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自杀基因与细胞因子联合非病毒基因疗法治疗自发性犬黑色素瘤

Suicide gene and cytokines combined nonviral gene therapy for spontaneous canine melanoma.

作者信息

Finocchiaro L M E, Fiszman G L, Karara A L, Glikin G C

机构信息

Unidad de Transferencia Genética, Instituto de Oncología A H Roffo, Universidad de Buenos Aires, Buenos Aires, Argentina.

出版信息

Cancer Gene Ther. 2008 Mar;15(3):165-72. doi: 10.1038/sj.cgt.7701096. Epub 2008 Jan 25.

DOI:10.1038/sj.cgt.7701096
PMID:18219342
Abstract

Canine spontaneous melanoma is a highly aggressive tumor resistant to current therapies. We evaluated the safety, efficacy and antitumor effects of direct intratumor injections of lipoplexes encoding herpes simplex thymidine kinase coadministrated with ganciclovir, and irradiated transgenic xenogeneic cells secreting 20-30 mug day(-1) of human granulocyte-macrophage colony-stimulating factor and interleukin-2. Toxicity was minimal or absent in all patients. This combined treatment (CT) induced tumor regression and a pronounced immune cell infiltration. The objective responses (47%: 21/45) averaged 80% of tumor mass loss. Local CT also induced systemic antitumor response evidenced by complete remission of one pulmonary metastasis and by the significantly higher percentage of metastasis-free patients (76: 34/45)) until the study ending compared to untreated (UC: 29%, 5/17), surgery-treated (CX: 48%, 11/23) or suicide gene-treated controls (SG: 56%, 9/16) (Fisher's exact test). CT significantly improved median survival time: 160 (57-509) days compared to UC (69 (10-169)), CX (82 (43-216)) or SG (94 (46-159)). CT also increased (P<0.00001, Kaplan-Meier analysis) metastasis-free survival: >509 (57-509) days with respect to UC: 41 (10-169), CX: 133 (43-216) and SG: >159 (41-159). Therefore, CT controlled tumor growth by delaying or preventing distant metastasis, thereby significantly extending survival and recovering the quality of life.

摘要

犬自发性黑色素瘤是一种对当前治疗具有高度抗性的侵袭性肿瘤。我们评估了直接瘤内注射编码单纯疱疹胸苷激酶并与更昔洛韦联合使用的脂质体,以及照射分泌20 - 30微克/天人类粒细胞 - 巨噬细胞集落刺激因子和白细胞介素 - 2的转基因异种细胞的安全性、有效性和抗肿瘤作用。所有患者的毒性极小或不存在。这种联合治疗(CT)诱导了肿瘤消退和明显的免疫细胞浸润。客观缓解率(47%:21/45)平均为肿瘤质量损失的80%。局部CT还诱导了全身抗肿瘤反应,表现为一处肺转移完全缓解,以及与未治疗(UC:29%,5/17)、手术治疗(CX:48%,11/23)或自杀基因治疗对照组(SG:56%,9/16)相比,直至研究结束时无转移患者的比例显著更高(76%:34/45)(Fisher精确检验)。CT显著改善了中位生存时间:与UC(69(10 - 169)天)、CX(82(43 - 216)天)或SG(94(46 - 159)天)相比为160(57 - 509)天。CT还增加了(P<0.00001,Kaplan - Meier分析)无转移生存期:相对于UC为>509(57 - 509)天,CX为133(43 - 216)天,SG为>159(41 - 159)天。因此,CT通过延迟或预防远处转移来控制肿瘤生长,从而显著延长生存期并恢复生活质量。

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