The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1

PURPOSE: Angiogenesis is an important mediator in tumor progression. Vascular endothelial growth factor (VEGF) is one of the major cytokines that can influence angiogenesis. However, the potential mechanism of tumor growth inhibition through anti-VEGF agents is still unclear. This study was performe...

Descripción completa

Detalles Bibliográficos
Autores principales: Li, Jiao, Cui, Yan, Wang, Qin, Guo, Dadong, Pan, Xuemei, Wang, Xingrong, Bi, Hongsheng, Chen, Wei, Liu, Zhengfeng, Zhao, Shengya
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4021672/
https://www.ncbi.nlm.nih.gov/pubmed/24868139
_version_ 1782316281168396288
author Li, Jiao
Cui, Yan
Wang, Qin
Guo, Dadong
Pan, Xuemei
Wang, Xingrong
Bi, Hongsheng
Chen, Wei
Liu, Zhengfeng
Zhao, Shengya
author_facet Li, Jiao
Cui, Yan
Wang, Qin
Guo, Dadong
Pan, Xuemei
Wang, Xingrong
Bi, Hongsheng
Chen, Wei
Liu, Zhengfeng
Zhao, Shengya
author_sort Li, Jiao
collection PubMed
description PURPOSE: Angiogenesis is an important mediator in tumor progression. Vascular endothelial growth factor (VEGF) is one of the major cytokines that can influence angiogenesis. However, the potential mechanism of tumor growth inhibition through anti-VEGF agents is still unclear. This study was performed to examine whether ranibizumab could inhibit malignant melanoma growth in vitro and to determine the safety of ranibizumab on human adult retinal pigment epithelium cell line (ARPE-19 cells). METHODS: Malignant melanoma cells obtained from a clinic were cultured in vitro. VEGF concentrations secreted by malignant melanoma cells and the ARPE-19 cells were examined by enzyme-linked immunosorbent assay (ELISA). The two kinds of cells were both treated with VEGF and its antagonist, ranibizumab. The dynamic changes of the two types of cells were monitored by real-time cell electronic sensing (RT-CES) assay. The effect of ranibizumab on both types of cells was verified by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl (MTT) assay. The expression of VEGF receptor 1 (VEGFR1) RNA in uveal melanoma was further investigated through the PCR technique. RESULTS: The levels of VEGF secreted by malignant melanoma cells were much higher than those of ARPE-19 cells, and were markedly decreased in the action of 0.1 mg/ml ranibizumab. However, there was no obvious reduction of VEGF in the presence of ranibizumab for ARPE-19 (p>0.05). Meanwhile, RT-CES showed that the viability of malignant melanoma cells increased greatly in the presence of VEGF. When VEGF was 20 ng/ml, viability of the malignant melanoma cells increased by 40% compared with the negative control. There was no evident effect on proliferation of ARPE-19 (p>0.05). Furthermore, the growth of malignant melanoma cells was obviously inhibited after ranibizumab intervention. When ranibizumab was administered at 0.25 mg/ml, the survival rate of the malignant melanoma cells decreased to 57.5%. Nevertheless, low-dose exposure to ranibizumab had only a slight effect on the growth of ARPE-19, and PCR result demonstrated that VEGFR1 plays a role in this tumor tissue rather than VEGFR2. CONCLUSIONS: Ranibizumab can selectively inhibit malignant melanoma cell proliferation by decreasing the expression of VEGF; the possible mechanism of the inhibitory effect may involve VEGFR1 antagonism.
format Online
Article
Text
id pubmed-4021672
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Molecular Vision
record_format MEDLINE/PubMed
spelling pubmed-40216722014-05-27 The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1 Li, Jiao Cui, Yan Wang, Qin Guo, Dadong Pan, Xuemei Wang, Xingrong Bi, Hongsheng Chen, Wei Liu, Zhengfeng Zhao, Shengya Mol Vis Research Article PURPOSE: Angiogenesis is an important mediator in tumor progression. Vascular endothelial growth factor (VEGF) is one of the major cytokines that can influence angiogenesis. However, the potential mechanism of tumor growth inhibition through anti-VEGF agents is still unclear. This study was performed to examine whether ranibizumab could inhibit malignant melanoma growth in vitro and to determine the safety of ranibizumab on human adult retinal pigment epithelium cell line (ARPE-19 cells). METHODS: Malignant melanoma cells obtained from a clinic were cultured in vitro. VEGF concentrations secreted by malignant melanoma cells and the ARPE-19 cells were examined by enzyme-linked immunosorbent assay (ELISA). The two kinds of cells were both treated with VEGF and its antagonist, ranibizumab. The dynamic changes of the two types of cells were monitored by real-time cell electronic sensing (RT-CES) assay. The effect of ranibizumab on both types of cells was verified by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl (MTT) assay. The expression of VEGF receptor 1 (VEGFR1) RNA in uveal melanoma was further investigated through the PCR technique. RESULTS: The levels of VEGF secreted by malignant melanoma cells were much higher than those of ARPE-19 cells, and were markedly decreased in the action of 0.1 mg/ml ranibizumab. However, there was no obvious reduction of VEGF in the presence of ranibizumab for ARPE-19 (p>0.05). Meanwhile, RT-CES showed that the viability of malignant melanoma cells increased greatly in the presence of VEGF. When VEGF was 20 ng/ml, viability of the malignant melanoma cells increased by 40% compared with the negative control. There was no evident effect on proliferation of ARPE-19 (p>0.05). Furthermore, the growth of malignant melanoma cells was obviously inhibited after ranibizumab intervention. When ranibizumab was administered at 0.25 mg/ml, the survival rate of the malignant melanoma cells decreased to 57.5%. Nevertheless, low-dose exposure to ranibizumab had only a slight effect on the growth of ARPE-19, and PCR result demonstrated that VEGFR1 plays a role in this tumor tissue rather than VEGFR2. CONCLUSIONS: Ranibizumab can selectively inhibit malignant melanoma cell proliferation by decreasing the expression of VEGF; the possible mechanism of the inhibitory effect may involve VEGFR1 antagonism. Molecular Vision 2014-05-13 /pmc/articles/PMC4021672/ /pubmed/24868139 Text en Copyright © 2014 Molecular Vision. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Li, Jiao
Cui, Yan
Wang, Qin
Guo, Dadong
Pan, Xuemei
Wang, Xingrong
Bi, Hongsheng
Chen, Wei
Liu, Zhengfeng
Zhao, Shengya
The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title_full The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title_fullStr The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title_full_unstemmed The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title_short The proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing VEGF through VEGFR1
title_sort proliferation of malignant melanoma cells could be inhibited by ranibizumab via antagonizing vegf through vegfr1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4021672/
https://www.ncbi.nlm.nih.gov/pubmed/24868139
work_keys_str_mv AT lijiao theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT cuiyan theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT wangqin theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT guodadong theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT panxuemei theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT wangxingrong theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT bihongsheng theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT chenwei theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT liuzhengfeng theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT zhaoshengya theproliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT lijiao proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT cuiyan proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT wangqin proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT guodadong proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT panxuemei proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT wangxingrong proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT bihongsheng proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT chenwei proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT liuzhengfeng proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1
AT zhaoshengya proliferationofmalignantmelanomacellscouldbeinhibitedbyranibizumabviaantagonizingvegfthroughvegfr1

Ejemplares similares