Porcine epidemic viruses, such as
pseudorabies virus (PRV) and
porcine circovirus 2 (PCV2), are among the most economically damaging
pathogens affecting the swine industry. Importantly, previous studies
have shown that cases of human infection with PRV occur frequently,
indicating the considerable risk of PRV transmission from pigs to
humans. Zinc finger CCCH-type containing 11A (ZC3H11A) has been confirmed
to play a crucial role in maintaining the nuclear export of mRNA under
stress in humans, but its role in pigs remains unknown. In this study,
we observed that ZC3H11A interacted with the transcription and export
complex and played an important role in mRNA export. Specifically,
we knocked out ZC3H11A in PK-15 cells with CRISPR/Cas9 and challenged
them with PRV and PCV2. The results showed that the proliferation
of the virus was significantly inhibited in ZC3H11A–/– cells, indicating that porcine ZC3H11A is indispensable for the
proliferation of PRV and PCV2. Furthermore, our study demonstrated
that the inactivation of ZC3H11A in host cells also inhibited the
proliferation of PRV and PCV2. Taken together, the results of our
study indicated that ZC3H11A is important for maintaining the export
of mRNAs, which in turn facilitates the proliferation of PRV and PCV2,
suggesting that it can be a potential target for producing antiviral
pigs and drugs.
As the standard of living improves, chronic diseases and end-stage organ failure have been a regular occurrence in human beings. Organ transplantation has become one of the hopes in the fight against chronic diseases and end-stage organ failure. However, organs available for transplantation are far from sufficient to meet the demand, leading to a major organ shortage crisis. To solve this problem, researchers have turned to pigs as their target since pigs have many advantages as xenograft donors. Pigs are considered the ideal organ donor for human xenotransplantation, but direct transplantation of porcine organs to humans faces many obstacles, such as hyperacute rejection, acute humoral xenograft rejection, coagulation dysregulation, inflammatory response, coagulation dysregulation, and endogenous porcine retroviral infection. Many transgenic strategies have been developed to overcome these obstacles. This review provides an overview of current advances in genetically modified pigs for xenotransplantation. Future genetic engineering-based delivery of safe and effective organs and tissues for xenotransplantation remains our goal.
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