4.6 Article

Transmission of Atherosclerosis Susceptibility with Gut Microbial Transplantation

期刊

JOURNAL OF BIOLOGICAL CHEMISTRY
卷 290, 期 9, 页码 5647-5660

出版社

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M114.618249

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资金

  1. National Institutes of Health from the Office of Dietary Supplements [R01 HL103866, P20 HL113452, HL28481, HL30568]
  2. Cleveland Heart Lab, Inc.
  3. Esperion
  4. Liposciences Inc.
  5. Merck Co., Inc.
  6. Pfizer Inc.
  7. Proctor Gamble
  8. Abbott
  9. Cleveland HeartLab
  10. Liposciences, Inc.
  11. Takeda
  12. National Institutes of Health [T32 GM088088]
  13. MOBILITAS [MJD252]
  14. FP7-People-IOF from the European Union [330381]

向作者/读者索取更多资源

Recent studies indicate both clinical and mechanistic links between atherosclerotic heart disease and intestinal microbial metabolism of certain dietary nutrients producing trimethylamine N-oxide (TMAO). Here we test the hypothesis that gut microbial transplantation can transmit choline diet-induced TMAO production and atherosclerosis susceptibility. First, a strong association was noted between atherosclerotic plaque and plasma TMAO levels in a mouse diversity panel (n = 22 strains, r = 0.38;p = 0.0001). An atherosclerosis-prone and high TMAO-producing strain, C57BL/6J, and an atherosclerosis-resistant and low TMAO-producing strain, NZW/LacJ, were selected as donors for cecal microbial transplantation into apolipoprotein e null mice in which resident intestinal microbes were first suppressed with antibiotics. Trimethylamine (TMA) and TmAo levels were initially higher in recipients on choline diet that received cecal microbes from C57B1/6J inbred mice; however, durability of choline diet-dependent differences in TMA/TMAO levels was not maintained to the end of the study. Mice receiving C57BL/6J cecal microbes demonstrated choline diet-dependent enhancement in atherosclerotic plaque burden as compared with recipients of NZW/LacJ microbes. Microbial DNA analyses in feces and cecum revealed transplantation of donor microbial community features into recipients with differences in taxa proportions between donor strains that were transmissible to recipients and that tended to show coincident proportions with TMA() levels. Proportions of specific taxa were also identified that correlated with plasma TmAo levels in donors and recipients and with atherosclerotic lesion area in recipients. Atherosclerosis susceptibility may be transmitted via transplantation of gut microbiota. Gut microbes may thus represent a novel therapeutic target for modulating atherosclerosis susceptibility.

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