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Literature DB >> 28829429

Establishing Dual Resistance to EGFR-TKI and MET-TKI in Lung Adenocarcinoma Cells In Vitro with a 2-step Dose-escalation Procedure.

Toshimitsu Yamaoka¹, Motoi Ohba², Satoru Arata³, Tohru Ohmori².

Abstract

Drug resistance is a major challenge in cancer therapy. The generation of resistant sublines in vitro is necessary for discovering novel mechanisms to overcome this challenge. Here, a 2-step dose-escalation method for establishing dual-resistance to an epidermal growth factor receptor (EGFR)-tyrosine kinase inhibitor (TKI), gefitinib, and a MET-TKI, PHA665752, is described. This method is based on simple stepwise dose-escalation of inhibitors for inducing acquired resistance in cell lines. The alternate method for generating resistant sublines involves exposing the cells to high concentrations of the inhibitor in one step. The stepwise dose-escalation method has a higher possibility of successfully inducing acquired resistance than this method. Activating EGFR mutations are biomarkers of a response to treatment with EGFR-TKI, which is an applied first-line treatment for non-small cell lung cancers (NSCLC) that harbor these mutations. However, despite reports of effective responses, the use of EGFR-TKI is limited because tumors inevitably acquire resistance. The major mechanisms behind EGFR-TKI resistance include a secondary mutation at the gatekeeper site, T790M in exon 20 of EGFR, and a bypass signal of MET. Thus, a potential solution for this issue would be a combination of EGFR-TKI and MET-TKI. This combined treatment has been shown to be effective in an in vitro study model. Acquired gefitinib-resistance was established through MET-amplification by stepwise dose-escalation of gefitinib for 12 months, and a cell line named PC-9MET1000 was generated in a previous study. To further investigate the mechanisms of acquired MET-TKI and EGFR-TKI resistance, a MET-TKI, PHA665752, was administered to these cells with stepwise dose-escalation in the presence of gefitinib for 12 months. This protocol has also been successfully applied for a number of combination therapies to establish acquired resistance to other inhibitor molecules.

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Year: 2017 PMID： 28829429 PMCID： PMC5614313 DOI： 10.3791/55967

Source DB: PubMed Journal: J Vis Exp ISSN： 1940-087X Impact factor: 1.355

20 in total

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Authors: Kazuhiko Shien; Shinichi Toyooka; Hiromasa Yamamoto; Junichi Soh; Masaru Jida; Kelsie L Thu; Shinsuke Hashida; Yuho Maki; Eiki Ichihara; Hiroaki Asano; Kazunori Tsukuda; Nagio Takigawa; Katsuyuki Kiura; Adi F Gazdar; Wan L Lam; Shinichiro Miyoshi
Journal: Cancer Res Date: 2013-03-29 Impact factor: 12.701

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Authors: T Mosmann
Journal: J Immunol Methods Date: 1983-12-16 Impact factor: 2.303

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Journal: Oncogene Date: 2010-02-01 Impact factor: 9.867

4. Establishment of three cisplatin-resistant endometrial cancer cell lines using two methods of cisplatin exposure.

Authors: Yasukazu Sagawa; Atsuya Fujitoh; Hirotaka Nishi; Hiroe Ito; Tamaki Yudate; Keiichi Isaka
Journal: Tumour Biol Date: 2010-11-27

5. Novel mutations of the MET proto-oncogene in papillary renal carcinomas.

Authors: L Schmidt; K Junker; N Nakaigawa; T Kinjerski; G Weirich; M Miller; I Lubensky; H P Neumann; H Brauch; J Decker; C Vocke; J A Brown; R Jenkins; S Richard; U Bergerheim; B Gerrard; M Dean; W M Linehan; B Zbar
Journal: Oncogene Date: 1999-04-08 Impact factor: 9.867

6. Novel mutation in the ATP-binding site of the MET oncogene tyrosine kinase in a HPRCC family.

Authors: M Olivero; G Valente; A Bardelli; P Longati; N Ferrero; C Cracco; C Terrone; S Rocca-Rossetti; P M Comoglio; M F Di Renzo
Journal: Int J Cancer Date: 1999-08-27 Impact factor: 7.396

7. EGF receptor gene mutations are common in lung cancers from "never smokers" and are associated with sensitivity of tumors to gefitinib and erlotinib.

Authors: William Pao; Vincent Miller; Maureen Zakowski; Jennifer Doherty; Katerina Politi; Inderpal Sarkaria; Bhuvanesh Singh; Robert Heelan; Valerie Rusch; Lucinda Fulton; Elaine Mardis; Doris Kupfer; Richard Wilson; Mark Kris; Harold Varmus
Journal: Proc Natl Acad Sci U S A Date: 2004-08-25 Impact factor: 11.205

8. EGFR mutations in lung cancer: correlation with clinical response to gefitinib therapy.

Authors: J Guillermo Paez; Pasi A Jänne; Jeffrey C Lee; Sean Tracy; Heidi Greulich; Stacey Gabriel; Paula Herman; Frederic J Kaye; Neal Lindeman; Titus J Boggon; Katsuhiko Naoki; Hidefumi Sasaki; Yoshitaka Fujii; Michael J Eck; William R Sellers; Bruce E Johnson; Matthew Meyerson
Journal: Science Date: 2004-04-29 Impact factor: 47.728

9. Acquired Resistance Mechanisms to Combination Met-TKI/EGFR-TKI Exposure in Met-Amplified EGFR-TKI-Resistant Lung Adenocarcinoma Harboring an Activating EGFR Mutation.

Authors: Toshimitsu Yamaoka; Tohru Ohmori; Motoi Ohba; Satoru Arata; Yasunari Kishino; Yasunori Murata; Sojiro Kusumoto; Hiroo Ishida; Takao Shirai; Takashi Hirose; Tsukasa Ohnishi; Yasutsuna Sasaki
Journal: Mol Cancer Ther Date: 2016-09-09 Impact factor: 6.261

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Authors: James Bean; Cameron Brennan; Jin-Yuan Shih; Gregory Riely; Agnes Viale; Lu Wang; Dhananjay Chitale; Noriko Motoi; Janos Szoke; Stephen Broderick; Marissa Balak; Wen-Cheng Chang; Chong-Jen Yu; Adi Gazdar; Harvey Pass; Valerie Rusch; William Gerald; Shiu-Feng Huang; Pan-Chyr Yang; Vincent Miller; Marc Ladanyi; Chih-Hsin Yang; William Pao
Journal: Proc Natl Acad Sci U S A Date: 2007-12-18 Impact factor: 11.205

2 in total

Review 1. Receptor Tyrosine Kinase-Targeted Cancer Therapy.

Authors: Toshimitsu Yamaoka; Sojiro Kusumoto; Koichi Ando; Motoi Ohba; Tohru Ohmori
Journal: Int J Mol Sci Date: 2018-11-06 Impact factor: 5.923

2. A Cell Double-Barcoding System for Quantitative Evaluation of Primary Tumors and Metastasis in Animals That Uncovers Clonal-Specific Anti-Cancer Drug Effects.

Authors: Arkadi Hesin; Santosh Kumar; Valid Gahramanov; Maria Becker; Maria Vilenchik; Ilya Alexandrov; Julia Yaglom; Michael Y Sherman
Journal: Cancers (Basel) Date: 2022-03-08 Impact factor: 6.639

2 in total