Becerra Celyna Y, Wells Riley K, Kunihiro Braden P, Lee Rosa H, Umeda Lesley, Allan Nina P, Rubas Noelle C, McCracken Trevor A, Nunokawa Chandler K L, Lee Ming-Hao, Pidlaoan Felix Gerard S, Phankitnirondorn Krit, Dye Christian K, Yamamoto Brennan Y, Peres Rafael, Juarez Ruben, Maunakea Alika K
Department of Anatomy, Biochemistry, and Physiology, John A. Burns School of Medicine, Honolulu, HI, United States.
IDeA Networks of Biomedical Research Excellence (INBRE), University of Hawaii at Manoa, Honolulu, HI, United States.
Front Genet. 2023 Apr 19;14:1125217. doi: 10.3389/fgene.2023.1125217. eCollection 2023.
Native Hawaiian and other Pacific Islander (NHPI) populations experience higher rates of immunometabolic diseases compared to other racial-ethnic groups in Hawaii. As annual NHPI mortality rates for suicide and type 2 diabetes mellitus (T2DM) exceed those of the state as a whole, understanding the social and biological mechanisms underlying these disparities are urgently needed to enable preventive strategies. A community-based approach was used to investigate the immunoepigenetic-gut microbiome axis in an NHPI-enriched cohort of Oahu residents ( = 68). Self-esteem (SE) data was collected using a modified Rosenberg self-esteem (SE) assessment as a proxy measure for mental wellbeing in consideration for cultural competency. T2DM status was evaluated using point-of-care A1c (%) tests. Stool samples were collected for 16s-based metagenomic sequencing analyses. Plasma from blood samples were isolated by density-gradient centrifugation. Peripheral blood mononuclear cells (PBMCs) were collected from the same samples and enriched for monocytes using negative selection techniques. Flow-cytometry was used for immunoprofiling assays. Monocyte DNA was extracted for Illumina EPIC array-based methylation analysis. Compared to individuals with normal SE (NSE), those with low SE (LSE) exhibited significantly higher plasma concentrations (pg/ml) of proinflammatory cytokines IL-8 ( = 0.051) and TNF-α ( = 0.011). Metagenomic analysis revealed that the relative abundance (%) of specific gut bacteria significantly differed between SE groups - some of which directly correlated with SE scores. Gene ontology analysis revealed that 104 significantly differentially methylated loci (DML) between SE groups were preferentially located at genes involved in immunometabolic processes. Horvath clock analyses indicated epigenetic age (Epi-Age) deceleration in individuals with LSE and acceleration in individuals with NSE ( = 0.042), yet was not reproduced by other clocks. These data reveal novel differences in the immunoepigenetic-gut microbiome axis with respect to SE, warranting further investigation into its relationship to brain activity and mental health in NHPI. Unexpected results from Epi-Age analyses warrant further investigation into the relationship between biological age and disparate health outcomes among the NHPI population. The modifiable component of epigenetic processes and the gut microbiome makes this axis an attractive target for potential therapeutics, biomarker discovery, and novel prevention strategies.
与夏威夷其他种族群体相比,夏威夷原住民和其他太平洋岛民(NHPI)人群患免疫代谢疾病的比率更高。由于NHPI人群的自杀和2型糖尿病(T2DM)年度死亡率超过了整个夏威夷州,因此迫切需要了解这些差异背后的社会和生物学机制,以制定预防策略。本研究采用基于社区的方法,对瓦胡岛居民中NHPI富集队列(n = 68)的免疫表观遗传-肠道微生物群轴进行了调查。考虑到文化适应性,使用改良的罗森伯格自尊(SE)评估收集自尊(SE)数据,作为心理健康的替代指标。使用即时护理糖化血红蛋白(A1c,%)测试评估T2DM状态。收集粪便样本进行基于16S的宏基因组测序分析。通过密度梯度离心从血样中分离血浆。从相同样本中收集外周血单核细胞(PBMC),并使用阴性选择技术富集单核细胞。采用流式细胞术进行免疫表型分析。提取单核细胞DNA,进行基于Illumina EPIC芯片的甲基化分析。与正常自尊(NSE)个体相比,低自尊(LSE)个体的促炎细胞因子IL-8(p = 0.051)和TNF-α(p = 0.011)的血浆浓度(pg/ml)显著更高。宏基因组分析显示,特定肠道细菌的相对丰度(%)在不同自尊组之间存在显著差异,其中一些与自尊评分直接相关。基因本体分析显示,自尊组之间104个显著差异甲基化位点(DML)优先位于参与免疫代谢过程的基因上。霍瓦斯时钟分析表明,低自尊个体的表观遗传年龄(Epi-Age)减速,正常自尊个体的表观遗传年龄加速(p = 0.042),但其他时钟未重现这一结果。这些数据揭示了免疫表观遗传-肠道微生物群轴在自尊方面的新差异,值得进一步研究其与NHPI人群大脑活动和心理健康的关系。表观遗传年龄分析的意外结果值得进一步研究NHPI人群中生物学年龄与不同健康结果之间的关系。表观遗传过程和肠道微生物群的可调节成分使该轴成为潜在治疗、生物标志物发现和新型预防策略的有吸引力的靶点。
