Widespread Macromolecular Interaction Perturbations in Human Genetic Disorders
- Sahni, Nidhi
- Yi, Song
- Taipale, Mikko
- Fuxman Bass, Juan I.
- Coulombe-Huntington, Jasmin
- Yang, Fan
- Peng, Jian
- Weile, Jochen
- Karras, Georgios I.
- Wang, Yang
- Kovács, István A.
- Kamburov, Atanas
- Krykbaeva, Irina
- Lam, Mandy H.
- Tucker, George
- Khurana, Vikram
- Sharma, Amitabh
- Liu, Yang-Yu
- Yachie, Nozomu
- Zhong, Quan
- Shen, Yun
- Palagi, Alexandre
- San-Miguel, Adriana
- Fan, Changyu
- Balcha, Dawit
- Dricot, Amelie
- Jordan, Daniel M.
- Walsh, Jennifer M.
- Shah, Akash A.
- Yang, Xinping
- Stoyanova, Ani K.
- Leighton, Alex
- Calderwood, Michael A.
- Jacob, Yves
- Cusick, Michael E.
- Salehi-Ashtiani, Kourosh
- Whitesell, Luke J.
- Sunyaev, Shamil
- Berger, Bonnie
- Barabási, Albert-László
- Charloteaux, Benoit
- Hill, David E.
- Hao, Tong
- Roth, Frederick P.
- Xia, Yu
- Walhout, Albertha J.M.
- Lindquist, Susan
- Vidal, Marc
DOIAbstract
SummaryHow disease-associated mutations impair protein activities in the context of biological networks remains mostly undetermined. Although a few renowned alleles are well characterized, functional information is missing for over 100,000 disease-associated variants. Here we functionally profile several thousand missense mutations across a spectrum of Mendelian disorders using various interaction assays. The majority of disease-associated alleles exhibit wild-type chaperone binding profiles, suggesting they preserve protein folding or stability. While common variants from healthy individuals rarely affect interactions, two-thirds of disease-associated alleles perturb protein-protein interactions, with half corresponding to “edgetic” allele...
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