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唾液腺中转基因产物全身递送的证据。

Evidence for the systemic delivery of a transgene product from salivary glands.

作者信息

Kagami H, O'Connell B C, Baum B J

机构信息

Clinical Investigations and Patient Care Branch, National Institute of Dental Research, National Institutes of Health, Bethesda, MD 20892-1190, USA.

出版信息

Hum Gene Ther. 1996 Nov 10;7(17):2177-84. doi: 10.1089/hum.1996.7.17-2177.

Abstract

The aim of this study was to assess the feasibility of using gene transfer to salivary glands to direct the systemic delivery of therapeutic proteins in vivo. We used a replication-deficient recombinant adenovirus vector (Ad alpha 1AT) that encodes human alpha 1-antitrypsin (h alpha 1-AT), which we used as a marker protein. Ad alpha 1AT (5 x 10(9) pfu) was administered by retrograde ductal instillation to the submandibular glands of male rats. The amount of h alpha 1-AT found in the salivary glands, saliva, serum, and other tissues was analyzed by a sensitive enzyme-linked immunosorbent assay (ELISA). Maximal levels of the marker protein were detected at 24-48 hr post-virus administration for glands (274 ng/mg protein), saliva (approximately 313 ng/ml), and serum (approximately 5 ng/ml). Serum levels remained elevated for 96 hr, whereas the measured half-life for the marker protein was approximately 2 hr. Generally little to no h alpha 1-AT was detectable in most other organs. However, we were able to measure low levels of marker protein in tissues immediately surrounding infected glands. In all animals studied, levels of h alpha 1-AT were higher in the glandular venous effluent than in arterial blood. Similar results were found with parotid glands. The aggregate data demonstrate that salivary glands may be a target for the nonsurgical, systemic delivery of transgene-encoded therapeutic proteins for diseases that require relatively low circulating protein levels.

摘要

本研究的目的是评估利用基因转移至唾液腺来在体内直接进行治疗性蛋白质全身递送的可行性。我们使用了一种编码人α1 -抗胰蛋白酶(hα1 - AT)的复制缺陷型重组腺病毒载体(Adα1AT),将其用作标记蛋白。通过逆行导管灌注法将Adα1AT(5×10⁹ 空斑形成单位)给予雄性大鼠的下颌下腺。采用灵敏的酶联免疫吸附测定(ELISA)法分析唾液腺、唾液、血清及其他组织中hα1 - AT的含量。在病毒给药后24 - 48小时,腺体(274 ng/mg蛋白质)、唾液(约313 ng/ml)和血清(约5 ng/ml)中检测到标记蛋白的最高水平。血清水平在96小时内持续升高,而标记蛋白的测得半衰期约为2小时。在大多数其他器官中通常几乎检测不到或检测不到hα1 - AT。然而,我们能够在受感染腺体周围的组织中检测到低水平的标记蛋白。在所有研究的动物中,腺体静脉流出液中hα1 - AT的水平高于动脉血中的水平。在腮腺中也发现了类似的结果。汇总数据表明,对于需要相对低循环蛋白水平的疾病,唾液腺可能是用于非手术全身递送转基因编码治疗性蛋白质的一个靶点。

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