Heparanase is an endoglycosidase involved in remodeling the extracellular matrix and thereby in regulating multiple cellular processes and biological activities. It cleaves heparan sulfate (HS) side chains of HS proteoglycans into smaller fragments and hence regulates tissue morphogenesis, differentiation, and homeostasis. Heparanase is overexpressed in various carcinomas, sarcomas, and hematological malignancies, and its upregulation correlates with increased tumor size, tumor angiogenesis, enhanced metastasis, and poor prognosis. In contrast, knockdown or inhibition of heparanase markedly attenuates tumor progression, further underscoring the potential of anti-heparanase therapy. Heparanase inhibitors were employed to interfere with tumor progression in preclinical studies, and selected heparin mimetics are being examined in clinical trials. However, despite tremendous efforts, the discovery of heparanase inhibitors with high clinical benefit and minimal adverse effects remains a therapeutic challenge. This review discusses the key roles of heparanase in cancer progression focusing on the status of natural, chemically modified, and synthetic heparanase inhibitors in various types of malignancies.
Design of chemically novel, biologically potent small heterocyclic molecules with anticancer
activities, which targets the enzyme heparanase has gained prominent clinical interest. We have synthesized a
novel class of carboxamide derivatives by coupling various substituted aromatic acid hydrazides and triazoleamine
with pyrrolidine carboxylic acid by using coupling agents. The synthesized compounds are characterized
by spectroscopic techniques such as FT-IR, HRMS and NMR. These compounds are investigated for
cytotoxicity on different cancer cell lines and heparanase inhibitory activity. Most of them showed moderate
heparanase inhibitory activity and good cytotoxicity.
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