4.8 Article

Regional variation limits applications of healthy gut microbiome reference ranges and disease models

Journal

NATURE MEDICINE
Volume 24, Issue 10, Pages 1532-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41591-018-0164-x

Keywords

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Funding

  1. National Projects of Major Infectious Disease Control and Prevention [2017ZX10103011]
  2. National Natural Science Foundation of China [NSFC31570497, 31322003, 81671171]
  3. China Postdoctoral Science Foundation [C1090132]
  4. Science and Technology Planning Project of Guangdong Province, China [2015A030401055]

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Dysbiosis, departure of the gut microbiome from a healthy state, has been suggested to be a powerful biomarker of disease incidence and progression(1-3). Diagnostic applications have been proposed for inflammatory bowel disease diagnosis and prognosis(4), colorectal cancer prescreening(5) and therapeutic choices in melanoma(6). Noninvasive sampling could facilitate large-scale public health applications, including early diagnosis and risk assessment in metabolic(7) and cardiovascular diseases(8). To understand the generalizability of microbiota-based diagnostic models of metabolic disease, we characterized the gut microbiota of 7,009 individuals from 14 districts within 1 province in China. Among phenotypes, host location showed the strongest associations with microbiota variations. Microbiota-based metabolic disease models developed in one location failed when used elsewhere, suggesting that such models cannot be extrapolated. Interpolated models performed much better, especially in diseases with obvious microbiota-related characteristics. Interpolation efficiency decreased as geographic scale increased, indicating a need to build localized baseline and disease models to predict metabolic risks.

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