عنوان المقالة:target identification for neuroendocrine tumors
د محمد محمود محمد عبد الفتاح | DR MOHAMMAD MAHMOUD MOHAMMAD ADEL FATAH | 9935
نوع النشر
مجلة علمية
المؤلفون بالعربي
cancer researches
الملخص العربي
Early diagnosis and targeted therapy are pivotal tools for the treatment success of neuroendocrine tumors. The use of somatostatin analogs brought great benefits for NET patients, especially for inoperable or metastasized gastroenteropancreatic tumors. However, this treatment modality cannot be applied in all cases. Around one third of tumors do not overexpress somatostatin receptors, thus are not susceptibl e for octreotide or similar SST analogs. Further G protein-coupled receptors (GPCR) have to be investigated in neuroendocrine tumors for their use in alternative targeting approaches. A novel DNA microarray was developed, for investigation of 368 genes, most of them GPCRs (357). This array was designed to detect differential splice variants and expression levels in parallel. Pancreatic neuroendocrine tumor samples and control pancreas tissue were hybridized on these DNA microarrays. After applying splice detection and expression level analysis tools, several novel potential targets where identified (for example GIPR, MC1R, FN1, TUBB3). These newly found receptors and extracellu lar matrix proteins were validated with higher sample numbers, in both protein- (Westernblot, immunohistochemistry) and mRNA-based (qPCR) assays. For peptide G protein-coupled receptors, the two highly overexpressed genes MC1R and GIPR were identified and validated. Gastric inhibitory polypeptide receptor (GIPR) has been shown to have similar expression levels as somatostatin receptor 2 in pancreatic and ileal neuroendocrine tumors. The NET cell lines H727 and KRJ-1 can be stimulated in functional cAMP production assays with the human GIP1-42 peptide ligand. In direct comparison, MC1R is, on an absolute scale, less expressed than GIPR but shows still a very high significant differentially expression towards healthy control tissues. Neuroendocrine human cell lines LCC-18 and CM could be stimulated by applying both alphamelanocortin but as well MC1R specific peptides and small molecules. In a two rounds of peptide optimization, 43 novel ligands were designed. These have been analyzed in cyclic adenosinmonophosphat production assays and in radioactive receptor-ligand binding studies with th e human melanocortin 1, 3, 4 and 5 receptors. Here, several highly potent and very specific MC1R ligands were designed which are composed of one C-terminal fatty acid and four amino acids. These novel compoun ds will be evaluated for their potential use in diagnostic or therapeutic application in the future.
تاريخ النشر
18/07/2016
الناشر
dr mohammad mahmoud
رابط الملف
تحميل (297 مرات التحميل)
رجوع