NCK-associated protein 1 regulates metastasis and is a novel prognostic marker for colorectal cancer

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作者
Mi Ri Kwon
Jae Hee Lee
Jin Park
Seok Soon Park
Eun Jin Ju
Eun Jung Ko
Seol Hwa Shin
Ga Won Son
Hye Won Lee
Yeon Joo Kim
Si Yeol Song
Seong-Yun Jeong
Eun Kyung Choi
机构
[1] University of Ulsan College of Medicine,Department of Medical Science, Asan Medical Institute of Convergence Science and Technology, Asan Medical Center
[2] ASAN Medical Center,Asan Institute for Life Sciences
[3] ASAN Medical Center,Asan Preclinical Evaluation Center for Cancer Therapeutix
[4] University of Ulsan College of Medicine,Department of Radiation Oncology, ASAN Medical Center
[5] University of Ulsan College of Medicine,Department of Convergence Medicine, ASAN Medical Center
[6] Samsung Bioepis Co.,Quality Evaluation Team
[7] Ltd,undefined
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Metastatic colorectal cancer (CRC) remains a substantial problem for mortality and requires screening and early detection efforts to increase survival. Epithelial-mesenchymal transition (EMT) and circulation of tumor cells in the blood play important roles in metastasis. To identify a novel target for metastasis of CRC, we conducted a gene microarray analysis using extracted RNA from the blood of preclinical models. We found that NCK-associated protein 1 (NCKAP1) was significantly increased in the blood RNA of patient-derived xenograft (PDX) models of colon cancer. In the NCKAP1 gene knockdown-induced human colon cancer cell lines HCT116 and HT29, there was a reduced wound healing area and significant inhibition of migration and invasion. As the result of marker screening for cytoskeleton and cellular interactions, CRC treated with siRNA of NCKAP1 exhibited significant induction of CDH1 and phalloidin expression, which indicates enhanced adherent cell junctions and cytoskeleton. In HCT116 cells with a mesenchymal state induced by TGFβ1, metastasis was inhibited by NCKAP1 gene knockdown through the inhibition of migration, and there was increased CTNNB1 expression and decreased FN expression. We established metastasis models for colon cancer to liver transition by intrasplenic injection shRNA of NCKAP1-transfected HCT116 cells or by implanting tumor tissue generated with the cells on cecal pouch. In metastasis xenograft models, tumor growth and liver metastasis were markedly reduced. Taken together, these data demonstrate that NCKAP1 is a novel gene regulating EMT that can contribute to developing a diagnostic marker for the progression of metastasis and new therapeutics for metastatic CRC treatment.
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