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Production of Transgenic Calves Expressing an shRNA Targeting Myostatin

机译:表达靶向肌生长抑制素的shRNA的转基因小牛的生产

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摘要

Myostatin (MSTN) is a well-known negative regulator of muscle growth. Animals that possess mutations within this gene display an enhanced muscling phenotype, a desirable agricultural trait. Increased neonatal morbidity is common, however, resulting from complications arising from the birth of offspring with increased fetal muscle mass. The objective of the current research was to generate an attenuated MSTN-null phenotype in a large-animal model using RNA interference to enhance muscle development without the detrimental consequences of an inactivating mutation. To this end, we identified a series of short interfering RNAs that demonstrated effective suppression of MSTN mRNA and protein levels. To produce transgenic offspring capable of stable MSTN suppression in vivo, a recombinant lentiviral vector expressing a short hairpin RNA (shRNA) targeting MSTN for silencing was introduced into bovine fetal fibroblasts. These cells were used as nucleus donors for somatic cell nuclear transfer (SCNT). Twenty blastocysts were transferred into seven recipient cows resulting in five pregnancies. One transgenic calf developed to term, but died following delivery by Caesarean-section. As an alternative strategy, microinjection of recombinant lentiviral particles into the perivitelline space of in vitro-produced bovine zygotes was utilized to produce 40 transgenic blastocysts that were transferred into 14 recipient cows, resulting in 7 pregnancies. Five transgenic calves were produced, of which three expressed the transgene. This is the first report of transgenic livestock produced by direct injection of a recombinant lentivirus, and expressing transgenes encoding shRNAs targeting an endogenous gene (myostatin) for silencing.
机译:Myostatin(MSTN)是肌肉生长的负调节剂。在该基因内具有突变的动物表现出增强的肌肉表型,这是理想的农业性状。然而,新生儿发病率增加是常见的,这是由于后代的出生伴随胎儿肌肉质量增加而引起的并发症。当前研究的目的是在大动物模型中使用RNA干扰产生减毒的MSTN-null表型,以增强肌肉发育而不会导致失活突变的不利后果。为此,我们鉴定了一系列短干扰RNA,它们证明了对MSTN mRNA和蛋白质水平的有效抑制。为了产生能够在体内稳定地抑制MSTN的转基因后代,将表达靶向MSTN以沉默的短发夹RNA(shRNA)的重组慢病毒载体引入牛胎儿成纤维细胞中。这些细胞用作体细胞核移植(SCNT)的核供体。将二十个胚泡转移到七只受体母牛中,导致五次怀孕。一只转基因小牛发育至足月,但经剖腹产分娩后死亡。作为一种替代策略,将重组慢病毒颗粒显微注射到体外产生的牛合子的玻璃体周腔中可产生40个转基因胚泡,这些胚泡被转移到14头受牛中,导致7例妊娠。产生了五只转基因牛,其中三只表达了转基因。这是通过直接注射重组慢病毒而产生的转基因家畜的首次报道,并表达编码靶向内源基因(肌生长抑制素)的shRNA的转基因进行沉默。

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