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Article Publish Status: FREE
Abstract Title:

Docosahexaenoic acid supplementation represses the early immune response against murine cytomegalovirus but enhances NK cell effector function.

Abstract Source:

BMC Immunol. 2022 04 19 ;23(1):17. Epub 2022 Apr 19. PMID: 35439922

Abstract Author(s):

Shuting Wu, Shanshan Wang, Lili Wang, Hongyan Peng, Shuju Zhang, Qinglan Yang, Minghui Huang, Yana Li, Shuzhen Guan, Wenjuan Jiang, Zhaohui Zhang, Qinghua Bi, Liping Li, Yuan Gao, Peiwen Xiong, Zhaoyang Zhong, Bo Xu, Yafei Deng, Youcai Deng

Article Affiliation:

Shuting Wu

Abstract:

BACKGROUND: Docosahexaenoic acid (DHA) supplementation is beneficial for several chronic diseases; however, its effect on immune regulation is still debated. Given the prevalence of cytomegalovirus (CMV) infection and because natural killer (NK) cells are a component of innate immunity critical for controlling CMV infection, the current study explored the effect of a DHA-enriched diet on susceptibility to murine (M) CMV infection and the NK cell effector response to MCMV infection.

RESULTS: Male C57BL/6 mice fed a control or DHA-enriched diet for 3 weeks were infected with MCMV and sacrificed at the indicated time points postinfection. Compared with control mice, DHA-fed mice had higher liver and spleen viral loads at day 7 postinfection, but final MCMV clearance was not affected. The total numbers of NK cells and their terminal mature cellsubset (KLRG1and Ly49HNK cells) were reduced compared with those in control mice at day 7 postinfection but not day 21. DHA feeding resulted in higher IFN-γ and granzyme B expression in splenic NK cells at day 7 postinfection. A mechanistic analysis showed that the splenic NK cells of DHA-fed mice had enhanced glucose uptake, increased CD71 and CD98 expression, and higher mitochondrial mass than control mice. In addition, DHA-fed mice showed reductions in the total numbers and activation levels of CD4and CD8T cells.

CONCLUSIONS: These results suggest that DHA supplementation represses the early response to CMV infection but preserves NK cell effector functions by improving mitochondrial activity, which may play critical roles in subsequent MCMV clearance.

Study Type : Animal Study

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