Author
Listed:
- Alexander K. Beaver
(Johns Hopkins School of Medicine
Johns Hopkins Bloomberg School of Public Health)
- Zhibek Keneskhanova
(Ludwig-Maximilians-Universität München
Ludwig-Maximilians-Universität München)
- Raúl O. Cosentino
(Ludwig-Maximilians-Universität München
Ludwig-Maximilians-Universität München)
- Brian L. Weiss
(Yale School of Public Health)
- Erick O. Awuoche
(Yale School of Public Health)
- Gretchen M. Smallenberger
(Yale School of Public Health)
- Gracyn Y. Buenconsejo
(Johns Hopkins Bloomberg School of Public Health)
- Nathan P. Crilly
(Johns Hopkins School of Medicine
Johns Hopkins Bloomberg School of Public Health)
- Jaclyn E. Smith
(Johns Hopkins Bloomberg School of Public Health)
- Jill M. C. Hakim
(Johns Hopkins Bloomberg School of Public Health)
- Bailin Zhang
(Johns Hopkins Bloomberg School of Public Health)
- Bryce Bobb
(Johns Hopkins Bloomberg School of Public Health)
- Filipa Rijo-Ferreira
(Berkeley Public Health Molecular and Cell Biology Department)
- Luisa M. Figueiredo
(Gulbenkian Institute for Molecular Medicine)
- Serap Aksoy
(Yale School of Public Health)
- T. Nicolai Siegel
(Ludwig-Maximilians-Universität München
Ludwig-Maximilians-Universität München)
- Monica R. Mugnier
(Johns Hopkins Bloomberg School of Public Health)
Abstract
The protozoan parasite Trypanosoma brucei evades clearance by the host immune system through antigenic variation of its dense variant surface glycoprotein (VSG) coat, periodically ‘switching’ expression of the VSG using a large genomic repertoire of VSG-encoding genes1–6. Recent studies of antigenic variation in vivo have focused near exclusively on parasites in the bloodstream6–8, but research has shown that many, if not most, parasites reside in the interstitial spaces of tissues9–13. We sought to explore the dynamics of antigenic variation in extravascular parasite populations using VSG-seq7, a high-throughput sequencing approach for profiling VSGs expressed in populations of T. brucei. Here we show that tissues, not the blood, are the primary reservoir of antigenic diversity during both needle- and tsetse bite-initiated T. brucei infections, with more than 75% of VSGs found exclusively within extravascular spaces. We found that this increased diversity is correlated with slower parasite clearance in tissue spaces. Together, these data support a model in which the slower immune response in extravascular spaces provides more time to generate the antigenic diversity needed to maintain a chronic infection. Our findings reveal the important role that extravascular spaces can have in pathogen diversification.
Suggested Citation
Alexander K. Beaver & Zhibek Keneskhanova & Raúl O. Cosentino & Brian L. Weiss & Erick O. Awuoche & Gretchen M. Smallenberger & Gracyn Y. Buenconsejo & Nathan P. Crilly & Jaclyn E. Smith & Jill M. C. , 2024.
"Tissue spaces are reservoirs of antigenic diversity for Trypanosoma brucei,"
Nature, Nature, vol. 636(8042), pages 430-437, December.
Handle:
RePEc:nat:nature:v:636:y:2024:i:8042:d:10.1038_s41586-024-08151-z
DOI: 10.1038/s41586-024-08151-z
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