Literature DB >> 25917881

Germline transmission in transgenic Huntington's disease monkeys.

Sean Moran1, Tim Chi1, Melinda S Prucha1, Kwang Sung Ahn1, Fawn Connor-Stroud2, Sherrie Jean2, Kenneth Gould2, Anthony W S Chan3.   

Abstract

Transgenic nonhuman primate models are an increasingly popular model for neurologic and neurodegenerative disease because their brain functions and neural anatomies closely resemble those of humans. Transgenic Huntington's disease monkeys (HD monkeys) developed clinical features similar to those seen in HD patients, making the monkeys suitable for a preclinical study of HD. However, until HD monkey colonies can be readily expanded, their use in preclinical studies will be limited. In the present study, we confirmed germline transmission of the mutant huntingtin (mHTT) transgene in both embryonic stem cells generated from three male HD monkey founders (F0) and in second-generation offspring (F1) produced via artificial insemination by using intrauterine insemination technique. A total of five offspring were produced from 15 females that were inseminated by intrauterine insemination using semen collected from the three HD founders (5 of 15, 33%). Thus far, sperm collected from the HD founder (rHD8) has led to two F1 transgenic HD monkeys with germline transmission rate at 100% (2 of 2). mHTT expression was confirmed by quantitative real-time polymerase chain reaction using skin fibroblasts from the F1 HD monkeys and induced pluripotent stem cells established from one of the F1 HD monkeys (rHD8-2). Here, we report the stable germline transmission and expression of the mHTT transgene in HD monkeys, which suggest possible expansion of HD monkey colonies for preclinical and biomedical research studies.
Copyright © 2015 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Germline transmission; Second generation; Transgenic Huntington's disease monkey; Ultrasound-guided intrauterine insemination

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Year:  2015        PMID: 25917881      PMCID: PMC4631054          DOI: 10.1016/j.theriogenology.2015.03.016

Source DB:  PubMed          Journal:  Theriogenology        ISSN: 0093-691X            Impact factor:   2.740


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