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Analysis of genetically engineered oncolytic herpes simplex viruses in human prostate cancer organotypic cultures.

机译:在人类前列腺癌器官型培养物中分析基因工程溶瘤性单纯疱疹病毒。

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Oncolytic herpes simplex viruses type 1 (oHSVs) such as G47Delta and G207 are genetically engineered for selective replication competence in cancer cells. Several factors can influence the overall effectiveness of oHSV tropism, including HSV-1 receptor expression, extracellular matrix milieu and cellular permissiveness. We have taken advantage of human prostate organ cultures derived from radical prostatectomies to investigate oHSV tropism. In this study, we show that both G47Delta and G207 specifically replicate in epithelial cells of the prostatic glands but not in the surrounding stroma. In contrast, both the epithelial and stromal cell compartments were readily infected by wild-type HSV-1. Analysis of oHSV replication in prostate surgical specimens 3 days post infection showed that G47Delta generated approximately 30-fold more viral progeny than did G207. This correlated with the enhanced expression of G47Delta-derived glycoprotein gB protein levels as compared with G207. In benign prostate tissues, G207 and G47Delta titers were notably reduced, whereas strain F titers were maintained at similar levels compared with prostate cancer specimens. Overall, our results show that these oncolytic herpes vectors show both target specificity and replication competence in human prostate cancer specimens and point to the utility of using human prostate organ cultures in assessing oHSV tropism and cellular specificity.
机译:1型溶瘤性单纯疱疹病毒(oHSV)(例如G47Delta和G207)经过基因工程改造,可在癌细胞中选择性复制。几个因素可以影响oHSV向性的整体有效性,包括HSV-1受体表达,细胞外基质环境和细胞介导性。我们已利用源自根治性前列腺切除术的人类前列腺器官文化来研究oHSV嗜性。在这项研究中,我们表明G47Delta和G207都在前列腺的上皮细胞中特异性复制,但在周围的基质中不复制。相反,野生型HSV-1容易感染上皮和基质细胞区室。感染后3天,前列腺手术标本中的oHSV复制分析表明,G47Delta产生的病毒后代比G207多大约30倍。与G207相比,这与G47Delta衍生的糖蛋白gB蛋白水平的表达增强有关。在良性前列腺组织中,与前列腺癌标本相比,G207和G47Delta滴度显着降低,而F株滴度保持在相似的水平。总体而言,我们的结果表明,这些溶瘤疱疹载体在人前列腺癌标本中既显示了靶标特异性,又显示了复制能力,并指出了使用人前列腺器官培养物评估oHSV向性和细胞特异性的实用性。

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