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成人人类肉瘤。II. 医学肿瘤学。

Adult human sarcomas. II. Medical oncology.

作者信息

Sinkovics Joseph G

机构信息

The University of South Florida, Cancer Institute of St Joseph's Hospital, HL Moffitt Cancer Center, The University of South Florida College of Medicine, FL, USA.

出版信息

Expert Rev Anticancer Ther. 2007 Feb;7(2):183-210. doi: 10.1586/14737140.7.2.183.

DOI:10.1586/14737140.7.2.183
PMID:17288529
Abstract

Human sarcoma cells can be killed by radio- and chemotherapy, but tumor cells acquiring resistance frequently kill the patient. A keen understanding of the intracellular course of oncogenic cascades leads to the discovery of small molecular inhibitors of the involved phosphorylated kinases. Targeted therapy complements chemotherapy. Oncogene silencing is feasible by small interfering RNA. The restoration of some of the mutated or deleted tumor-suppressor genes (p53, Rb, PTEN, hSNF, INK/ARF and WT) by demethylation or reacetylation of their histones has been accomplished. Genetically engineered or naturally oncolytic viruses selectively lyse tumors and leave healthy tissues intact. Adeno- or retroviral vectors deliver genes of immunological costimulators, tumor antigens, chemo- or cytokines and/or tumor-suppressor proteins into tumor (sarcoma) cells. Suicide gene delivery results in apoptosis induction. Genes of enzymes that target prodrugs as their substrates render tumor cells highly susceptible to chemotherapy, with the prodrug to be targeted intracellularly. It will be combinations of sophisticated surgical removal of the nonencapsulated and locally invasive primary sarcomas, advanced forms of radiotherapy to the involved sites and immunotherapy with sarcoma vaccines that will cure primary sarcomas. Adoptive immunotherapy with immune lymphocytes will be operational in metastatic disease only when populations of regulatory T cells are controlled. Targeted therapy with small molecular inhibitors of oncogene cascades, the driving forces of sarcoma cells, alteration of the tumor stroma from a supportive to a tumor-hostile environment, reactivation or replacement of wild-type tumor-suppressor genes, and radio-chemotherapy (with much reduced toxicity) will eventually accomplish the cure of metastatic sarcomas.

摘要

人类肉瘤细胞可被放疗和化疗杀死,但获得耐药性的肿瘤细胞常常会导致患者死亡。深入了解致癌级联反应的细胞内过程,促使人们发现了相关磷酸化激酶的小分子抑制剂。靶向治疗是化疗的补充。通过小分子干扰RNA使癌基因沉默是可行的。通过对某些突变或缺失的肿瘤抑制基因(p53、Rb、PTEN、hSNF、INK/ARF和WT)的组蛋白进行去甲基化或再乙酰化,已实现这些基因的恢复。基因工程改造的或天然的溶瘤病毒可选择性地裂解肿瘤并使健康组织保持完整。腺病毒或逆转录病毒载体将免疫共刺激分子、肿瘤抗原、化疗药物或细胞因子和/或肿瘤抑制蛋白的基因导入肿瘤(肉瘤)细胞中。导入自杀基因可诱导细胞凋亡。以前体药物为底物的酶基因使肿瘤细胞对化疗高度敏感,前体药物在细胞内发挥作用。复杂的手术切除非包膜性和局部浸润性原发性肉瘤、对受累部位采用先进的放射治疗以及使用肉瘤疫苗进行免疫治疗相结合,将治愈原发性肉瘤。只有当调节性T细胞群体得到控制时,采用免疫淋巴细胞的过继性免疫治疗才会对转移性疾病有效。用癌基因级联反应的小分子抑制剂进行靶向治疗、将肿瘤基质从支持性环境改变为对肿瘤有敌意的环境、重新激活或替代野生型肿瘤抑制基因以及进行毒性大大降低的放化疗最终将实现转移性肉瘤的治愈。

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Adult human sarcomas. II. Medical oncology.成人人类肉瘤。II. 医学肿瘤学。
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Does chemotherapy augment anti-tumor immunotherapy by preferential impairment of regulatory T cells?化疗是否通过优先损害调节性T细胞来增强抗肿瘤免疫疗法?
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