Assessing Lysine and Cysteine Reactivities for Designing Targeted Covalent Kinase Inhibitors
Targeted covalent inhibitor design is gaining increasing interest and acceptance. A typical covalent kinase inhibitor design targets a reactive cysteine; however, this strategy is limited by the low abundance of cysteine and acquired drug resistance from point mutations. Inspired by the recent devel...
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| Veröffentlicht in: | Journal of the American Chemical Society 2019-04, Vol.141 (16), p.6553-6560 |
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| creator | Liu, Ruibin Yue, Zhi Tsai, Cheng-Chieh Shen, Jana |
| description | Targeted covalent inhibitor design is gaining increasing interest and acceptance. A typical covalent kinase inhibitor design targets a reactive cysteine; however, this strategy is limited by the low abundance of cysteine and acquired drug resistance from point mutations. Inspired by the recent development of lysine-targeted chemical probes, we asked if nucleophilic (reactive) catalytic lysines are common on the basis of the published crystal structures of the human kinome. Using a newly developed pK a prediction tool based on continuous constant pH molecular dynamics, the catalytic lysines of eight unique kinases from various human kinase groups were retrospectively and prospectively predicted to be nucleophilic, when kinase is in the rare DFG-out/αC-out type of conformation. Importantly, other reactive lysines as well as cysteines at various locations were also identified. On the basis of the findings, we proposed a new strategy in which selective type II reversible kinase inhibitors are modified to design highly selective, lysine-targeted covalent inhibitors. Traditional covalent drugs were discovered serendipitously; the presented tool, which can assess the reactivities of any potentially targetable residues, may accelerate the rational discovery of new covalent inhibitors. Another significant finding of the work is that lysines and cysteines in kinases may adopt neutral and charged states at physiological pH, respectively. This finding may shift the current paradigm of computational studies of kinases, which assume fixed solution protonation states. |
| doi_str_mv | 10.1021/jacs.8b13248 |
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A typical covalent kinase inhibitor design targets a reactive cysteine; however, this strategy is limited by the low abundance of cysteine and acquired drug resistance from point mutations. Inspired by the recent development of lysine-targeted chemical probes, we asked if nucleophilic (reactive) catalytic lysines are common on the basis of the published crystal structures of the human kinome. Using a newly developed pK a prediction tool based on continuous constant pH molecular dynamics, the catalytic lysines of eight unique kinases from various human kinase groups were retrospectively and prospectively predicted to be nucleophilic, when kinase is in the rare DFG-out/αC-out type of conformation. Importantly, other reactive lysines as well as cysteines at various locations were also identified. On the basis of the findings, we proposed a new strategy in which selective type II reversible kinase inhibitors are modified to design highly selective, lysine-targeted covalent inhibitors. Traditional covalent drugs were discovered serendipitously; the presented tool, which can assess the reactivities of any potentially targetable residues, may accelerate the rational discovery of new covalent inhibitors. Another significant finding of the work is that lysines and cysteines in kinases may adopt neutral and charged states at physiological pH, respectively. 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Am. Chem. Soc</addtitle><description>Targeted covalent inhibitor design is gaining increasing interest and acceptance. A typical covalent kinase inhibitor design targets a reactive cysteine; however, this strategy is limited by the low abundance of cysteine and acquired drug resistance from point mutations. Inspired by the recent development of lysine-targeted chemical probes, we asked if nucleophilic (reactive) catalytic lysines are common on the basis of the published crystal structures of the human kinome. Using a newly developed pK a prediction tool based on continuous constant pH molecular dynamics, the catalytic lysines of eight unique kinases from various human kinase groups were retrospectively and prospectively predicted to be nucleophilic, when kinase is in the rare DFG-out/αC-out type of conformation. Importantly, other reactive lysines as well as cysteines at various locations were also identified. On the basis of the findings, we proposed a new strategy in which selective type II reversible kinase inhibitors are modified to design highly selective, lysine-targeted covalent inhibitors. Traditional covalent drugs were discovered serendipitously; the presented tool, which can assess the reactivities of any potentially targetable residues, may accelerate the rational discovery of new covalent inhibitors. Another significant finding of the work is that lysines and cysteines in kinases may adopt neutral and charged states at physiological pH, respectively. This finding may shift the current paradigm of computational studies of kinases, which assume fixed solution protonation states.</description><subject>crystal structure</subject><subject>cysteine</subject><subject>drug resistance</subject><subject>drugs</subject><subject>enzyme inhibitors</subject><subject>humans</subject><subject>Lewis bases</subject><subject>lysine</subject><subject>molecular dynamics</subject><subject>phosphotransferases (kinases)</subject><subject>point mutation</subject><subject>prediction</subject><subject>protonation</subject><issn>0002-7863</issn><issn>1520-5126</issn><issn>1520-5126</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2019</creationdate><recordtype>article</recordtype><recordid>eNqNkc9rFDEUx4Modlu9eZY5enDa_M7MRShbq6ULgtSbEDKZN9sss0nNm13Y_94MXauCB0-PL_m8b77Jl5A3jJ4zytnFxnk8bzomuGyekQVTnNaKcf2cLCilvDaNFifkFHFTpOQNe0lOBG2lUoItyPdLREAMcV2tDmVA5WJfLQ84wSy-gvNT2IcpAFZDytUVYFjHGb9zeQ0TFDjt3Qhxqm5DdAjVTbwPXZhSxlfkxeBGhNfHeUa-XX-8W36uV18-3SwvV7UrIabaS6WpNFIA8wakECCU44PrqGYgtdG-kczr3qjGqK53TA9FUapMWeidFGfkw6Pvw67bQu9LmOxG-5DD1uWDTS7Yv09iuLfrtLe6FYq3TTF4dzTI6ccOcLLbgB7G0UVIO7ScC6OoEIb-B0oFk6JtVUHfP6I-J8QMw1MiRu3cnZ27s8fuCv72z1c8wb_K-n31vLVJuxzLp_7b6yfuwKOR</recordid><startdate>20190424</startdate><enddate>20190424</enddate><creator>Liu, Ruibin</creator><creator>Yue, Zhi</creator><creator>Tsai, Cheng-Chieh</creator><creator>Shen, Jana</creator><general>American Chemical Society</general><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><scope>7S9</scope><scope>L.6</scope><scope>5PM</scope><orcidid>https://orcid.org/0000-0002-4231-7474</orcidid><orcidid>https://orcid.org/0000-0002-3234-0769</orcidid><orcidid>https://orcid.org/0000-0001-8395-9353</orcidid><orcidid>https://orcid.org/0000-0002-7140-2766</orcidid></search><sort><creationdate>20190424</creationdate><title>Assessing Lysine and Cysteine Reactivities for Designing Targeted Covalent Kinase Inhibitors</title><author>Liu, Ruibin ; Yue, Zhi ; Tsai, Cheng-Chieh ; Shen, Jana</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-a553t-c45604743e1c7e433e35a2fab061e4676c841c6d75875bda16fc6d0057e1cda43</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2019</creationdate><topic>crystal structure</topic><topic>cysteine</topic><topic>drug resistance</topic><topic>drugs</topic><topic>enzyme inhibitors</topic><topic>humans</topic><topic>Lewis bases</topic><topic>lysine</topic><topic>molecular dynamics</topic><topic>phosphotransferases (kinases)</topic><topic>point mutation</topic><topic>prediction</topic><topic>protonation</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Liu, Ruibin</creatorcontrib><creatorcontrib>Yue, Zhi</creatorcontrib><creatorcontrib>Tsai, Cheng-Chieh</creatorcontrib><creatorcontrib>Shen, Jana</creatorcontrib><collection>PubMed</collection><collection>CrossRef</collection><collection>MEDLINE - Academic</collection><collection>AGRICOLA</collection><collection>AGRICOLA - Academic</collection><collection>PubMed Central (Full Participant titles)</collection><jtitle>Journal of the American Chemical Society</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Liu, Ruibin</au><au>Yue, Zhi</au><au>Tsai, Cheng-Chieh</au><au>Shen, Jana</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Assessing Lysine and Cysteine Reactivities for Designing Targeted Covalent Kinase Inhibitors</atitle><jtitle>Journal of the American Chemical Society</jtitle><addtitle>J. Am. Chem. Soc</addtitle><date>2019-04-24</date><risdate>2019</risdate><volume>141</volume><issue>16</issue><spage>6553</spage><epage>6560</epage><pages>6553-6560</pages><issn>0002-7863</issn><issn>1520-5126</issn><eissn>1520-5126</eissn><abstract>Targeted covalent inhibitor design is gaining increasing interest and acceptance. A typical covalent kinase inhibitor design targets a reactive cysteine; however, this strategy is limited by the low abundance of cysteine and acquired drug resistance from point mutations. Inspired by the recent development of lysine-targeted chemical probes, we asked if nucleophilic (reactive) catalytic lysines are common on the basis of the published crystal structures of the human kinome. Using a newly developed pK a prediction tool based on continuous constant pH molecular dynamics, the catalytic lysines of eight unique kinases from various human kinase groups were retrospectively and prospectively predicted to be nucleophilic, when kinase is in the rare DFG-out/αC-out type of conformation. Importantly, other reactive lysines as well as cysteines at various locations were also identified. On the basis of the findings, we proposed a new strategy in which selective type II reversible kinase inhibitors are modified to design highly selective, lysine-targeted covalent inhibitors. Traditional covalent drugs were discovered serendipitously; the presented tool, which can assess the reactivities of any potentially targetable residues, may accelerate the rational discovery of new covalent inhibitors. Another significant finding of the work is that lysines and cysteines in kinases may adopt neutral and charged states at physiological pH, respectively. 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| subjects | crystal structure cysteine drug resistance drugs enzyme inhibitors humans Lewis bases lysine molecular dynamics phosphotransferases (kinases) point mutation prediction protonation |
| title | Assessing Lysine and Cysteine Reactivities for Designing Targeted Covalent Kinase Inhibitors |
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