Matrix Metalloproteinase 2 Secretion in WEHI 164 Fibrosarcoma Cells is Nitric Oxide-related and Modified by Morphine

Overview

Journal Eur J Pharmacol

Specialty Pharmacology

Date 2006 Jan 3

PMID 16386243

Citations 11

Authors

Ahmad Shariftabrizi

Artemissia-Phoebe Nifli

Mohammad Ansari

Farshid Saadat

Mohammad Reza Ebrahimkhani

Nastaran Alizadeh

Azadeh Nasseh

Vassilia-Ismini Alexaki

Ahmad Reza Dehpour

Elias Castanas

Mohammad Reza Khorramizadeh

Affiliations

Soon will be listed here.

Abstract

Matrix metalloproteinases (MMP) are ubiquitous enzymes involved in extracellular matrix remodeling, and as a consequence in a number of physiological and pathological states, including development, wound healing and cancer. A crucial feature of cancer progression and metastasis is the disruption of extracellular matrix, and spreading of proliferating cancer cells. Modulation of MMP is a main target of cancer research. Using the mouse fibrosarcoma cell line WEHI 164, producing high amounts of MMP-2, we investigated whether we could modulate its production. We report that MMP-2 is under the control of nitric oxide (NO)/nitric oxide synthase (NOS) system. In addition, we show that NOS activity is controlled by opioids in a non-opioid receptor-related manner. Finally, we provide evidence that morphine, when administrated at low, non-toxic concentrations (<10(-9) M) attenuates MMP-2 activity. We conclude that, as morphine is able to decrease metalloproteinase activity via the NO/NOS system, it may have a place in the treatment of several sarcomas including fibrosarcoma.

Citing Articles

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