肿瘤特异性抗原作为子宫内膜癌种系突变潜在疫苗候选物的计算预测

IF 0.4 Q4 PHARMACOLOGY & PHARMACY Advances in Pharmacology and Pharmacy Pub Date : 2019-10-01 DOI:10.13189/APP.2019.070401
Iqra Iftikhar, A. Khalid, Zainab Bibi, A. Mehmood, Muhammad Rizwan, Sajid Khan, Anum Munir
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引用次数: 0

摘要

子宫内膜癌是女性中第四大常见癌症。它起源于子宫内膜,并伴有细胞的异常生长。体征和症状包括盆腔疼痛和阴道异常出血。它有两类。1型肿瘤是雌激素依赖性的,它们在PTEN、PIK3CA中有突变,而2型肿瘤更敏感,在TP53中有突变。信号通路(PI3K)的过度激活导致抗凋亡。本研究旨在鉴定子宫内膜癌种系突变的肿瘤特异性抗原,该抗原可作为潜在的候选疫苗。种系突变数据来自宇宙数据库的癌症基因普查。基因突变在子宫内膜癌中起重要作用。肽库是利用肽设计库生成的。人类白细胞抗原等位基因通过NetMHC鉴定肽库。测定了等位基因与肽的结合亲和力。执行线性回归以生成图形。PTEN、TP53、PIK3CA、KRAS和CTNNB1被证明具有关键作用。共产生575个重叠的肽库,每个肽的长度为18-20个氨基酸。大约有58个hla被确定,它们与hla有很强的相互作用。回归分析表明:许多突变与肽的结合亲和力直接相关。由此,我们建议鉴定的TSA可作为直接靶向子宫内膜癌突变基因的个性化肽疫苗。本研究工作可用于实验室进一步验证。
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Computational Prediction of Tumor-Specific Antigens as Potential Vaccine Candidates against Germ-line Mutations in Endometrial Cancer
Endometrial cancer is the fourth most common cancer in women. It arises from the endometrium and accompanied by the abnormal growth of the cells. Sign and symptoms include pelvic pain and abnormal vaginal bleeding. It has two categories. Type 1 tumors are estrogen-dependent and they have mutations in PTEN, PIK3CA while Type 2 tumors are more sensitive and have mutations in TP53. Overactivation of the signaling pathway (PI3K) results in anti-apoptosis. Here, this study aims to identify Tumor-Specific Antigen for germline mutations in endometrial cancer which can be used as a potential vaccine candidate. The germline mutations data are obtained from cancer gene census of the cosmic database. Genes mutating with crucial role in endometrial cancer are considered. Peptides libraries are generated using peptide design library. Human leukocyte antigen alleles are identified for the peptide library through NetMHC. Binding affinities of alleles with peptide are determined. Linear regression is performed to generate graphs. PTEN, TP53, PIK3CA, KRAS, and CTNNB1 proved to have critical role. About 575 overlapping peptide libraries are generated and each peptide has a length of 18-20 amino acids. Approximately 58 HLAs are identified, having strong interactions with HLAs. Regression analysis shows that the no. of mutations are directly associated with a binding affinity of peptides. From this, we suggest that the identified TSA can be used as personalized peptide vaccines that directly target the mutated genes in endometrial cancer. This research work can be used in the laboratories for further validation.
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Advances in Pharmacology and Pharmacy
Advances in Pharmacology and Pharmacy PHARMACOLOGY & PHARMACY-
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