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Activin receptor
From Proteopedia
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'''Activin receptors''' (Acvr) are integral to the activin and myostatin signalling pathway. Binding of activin to the Acvr on muscle cell membrane leads to enhanced muscle protein breakdown and debilitating loss of muscle mass and functional capacity<ref>PMID:23721881</ref>. | '''Activin receptors''' (Acvr) are integral to the activin and myostatin signalling pathway. Binding of activin to the Acvr on muscle cell membrane leads to enhanced muscle protein breakdown and debilitating loss of muscle mass and functional capacity<ref>PMID:23721881</ref>. | ||
| + | *'''Acvr1''' is involved in bone, heart, cartilage, nervous and reproductive system development and regulation<ref>PMID:31683698</ref>. | ||
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| + | See also: [[Enzyme-linked receptor]]. | ||
== Disease == | == Disease == | ||
| - | A mutation in | + | A mutation in Acvr1 exists in individuals with the rare developmental disorder fibrodysplasia ossificans progressiva<ref>PMID:28918311</ref>. |
== Relevance == | == Relevance == | ||
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**[[6acr]], [[6gi6]], [[6gip]], [[6gin]], [[4bgg]], [[3q4u]], [[3mtf]], [[6t6d]], [[6jux]], [[6tnb]], [[6tn8]], [[6t8n]], [[6szm]], [[6eix]], [[6srh]], [[5oy6]], [[6z36]], [[6zgc]], [[7a21]], [[7c3g]] - hAcvr1 kinase domain (mutant) + inhibitor<br /> | **[[6acr]], [[6gi6]], [[6gip]], [[6gin]], [[4bgg]], [[3q4u]], [[3mtf]], [[6t6d]], [[6jux]], [[6tnb]], [[6tn8]], [[6t8n]], [[6szm]], [[6eix]], [[6srh]], [[5oy6]], [[6z36]], [[6zgc]], [[7a21]], [[7c3g]] - hAcvr1 kinase domain (mutant) + inhibitor<br /> | ||
**[[3h9r]], [[4c02]], [[6i1s]] - hAcvr1 kinase domain + FKBP12 + inhibitor<br /> | **[[3h9r]], [[4c02]], [[6i1s]] - hAcvr1 kinase domain + FKBP12 + inhibitor<br /> | ||
| + | **[[7nns]] - hAcvr1 kinase domain + drug<br /> | ||
*Activin receptor type 2 | *Activin receptor type 2 | ||
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**[[4asx]], [[3soc]], [[3q4t]] - hAcvr2A kinase domain + inhibitor<br /> | **[[4asx]], [[3soc]], [[3q4t]] - hAcvr2A kinase domain + inhibitor<br /> | ||
**[[5nh3]] - hAcvr2A LBD + antibody<br /> | **[[5nh3]] - hAcvr2A LBD + antibody<br /> | ||
| + | **[[7u5p]] - hAcvr2A LBD + inhibin<br /> | ||
**[[2goo]], [[2h64]], [[2h62]] - mAcvr2A LBD + BMP-2 + ALK3<br /> | **[[2goo]], [[2h64]], [[2h62]] - mAcvr2A LBD + BMP-2 + ALK3<br /> | ||
**[[1lx5]] - mAcvr2A LBD + BMP-7<br /> | **[[1lx5]] - mAcvr2A LBD + BMP-7<br /> | ||
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**[[2qlu]] - hAcvr2B kinase domain<br /> | **[[2qlu]] - hAcvr2B kinase domain<br /> | ||
**[[5ngv]], [[5nhr]] - hAcvr2B LBD + antibody<br /> | **[[5ngv]], [[5nhr]] - hAcvr2B LBD + antibody<br /> | ||
| + | **[[7oly]] - hAcvr2B LBD + hAcvr1B LBD + antibody + inhibin<br /> | ||
| + | **[[7mrz]] - hAcvr2B LBD + hAcvr1B LBD + antibody + GDF11<br /> | ||
**[[1s4y]] - mAcvr2B LBD + inhibin<br /> | **[[1s4y]] - mAcvr2B LBD + inhibin<br /> | ||
**[[1nyu]] - rAcvr2B LBD + inhibin - rat<br /> | **[[1nyu]] - rAcvr2B LBD + inhibin - rat<br /> | ||
Current revision
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3D structures of activin receptor
Updated on 21-May-2024
References
- ↑ Han HQ, Zhou X, Mitch WE, Goldberg AL. Myostatin/activin pathway antagonism: molecular basis and therapeutic potential. Int J Biochem Cell Biol. 2013 Oct;45(10):2333-47. doi:, 10.1016/j.biocel.2013.05.019. Epub 2013 May 28. PMID:23721881 doi:http://dx.doi.org/10.1016/j.biocel.2013.05.019
- ↑ Valer JA, Sánchez-de-Diego C, Pimenta-Lopes C, Rosa JL, Ventura F. ACVR1 Function in Health and Disease. Cells. 2019 Oct 31;8(11):1366. PMID:31683698 doi:10.3390/cells8111366
- ↑ Williams E, Bullock AN. Structural basis for the potent and selective binding of LDN-212854 to the BMP receptor kinase ALK2. Bone. 2017 Sep 12. pii: S8756-3282(17)30340-X. doi: 10.1016/j.bone.2017.09.004. PMID:28918311 doi:http://dx.doi.org/10.1016/j.bone.2017.09.004
- ↑ Roh JD, Hobson R, Chaudhari V, Quintero P, Yeri A, Benson M, Xiao C, Zlotoff D, Bezzerides V, Houstis N, Platt C, Damilano F, Lindman BR, Elmariah S, Biersmith M, Lee SJ, Seidman CE, Seidman JG, Gerszten RE, Lach-Trifilieff E, Glass DJ, Rosenzweig A. Activin type II receptor signaling in cardiac aging and heart failure. Sci Transl Med. 2019 Mar 6;11(482). pii: 11/482/eaau8680. doi:, 10.1126/scitranslmed.aau8680. PMID:30842316 doi:http://dx.doi.org/10.1126/scitranslmed.aau8680
- ↑ Mohedas AH, Wang Y, Sanvitale CE, Canning P, Choi S, Xing X, Bullock AN, Cuny GD, Yu PB. Structure-activity relationship of 3,5-diaryl-2-aminopyridine ALK2 inhibitors reveals unaltered binding affinity for fibrodysplasia ossificans progressiva causing mutants. J Med Chem. 2014 Oct 9;57(19):7900-15. doi: 10.1021/jm501177w. Epub 2014 Sep 4. PMID:25101911 doi:http://dx.doi.org/10.1021/jm501177w
