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Frontline Science: Tryptophan restriction arrests B cell development and enhances microbial diversity in WT and prematurely aging Ercc1-/?7mice

Authors :
Beek, Adriaan A.
Hugenholtz, Floor
Meijer, Ben
Sovran, Bruno
Perdijk, Olaf
Vermeij, Wilbert P.
Brandt, Renata M. C.
Barnhoorn, Sander
Hoeijmakers, Jan H. J.
Vos, Paul
Leenen, Pieter J. M.
Hendriks, Rudi W.
Savelkoul, Huub F. J.
Source :
Journal of Leukocyte Biology; April 2017, Vol. 101 Issue: 4 p811-821, 11p
Publication Year :
2017

Abstract

Dietary Trp restriction linked to B cell development in BM and gut microbial composition. With aging, tryptophan metabolism is affected. Tryptophan has a crucial role in the induction of immune tolerance and the maintenance of gut microbiota. We, therefore, studied the effect of dietary tryptophan restriction in young wild-type (WT) mice (118-wk life span) and in DNA-repair deficient, premature-aged (Ercc1-/?7) mice (20-wk life span). First, we found that the effect of aging on the distribution of B and T cells in bone marrow (BM) and in the periphery of 16-wk-old Ercc1-/?7mice was comparable to that in 18-mo-old WT mice. Dietary tryptophan restriction caused an arrest of B cell development in the BM, accompanied by diminished B cell frequencies in the periphery. In general, old Ercc1-/?7mice showed similar responses to tryptophan restriction compared with young WT mice, indicative of age-independent effects. Dietary tryptophan restriction increased microbial diversity and made the gut microbiota composition of old Ercc1-/?7mice more similar to that of young WT mice. The decreased abundances of Alistipes and Akkermansia spp. after dietary tryptophan restriction correlated significantly with decreased B cell precursor numbers. In conclusion, we report that dietary tryptophan restriction arrests B cell development and concomitantly changes gut microbiota composition. Our study suggests a beneficial interplay between dietary tryptophan, B cell development, and gut microbial composition on several aspects of age-induced changes.

Details

Language :
English
ISSN :
07415400 and 19383673
Volume :
101
Issue :
4
Database :
Supplemental Index
Journal :
Journal of Leukocyte Biology
Publication Type :
Periodical
Accession number :
ejs44318894
Full Text :
https://doi.org/10.1189/jlb.1HI0216-062RR