MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.

MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.

The therapeutic options for advanced gastric cancer are still limited. Several drugs targeting the epidermal growth factor receptor family have been developed. So far, the HER2 antibody trastuzumab is the only drug targeting the HER-family that is available to gastric cancer patients. The pan-HER in...

Full description

Bibliographic Details
Main Authors: Karolin Ebert, Julian Mattes, Thomas Kunzke, Gwen Zwingenberger, Birgit Luber
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0223225
id doaj-aeb2ed7557e444b8b678ebd28722d976
record_format Article
spelling doaj-aeb2ed7557e444b8b678ebd28722d9762021-03-03T21:21:34ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01149e022322510.1371/journal.pone.0223225MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.Karolin EbertJulian MattesThomas KunzkeGwen ZwingenbergerBirgit LuberThe therapeutic options for advanced gastric cancer are still limited. Several drugs targeting the epidermal growth factor receptor family have been developed. So far, the HER2 antibody trastuzumab is the only drug targeting the HER-family that is available to gastric cancer patients. The pan-HER inhibitor afatinib is currently investigated in clinical trials and shows promising results in cell culture experiments and patient-derived xenograft (PDX) models. However, some cell lines do not respond to afatinib treatment. The determination of resistance factors in these cell lines can help to find the best treatment option for gastric cancer patients. In this study, we analyzed the role of MET as a resistance factor for afatinib therapy in a gastric cancer cell line. MET expression in afatinib-resistant MET-amplified Hs746T cells was reduced by means of siRNA transfection. The effects of MET knockdown on signal transduction, cell proliferation and motility were examined. In addition to the manual assessment of cell motility, a computational motility analysis involving parameters such as (approximate) average speed, displacement entropy or radial effectiveness was realized. Moreover, the impact of afatinib was compared between MET knockdown cells and control cells. MET knockdown in Hs746T cells resulted in impaired signal transduction and reduced cell proliferation and motility. Moreover, the afatinib resistance of Hs746T cells was reversed after MET knockdown. Therefore, the amplification of MET is confirmed as a resistance factor in gastric cancer cells. Whether MET is a useful resistance marker for afatinib therapy or other HER-targeting drugs in patients should be investigated in clinical trials.https://doi.org/10.1371/journal.pone.0223225
collection DOAJ
language English
format Article
sources DOAJ
author Karolin Ebert
Julian Mattes
Thomas Kunzke
Gwen Zwingenberger
Birgit Luber
spellingShingle Karolin Ebert
Julian Mattes
Thomas Kunzke
Gwen Zwingenberger
Birgit Luber
MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
PLoS ONE
author_facet Karolin Ebert
Julian Mattes
Thomas Kunzke
Gwen Zwingenberger
Birgit Luber
author_sort Karolin Ebert
title MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
title_short MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
title_full MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
title_fullStr MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
title_full_unstemmed MET as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
title_sort met as resistance factor for afatinib therapy and motility driver in gastric cancer cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2019-01-01
description The therapeutic options for advanced gastric cancer are still limited. Several drugs targeting the epidermal growth factor receptor family have been developed. So far, the HER2 antibody trastuzumab is the only drug targeting the HER-family that is available to gastric cancer patients. The pan-HER inhibitor afatinib is currently investigated in clinical trials and shows promising results in cell culture experiments and patient-derived xenograft (PDX) models. However, some cell lines do not respond to afatinib treatment. The determination of resistance factors in these cell lines can help to find the best treatment option for gastric cancer patients. In this study, we analyzed the role of MET as a resistance factor for afatinib therapy in a gastric cancer cell line. MET expression in afatinib-resistant MET-amplified Hs746T cells was reduced by means of siRNA transfection. The effects of MET knockdown on signal transduction, cell proliferation and motility were examined. In addition to the manual assessment of cell motility, a computational motility analysis involving parameters such as (approximate) average speed, displacement entropy or radial effectiveness was realized. Moreover, the impact of afatinib was compared between MET knockdown cells and control cells. MET knockdown in Hs746T cells resulted in impaired signal transduction and reduced cell proliferation and motility. Moreover, the afatinib resistance of Hs746T cells was reversed after MET knockdown. Therefore, the amplification of MET is confirmed as a resistance factor in gastric cancer cells. Whether MET is a useful resistance marker for afatinib therapy or other HER-targeting drugs in patients should be investigated in clinical trials.
url https://doi.org/10.1371/journal.pone.0223225
work_keys_str_mv AT karolinebert metasresistancefactorforafatinibtherapyandmotilitydriveringastriccancercells
AT julianmattes metasresistancefactorforafatinibtherapyandmotilitydriveringastriccancercells
AT thomaskunzke metasresistancefactorforafatinibtherapyandmotilitydriveringastriccancercells
AT gwenzwingenberger metasresistancefactorforafatinibtherapyandmotilitydriveringastriccancercells
AT birgitluber metasresistancefactorforafatinibtherapyandmotilitydriveringastriccancercells
_version_ 1714817376751452160

Similar Items