miR-146b impaired TCR-mediated proliferation. Hence,we have identified 2 miRNAs that are upregulated as part of the cellular responseagainst transformationthat,whenoverrepresented, can effectively inhibit progression tomalignancy in the context of PTEN deficiency.
AB - Cancer develops by a multistep process during which cells acquire characteristics that allow them to evade apoptosis and proliferate unchecked. Sequential acquisition of genetic alterations drives this processbut alsocauses cellular stress, frequently prompting cells to enter a premalignant period during which they mount a defense against transformation. T cell-specific deletion of the tumor suppressor PTEN in mice induces premalignancy in the thymus and development of CD4+ T-cell lymphomas in the periphery. Here we sought to identify factors mediating the cellular defense against transformation during the premalignant period. We identified several microRNAs upregulated specifically inpremalignant thymocytes, including miR-146a,miR-146b,andthemiR-183/96/182 cluster. CD4-driven T cell-specific transgenic overexpression of mir-146a and mir-146b significantly delayed PTEN-deficient lymphomagenesis and delayed c-myc oncogene induction, a key driver of transformation in PTEN-deficient T-cell malignancies. We found that miR- 146a and miR-146b targeting of Traf6 attenuates TCR signaling in the thymus and inhibits downstream NF-ΚB-dependent induction of c-myc. Additionally, c-myc repression in mature CD4 T cells by miR-146b impaired TCR-mediated proliferation. Hence,we have identified 2 miRNAs that are upregulated as part of the cellular responseagainst transformationthat,whenoverrepresented, can effectively inhibit progression tomalignancy in the context of PTEN deficiency.
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U2 - 10.1182/blood-2013-11-539411
DO - 10.1182/blood-2013-11-539411
M3 - Article
C2 - 24735967
AN - SCOPUS:84903640883
SN - 0006-4971
VL - 123
SP - 4089
EP - 4100
JO - Blood
JF - Blood
IS - 26
ER -