Perturbation of Intracellular Purine Nucleotides Balance as Effective Strategy for Cancer Therapy

سال انتشار: 1394
محل انتشار: اولین سمپوزیوم بین المللی سرطان نسترن
کد COI اختصاصی: NASTARANCANSER01_102
زبان مقاله: انگلیسی
تعداد مشاهده: 549

نویسندگان

Department of Chemistry, Faculty of Science, Ferdowsi University of Mashhad, Mashhad, Iran

چکیده

It is entirely accepted that a metabolic change in purine nucleotide concentration occursduring carcinogenesis which facilitate the pathological process of malignant cells such asproliferation, invasion and metastasis. Nucleotides participate in many biochemicalprocesses as activated precursors and source of energy in nucleic acid biosynthesis and asintermediate products for synthesis of lipids and proteins. However, currently it has beendocumented that purine nucleotides act as signaling molecules which directly or indirectlyregulate stability, subcellular localization and activation of plethora of proteins in cells.Although biosynthesis of purine nucleotides is up-regulated in malignant versus normal cells,the ratio of [ATP] and [GTP] is maintained constant about 7 to 1, which is critical for cellbiological process. This biological fact makes GTP as rate limiting factor not only in nucleicacid synthesis but also in regulation of survival and death signaling molecules whosefunctions are regulated by GTP content. In this line, several strategies were developed thatimpact on intracellular GTP content and disrupt the ratio of [ATP]/[GTP]. For instant, inhibitorshave been introduced in which some of them are in clinical trial at phase I and II, targetedinosine 5Ëˆ-monophosphate dehydrogenase (IMPDH) (type II) as rate limiting enzyme inGTP biosynthesis pathways in malignant cells. Mycophenolic acid, the most potent andselective IMPDH inhibitor, by depletion of intracellular GTP content disrupts purinenucleotides balance and conducts tumor cells toward apoptosis. On the other hands it hasbeen ascertained that extracellular purine nucleotides, themselves act as signalingmolecules which uptake by tumor cells through transporters on plasma membrane. In thatrespect, it has been disclosed that uptake of extracellular GTP by tumor cells leadingperturbation of intracellular purine nucleotides balance which impact on signaling moleculesand tilt cellÊ¼s fate toward apoptosis. From therapeutic standpoint, modulation ofintracellular purine nucleotides by extracellular nucleotides or by selective inhibitors whichtarget rate limiting enzymes in nucleotides biosynthesis pathways could be considered as apotential therapeutic option for malignant cells.

کلیدواژه ها

Purine Nucleotides, Malignant Cells, Signaling Pathways, Apoptosis, Cancer Therapy

مقالات مرتبط جدید

اطلاعات بیشتر در مورد COI

COI مخفف عبارت CIVILICA Object Identifier به معنی شناسه سیویلیکا برای اسناد است. COI کدی است که مطابق محل انتشار، به مقالات کنفرانسها و ژورنالهای داخل کشور به هنگام نمایه سازی بر روی پایگاه استنادی سیویلیکا اختصاص می یابد.

کد COI به مفهوم کد ملی اسناد نمایه شده در سیویلیکا است و کدی یکتا و ثابت است و به همین دلیل همواره قابلیت استناد و پیگیری دارد.