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Changes in tumor-antigen expression profile as human small-cell lung cancers progress
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作者 Li-Sheng Ge Neil T. Hoa +4 位作者 nils lambrecht Maria Dacosta-Iyer Yi Ouyang Amir Abolhoda Martin R. Jadus 《Cancer Biology & Medicine》 SCIE CAS CSCD 2015年第2期96-105,共10页
Objective: Our group has previously observed that in patients with small-cell lung cancers(SCLCs), the expression of a tumor antigen, glioma big potassium(g BK) ion channel, is higher at the time of death than when th... Objective: Our group has previously observed that in patients with small-cell lung cancers(SCLCs), the expression of a tumor antigen, glioma big potassium(g BK) ion channel, is higher at the time of death than when the cancer is first treated by surgical resection. This study aimed to determine whether this dichotomy was common in other potential lung tumor antigens by examining the same patient samples using our more extensive profile analysis of tumor-antigen precursor protein(TAPP). We then tested the hypothesis that therapeutic intervention may inadvertently cause this increased g BK production.Methods: SCLC samples(eight surgical resections and three autopsy samples) and three control lungs were examined by quantitative real-time polymerase chain reaction for 42 potential TAPPs that represent potential T-cell-mediated immunological targets. Results: Twenty-two TAPP m RNAs displayed the same profile as g BK, i.e., more m RNAs were expressed at autopsy than in their surgical counterparts. B-cyclin and mouse double minute 2, human homolog of P53-binding protein were elevated in both autopsy and surgical specimens above the normal-lung controls. When HTB119 cells were incubated with doxorubicin, g BK was strongly induced, as confirmed by intracellular flow cytometry with a g BK-specific antibody.Conclusion: Our findings suggested that more immunological targets became available as the tumor responded to chemotherapy and proceeded toward its terminal stages. 展开更多
关键词 肿瘤抗原 T细胞 肺癌 表达谱 聚合酶链反应 手术切除 基因表达 GBK
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