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CAGE Binds to Beclin1 Regulates Autophagic Flux and CAGE-Derived Peptide Confers Sensitivity to Anti-cancer Drugs in Non-small Cell Lung Cancer Cells

机译：笼结合Beclin1调节自噬通量和CAGE衍生肽赋予非小细胞肺癌细胞抗癌药敏感性。

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摘要

The objective of this study was to determine the role of CAGE, a cancer/testis antigen, in resistance of non-small cell lung cancers to anti-cancer drugs. Erlotinib-resistant PC-9 cells (PC-9/ER) with EGFR mutations (ex 19 del + T790M of EGFR), showed higher level of autophagic flux than parental sensitive PC-9 cells. Erlotinib and osimertinib increased autophagic flux and induced the binding of CAGE to Beclin1 in PC-9 cells. The inhibition or induction of autophagy regulated the binding of CAGE to Beclin1 and the responses to anti-cancer drugs. CAGE showed binding to HER2 while HER2 was necessary for binding of CAGE to Beclin1. CAGE was responsible for high level of autophagic flux and resistance to anti-cancer drugs in PC-9/ER cells. A peptide corresponding to the DEAD box domain of CAGE, ²⁶⁶AQTGTGKT²⁷³, enhanced the sensitivity of PC-9/ER cells to erlotinib and osimertinib, inhibited the binding of CAGE to Beclin1 and regulated autophagic flux in PC-9/ER cells. Mutant CAGE-derived peptide ²⁶⁶AQTGTGAT²⁷³ or ²⁶⁶AQTGTGKA²⁷³ did not affect autophagic flux or the binding of CAGE to Beclin1. AQTGTGKT peptide showed binding to CAGE, but not to Beclin1. FITC-AQTGTGKT peptide showed co-localization with CAGE. AQTGTGKT peptide decreased tumorigenic potentials of PC-9/ER and H1975 cells, non-small cell lung cancer (NSCLC) cells with EGFR mutation (L885R/T790M), by inhibiting autophagic fluxand inhibiting the binding of CAGE to Beclin1. AQTGTGKT peptide also enhanced the sensitivity of H1975 cells to anti-cancer drugs. AQTGTGKT peptide showed tumor homing potential based on ex vivo homing assays of xenograft of H1975 cells. AQTGTGKT peptide restored expression levels of miR-143-3p and miR-373-5p, decreased autophagic flux and conferred sensitivity to anti-cancer drugs. These results present evidence that combination of anti-cancer drug with CAGE-derived peptide could overcome resistance of non-small cell lung cancers to anti-cancer drugs.

机译：这项研究的目的是确定癌症/睾丸抗原CAGE在非小细胞肺癌对抗癌药物耐药中的作用。具有EGFR突变（EGFR的19 del + T790M）的耐厄洛替尼的PC-9细胞（PC-9 / ER）显示出比亲代敏感的PC-9细胞更高的自噬通量。厄洛替尼和奥西替尼增加PC-9细胞中自噬通量并诱导CAGE与Beclin1结合。自噬的抑制或诱导调节了CAGE与Beclin1的结合以及对抗癌药物的反应。 CAGE显示与HER2结合，而HER2是CAGE与Beclin1结合所必需的。 CAGE导致PC-9 / ER细胞中高水平的自噬通量和对抗癌药物的耐药性。对应于CAGE DEAD盒结构域的肽^{266 AQTGTGKT ^{273 增强PC-9 / ER细胞对厄洛替尼和奥西替尼的敏感性，抑制CAGE与Beclin1和调节PC-9 / ER细胞中的自噬通量。突变的CAGE衍生肽^{266 AQTGTGAT ^{273 或^{266 AQTGTGKA ^{273 不影响自噬通量或CAGE的结合到Beclin1。 AQTGTGKT肽显示与CAGE结合，但不与Beclin1结合。 FITC-AQTGTGKT肽显示与CAGE共定位。 AQTGTGKT肽通过抑制自噬通量和抑制CAGE与Beclin1的结合，降低了PC-9 / ER和H1975细胞，具有EGFR突变的非小细胞肺癌（NSCLC）细胞（L885R / T790M）的致癌潜力。 AQTGTGKT肽还增强了H1975细胞对抗癌药的敏感性。基于H1975细胞异种移植的离体归巢测定，AQTGTGKT肽显示出肿瘤归巢潜力。 AQTGTGKT肽恢复了miR-143-3p和miR-373-5p的表达水平，降低了自噬通量并赋予了对抗癌药的敏感性。这些结果表明，抗癌药与CAGE衍生肽的组合可以克服非小细胞肺癌对抗癌药的耐药性。}}}}}}

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期刊名称 Frontiers in Oncology
作者
Minjeong Yeon; Jaewhan Byun; Hyuna Kim; Misun Kim; Hyun Suk Jung; Doyong Jeon; Youngmi Kim; Dooil Jeoung;
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作者单位

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年(卷),期 2018(8),-1
年度 2018
页码 599
总页数 16
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
anti-cancer drug-resistance autophagy cancer/testis antigen CAGE CAGE-derived peptide non-small cell lung cancers;

机译：抗癌药耐药性;自噬;癌症/睾丸抗原CAGE;CAGE衍生肽;非小细胞肺癌;

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专利

1. Expression profiles of non-small cell lung cancers on cDNA microarrays: Identification of genes for prediction of lymph-node metastasis and sensitivity to anti-cancer drugs [J] . Takefumi Kikuchi, Yataro Daigo, Toyomasa Katagiri, Oncogene . 2003,第14期

机译：非小细胞肺癌在cDNA微阵列上的表达谱：预测淋巴结转移和对抗癌药物敏感性的基因鉴定
2. Quantifying the sensitivities of EGF receptor (EGFR) tyrosine kinase inhibitors in drug resistant non-small cell lung cancer (NSCLC) cells using hydrogel-based peptide array [J] . Ghosh G., Yan X., Lee A.G., Biosensors & Bioelectronics: The International Journal for the Professional Involved with Research, Technology and Applications of Biosensers and Related Devices . 2010,第2期

机译：使用基于水凝胶的肽阵列定量分析EGF受体（EGFR）酪氨酸激酶抑制剂在耐药性非小细胞肺癌（NSCLC）细胞中的敏感性
3. Identification of a novel autophagic inhibitor cepharanthine to enhance the anti-cancer property of dacomitinib in non-small cell lung cancer [J] . Tang Zheng-Hai, Cao Wen-Xiang, Guo Xia, Cancer letters . 2018,第期

机译：鉴定新型自噬抑制剂Cepharanthine，以提高非小细胞肺癌Dacomitinib的抗癌性能
4. DEVELOPMENT OF A LIPOSOMAL DRUG CARRIER TO DELIVER SUFFICIENT ANTI-CANCER DRUG INTO MULTI DRUG RESISTANT (MDR)-SMALL CELL LUNG CANCER (SCLC) [C] . T. Kobavashi, Y. Okada, T. Ishida, International symposium on controlled release of bioactive materials;Consumer diversified products conference . 2001

机译：脂质体药物载体的开发，以将有效的抗癌药物输送到抗多药（MDR）-小细胞肺癌（SCLC）中
5. Elucidating the epigenetic mechanisms contributing to the anti-cancer efficacy of silibinin in non-small cell lung cancer. [D] . Mateen, Samiha. 2012

机译：阐明表观遗传机制有助于水飞蓟宾在非小细胞肺癌中的抗癌功效。
6. Quantifying the sensitivities of EGF receptor (EGFR) tyrosine kinase inhibitors in drug resistant non-small cell lung cancer (NSCLC) cells using hydrogel-based peptide array [O] . Gargi Ghosh, Eric Yan, Andrew G. Lee, -1

机译：使用水凝胶基肽阵列量化抗毒性非小细胞肺癌（NSCLC）细胞抗药性非小细胞肺癌（NSCLC）细胞的敏感性
7. Quantifying the sensitivities of EGF receptor (EGFR) tyrosine kinase inhibitors in drug resistant non-small cell lung cancer (NSCLC) cells using hydrogel-based peptide array [O] . Gargi Ghosh, Xiaoliang Yan, Andrew G. Lee, 2010

机译：使用水凝胶基肽阵列量化抗毒性非小细胞肺癌（NSCLC）细胞抗药性非小细胞肺癌（NSCLC）细胞的敏感性

CAGE Binds to Beclin1 Regulates Autophagic Flux and CAGE-Derived Peptide Confers Sensitivity to Anti-cancer Drugs in Non-small Cell Lung Cancer Cells

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