首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Increased fluid secretion after adenoviral-mediated transfer of the human aquaporin-1 cDNA to irradiated miniature pig parotid glands.
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Increased fluid secretion after adenoviral-mediated transfer of the human aquaporin-1 cDNA to irradiated miniature pig parotid glands.

机译:腺病毒介导的人类aquaporin-1 cDNA转移至受照小猪腮腺后,液体分泌增加。

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摘要

The treatment of most head and neck cancer patients includes ionizing radiation (IR). Salivary glands in the IR field suffer irreversible damage. Previously, we reported that adenoviral (Ad)-mediated transfer of the human aquaporin-1 (hAQP1) cDNA to rat submandibular glands following IR restored salivary flow to near normal levels. It is unclear if this strategy is useful in larger animals. Herein, we evaluated AdhAQP1-mediated gene transfer after parotid gland IR (20 Gy) in the miniature pig. Sixteen weeks following IR, salivation from the targeted gland was decreased by >80%. AdhAQP1 administration resulted in a dose-dependent increase in parotid salivary flow to approximately 80% of pre-IR levels on day 3. A control Ad vector was without significant effect. The effective AdhAQP1 dose was 2.5 x 10(5) pfu/microl infusate, a dose that leads to comparable transgene expression in murine and minipig salivary glands. Three days after Ad vector administration little change was observed in clinical chemistryand hematology values. These findings demonstrate that localized delivery of AdhAQP1 to IR-damaged salivary glands increases salivary secretion, without significant general adverse events, in a large animal model.
机译:大多数头颈癌患者的治疗包括电离辐射(IR)。 IR领域的唾液腺遭受不可逆的损害。以前,我们报道了IR感染后,腺病毒(Ad)介导的人类aquaporin-1(hAQP1)cDNA向大鼠下颌下腺的转移将唾液流量恢复到接近正常水平。目前尚不清楚这种策略是否适用于大型动物。本文中,我们评估了小型猪腮腺IR(20 Gy)后AdhAQP1介导的基因转移。 IR后十六周,目标腺的唾液分泌减少了> 80%。在第3天,AdhAQP1给药导致腮腺唾液流量以剂量依赖性方式增加至IR前水平的约80%,而对照Ad载体无明显作用。 AdhAQP1的有效剂量为2.5 x 10(5)pfu /微升输注液,该剂量可在鼠和小型猪唾液腺中产生相当的转基因表达。施用Ad载体三天后,临床化学和血液学值几乎未见变化。这些发现表明,在大型动物模型中,将AdhAQP1局部递送至IR受损的唾液腺可增加唾液分泌,而不会出现明显的一般不良事件。

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