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首页> 外文期刊>Cancer gene therapy >Assessment of intravenous pbi-shRNA PDX1 nanoparticle (OFHIRNA-PDX1) in yucatan swine
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Assessment of intravenous pbi-shRNA PDX1 nanoparticle (OFHIRNA-PDX1) in yucatan swine

机译:尤加坦猪中静脉内pbi-shRNA PDX1纳米颗粒(OFHIRNA-PDX1)的评估

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PDX1 (pancreatic and duodenal homeobox 1) is overexpressed in pancreatic cancer, and its reduction results in tumor regression. Bi-functional pbi-shRNA PDX1 nanoparticle (OFHIRNA-PDX1) utilizes the endogenous micro-RNA biogenesis pathway to effect cleavage- and non-cleavage-dependent degradation of PDX1 mRNA. We have shown that OFHIRNA-PDX1 reduces pancreatic tumor volume in xenograft models. Thus, we are now exploring biorelevant large animal safety of OFHIRNA-PDX1. Mini pigs were chosen as the biorelevant species based on the similarity of human and pig PDX1 target sequence. In the initial study, animals developed fever, lethargy, hyporexia and cutaneous hyperemia following administration of OFHIRNA-PDX1. Twenty-one days later, the same animals demonstrated less toxicity with a second OFHIRNA-PDX1 infusion in conjunction with a prophylactic regimen involving dexamethasone, diphenhydramine, Indocin and ranitidine. In a new group of animals, PDX1 protein (31?kDa) expression in the pancreas was significantly repressed at 48 and 72?h (85%, P=0.018 and 88%, P=0.013; respectively) following a single infusion of OFHIRNA-PDX1 but recovered to normal state within 7 days. In conclusion, a single intravenous infusion of OFHIRNA-PDX1 in conjunction with premedication in pigs was well tolerated and demonstrated significant PDX1 knockdown.
机译:PDX1(胰腺和十二指肠同源盒1)在胰腺癌中过表达,其减少导致肿瘤消退。双功能pbi-shRNA PDX1纳米颗粒(OFHIRNA-PDX1)利用内源性微RNA生物发生途径来实现PDX1 mRNA的裂解和非裂解依赖性降解。我们已经显示,OFHIRNA-PDX1减少异种移植模型中的胰腺肿瘤体积。因此,我们现在正在探索OFHIRNA-PDX1与生物有关的大型动物安全性。基于人与猪PDX1目标序列的相似性,选择小型猪作为生物相关物种。在最初的研究中,动物在服用OFHIRNA-PDX1后出现发烧,嗜睡,低氧和皮肤充血。 21天后,同一动物经第二次OFHIRNA-PDX1输注并结合地塞米松,苯海拉明,吲哚丁和雷尼替丁的预防方案后,毒性降低。在一组新动物中,单次输注OFHIRNA后,胰腺中PDX1蛋白(31?kDa)的表达在48和72?h时显着抑制(分别为85%,P = 0.018和88%,P = 0.013)。 -PDX1,但在7天内恢复到正常状态。总之,在猪中对OFHIRNA-PDX1进行静脉内单次输注并配合用药前的药物耐受性良好,并显示出显着的PDX1抑制作用。

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