Author
Listed:
- Albert Escobedo
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Busra Topal
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Micha B. A. Kunze
(University of Copenhagen)
- Juan Aranda
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Giulio Chiesa
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Daniele Mungianu
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Ganeko Bernardo-Seisdedos
(CIC bioGUNE)
- Bahareh Eftekharzadeh
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology)
- Margarida Gairí
(Scientific and Technological Centers University of Barcelona (CCiTUB))
- Roberta Pierattelli
(University of Florence)
- Isabella C. Felli
(University of Florence)
- Tammo Diercks
(CIC bioGUNE)
- Oscar Millet
(CIC bioGUNE)
- Jesús García
(The Barcelona Institute of Science and Technology)
- Modesto Orozco
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology
University of Barcelona)
- Ramon Crehuet
(Institute for Advanced Chemistry of Catalonia (IQAC-CSIC))
- Kresten Lindorff-Larsen
(University of Copenhagen)
- Xavier Salvatella
(The Barcelona Institute of Science and Technology
Joint BSC-IRB Research Programme in Computational Biology
ICREA, Passeig Lluís Companys 23)
Abstract
Polyglutamine (polyQ) tracts are regions of low sequence complexity frequently found in transcription factors. Tract length often correlates with transcriptional activity and expansion beyond specific thresholds in certain human proteins is the cause of polyQ disorders. To study the structural basis of the association between tract length, transcriptional activity and disease, we addressed how the conformation of the polyQ tract of the androgen receptor, associated with spinobulbar muscular atrophy (SBMA), depends on its length. Here we report that this sequence folds into a helical structure stabilized by unconventional hydrogen bonds between glutamine side chains and main chain carbonyl groups, and that its helicity directly correlates with tract length. These unusual hydrogen bonds are bifurcate with the conventional hydrogen bonds stabilizing α-helices. Our findings suggest a plausible rationale for the association between polyQ tract length and androgen receptor transcriptional activity and have implications for establishing the mechanistic basis of SBMA.
Suggested Citation
Albert Escobedo & Busra Topal & Micha B. A. Kunze & Juan Aranda & Giulio Chiesa & Daniele Mungianu & Ganeko Bernardo-Seisdedos & Bahareh Eftekharzadeh & Margarida Gairí & Roberta Pierattelli & Isabell, 2019.
"Side chain to main chain hydrogen bonds stabilize a polyglutamine helix in a transcription factor,"
Nature Communications, Nature, vol. 10(1), pages 1-11, December.
Handle:
RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-09923-2
DOI: 10.1038/s41467-019-09923-2
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