Enhanced Tumor-forming Capacity for Immortalized Melanocytes Expressing Melanoma Growth Stimulatory Activity/growth-regulated Cytokine Beta and Gamma Proteins

Overview

Journal Int J Cancer

Specialty Oncology

Date 1997 Oct 23

PMID 9334815

Citations 50

Authors

J D OWEN

R Strieter

M Burdick

H Haghnegahdar

L Nanney

R Shattuck-Brandt

A Richmond

Affiliations

Soon will be listed here.

Abstract

Three human MGSA/GRO genes encode 3 highly related chemokines, MGSA/GRO alpha, -beta and -gamma. All 3 MGSA/GRO proteins bind to the same receptors, but with differing affinities, and stimulate a number of biological responses including chemotaxis, angiogenesis, and growth regulation. We have previously demonstrated that MGSA/GRO alpha can be isolated from culture medium conditioned by malignant melanoma cells and that continuous secretion of MGSA/GRO alpha contributes to the transformation of immortalized murine melanocytes. The present study was designed to determine whether MGSA/GRO beta or -gamma have similar effects on melanocyte tumorigenicity. Stable Melan-a clones expressing either human MGSA/GRO beta or -gamma exhibited enhanced ability to form large colonies in soft agar and tumors in nude mice. The clones expressing the MGSA/GRO beta or -gamma transgene formed tumors within 2 months after injection; the tumors were highly pigmented and expressed immunoreactive MGSA/GRO beta or -gamma protein. Furthermore, when conditioned medium from Melan-a clones expressing MGSA/GRO alpha, -beta or -gamma transgenes were examined for the ability to induce angiogenesis in the rat cornea, strong angiogenic responses were observed. This angiogenic response was blocked by antibodies to the respective MGSA/GRO protein, but not by normal rabbit serum. By contrast, angiogenic responses were observed in only 2 of 12 corneal implants (17%) containing medium conditioned by Melan-a clones expressing the neomycin resistance marker alone.

Citing Articles

Pretreatment inflammatory markers predicting treatment outcomes in colorectal cancer.

An S, Shim H, Kim K, Kim B, Bang H, Do H Ann Coloproctol. 2022; 38(2):97-108.

PMID: 35345306 PMC: 9021854. DOI: 10.3393/ac.2021.01004.0143.

Chemokine (C-X-C motif) ligand 1/chemokine (C-X-C motif) receptor 2 autocrine loop contributes to cellular proliferation, migration and apoptosis in cervical cancer.

Sun J, Yuan J Bioengineered. 2022; 13(3):7579-7591.

PMID: 35264061 PMC: 9278969. DOI: 10.1080/21655979.2022.2036896.

Multifaceted role of chemokines in solid tumors: From biology to therapy.

Raza S, Rajak S, Tewari A, Gupta P, Chattopadhyay N, Sinha R Semin Cancer Biol. 2022; 86(Pt 3):1105-1121.

PMID: 34979274 PMC: 7613720. DOI: 10.1016/j.semcancer.2021.12.011.

The Role of Post-Translational Modifications of Chemokines by CD26 in Cancer.

De Zutter A, Van Damme J, Struyf S Cancers (Basel). 2021; 13(17).

PMID: 34503058 PMC: 8428238. DOI: 10.3390/cancers13174247.

The CC and CXC chemokines: major regulators of tumor progression and the tumor microenvironment.

Bikfalvi A, Billottet C Am J Physiol Cell Physiol. 2020; 318(3):C542-C554.

PMID: 31913695 PMC: 7099520. DOI: 10.1152/ajpcell.00378.2019.