Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells
Simple Summary Glucocorticoid therapy resistance in B-cell malignancies is often associated with constitutive activation of tyrosine kinases. Novel anticancer drugs targeting hyperactivated tyrosine kinases, such as Bruton's tyrosine kinase (BTK), have, therefore, gained much interest over the...
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| creator | Logie, Emilie Chirumamilla, Chandra S Perez-Novo, Claudina Shaw, Priyanka Declerck, Ken Palagani, Ajay Rangarajan, Savithri Cuypers, Bart De Neuter, Nicolas Mobashar Hussain Urf Turabe, Fazil Kumar Verma, Navin Bogaerts, Annemie Laukens, Kris Offner, Fritz Van Vlierberghe, Pieter Van Ostade, Xaveer Berghe, Wim Vanden |
| description | Simple Summary Glucocorticoid therapy resistance in B-cell malignancies is often associated with constitutive activation of tyrosine kinases. Novel anticancer drugs targeting hyperactivated tyrosine kinases, such as Bruton's tyrosine kinase (BTK), have, therefore, gained much interest over the past few decades and have already been approved for clinical use. In this study, we compared the therapeutic efficacy of the phytochemical kinase inhibitor withaferin A with the clinically approved BTK inhibitor ibrutinib to target hyperactivated tyrosine kinase signaling in glucocorticoid-resistant multiple myeloma cells. Our results demonstrate that withaferin A-induced cell death of glucocorticoid-resistant MM1R cells involves covalent cysteine targeting of multiple Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including BTK. Multiple myeloma (MM) is a hematological malignancy characterized by plasma cells' uncontrolled growth. The major barrier in treating MM is the occurrence of primary and acquired therapy resistance to anticancer drugs. Often, this therapy resistance is associated with constitutive hyperactivation of tyrosine kinase signaling. Novel covalent kinase inhibitors, such as the clinically approved BTK inhibitor ibrutinib (IBR) and the preclinical phytochemical withaferin A (WA), have, therefore, gained pharmaceutical interest. Remarkably, WA is more effective than IBR in killing BTK-overexpressing glucocorticoid (GC)-resistant MM1R cells. To further characterize the kinase inhibitor profiles of WA and IBR in GC-resistant MM cells, we applied phosphopeptidome- and transcriptome-specific tyrosine kinome profiling. In contrast to IBR, WA was found to reverse BTK overexpression in GC-resistant MM1R cells. Furthermore, WA-induced cell death involves covalent cysteine targeting of Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including inhibition of the hyperactivated BTK. Covalent interaction between WA and BTK could further be confirmed by biotin-based affinity purification and confocal microscopy. Similarly, molecular modeling suggests WA preferably targets conserved cysteines in the Hinge-6 region of the kinase cysteinome classification, favoring inhibition of multiple B-cell receptors (BCR) family kinases. Altogether, we show that WA's promiscuous inhibition of multiple BTK family tyrosine kinases represents a highly effective strategy to overcome GC-therapy resistance in MM. |
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| fullrecord | <record><control><sourceid>ghent</sourceid><recordid>TN_cdi_ghent_librecat_oai_archive_ugent_be_8711103</recordid><sourceformat>XML</sourceformat><sourcesystem>PC</sourcesystem><sourcerecordid>oai_archive_ugent_be_8711103</sourcerecordid><originalsourceid>FETCH-ghent_librecat_oai_archive_ugent_be_87111033</originalsourceid><addsrcrecordid>eNqdj81KxEAMx4souOi-Q27qobDTlVaP7qIIsre9l3Q2baPTGZlkKn0XH9YWPHg2lwR-5P9xlq2KTVXkZfl4f_7nvszWIu-bebZbU5XVKvvehxEdeQU7iRJ7AsXYkbLvILSwi0mDvxHQKQZZ8Ad7FILb3fHtDloc2E3QTPDF2mNLkX3-BJFOyZKApDjyrL8odS7ZYENUtoFPeSRhUZyNh-SUPx3BMJELA8LhYMCSc3KdXbTohNa_-yorXp6P-9e86-fEteMmkkWtA3KN0fY8Up26BTVUP1TGmLnnv55-ANtZahk</addsrcrecordid><sourcetype>Institutional Repository</sourcetype><iscdi>true</iscdi><recordtype>article</recordtype></control><display><type>article</type><title>Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells</title><source>MDPI - Multidisciplinary Digital Publishing Institute</source><source>Ghent University Academic Bibliography</source><source>Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals</source><source>PubMed Central</source><source>PubMed Central Open Access</source><creator>Logie, Emilie ; Chirumamilla, Chandra S ; Perez-Novo, Claudina ; Shaw, Priyanka ; Declerck, Ken ; Palagani, Ajay ; Rangarajan, Savithri ; Cuypers, Bart ; De Neuter, Nicolas ; Mobashar Hussain Urf Turabe, Fazil ; Kumar Verma, Navin ; Bogaerts, Annemie ; Laukens, Kris ; Offner, Fritz ; Van Vlierberghe, Pieter ; Van Ostade, Xaveer ; Berghe, Wim Vanden</creator><creatorcontrib>Logie, Emilie ; Chirumamilla, Chandra S ; Perez-Novo, Claudina ; Shaw, Priyanka ; Declerck, Ken ; Palagani, Ajay ; Rangarajan, Savithri ; Cuypers, Bart ; De Neuter, Nicolas ; Mobashar Hussain Urf Turabe, Fazil ; Kumar Verma, Navin ; Bogaerts, Annemie ; Laukens, Kris ; Offner, Fritz ; Van Vlierberghe, Pieter ; Van Ostade, Xaveer ; Berghe, Wim Vanden</creatorcontrib><description>Simple Summary Glucocorticoid therapy resistance in B-cell malignancies is often associated with constitutive activation of tyrosine kinases. Novel anticancer drugs targeting hyperactivated tyrosine kinases, such as Bruton's tyrosine kinase (BTK), have, therefore, gained much interest over the past few decades and have already been approved for clinical use. In this study, we compared the therapeutic efficacy of the phytochemical kinase inhibitor withaferin A with the clinically approved BTK inhibitor ibrutinib to target hyperactivated tyrosine kinase signaling in glucocorticoid-resistant multiple myeloma cells. Our results demonstrate that withaferin A-induced cell death of glucocorticoid-resistant MM1R cells involves covalent cysteine targeting of multiple Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including BTK. Multiple myeloma (MM) is a hematological malignancy characterized by plasma cells' uncontrolled growth. The major barrier in treating MM is the occurrence of primary and acquired therapy resistance to anticancer drugs. Often, this therapy resistance is associated with constitutive hyperactivation of tyrosine kinase signaling. Novel covalent kinase inhibitors, such as the clinically approved BTK inhibitor ibrutinib (IBR) and the preclinical phytochemical withaferin A (WA), have, therefore, gained pharmaceutical interest. Remarkably, WA is more effective than IBR in killing BTK-overexpressing glucocorticoid (GC)-resistant MM1R cells. To further characterize the kinase inhibitor profiles of WA and IBR in GC-resistant MM cells, we applied phosphopeptidome- and transcriptome-specific tyrosine kinome profiling. In contrast to IBR, WA was found to reverse BTK overexpression in GC-resistant MM1R cells. Furthermore, WA-induced cell death involves covalent cysteine targeting of Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including inhibition of the hyperactivated BTK. Covalent interaction between WA and BTK could further be confirmed by biotin-based affinity purification and confocal microscopy. Similarly, molecular modeling suggests WA preferably targets conserved cysteines in the Hinge-6 region of the kinase cysteinome classification, favoring inhibition of multiple B-cell receptors (BCR) family kinases. Altogether, we show that WA's promiscuous inhibition of multiple BTK family tyrosine kinases represents a highly effective strategy to overcome GC-therapy resistance in MM.</description><identifier>ISSN: 2072-6694</identifier><identifier>EISSN: 2072-6694</identifier><language>eng</language><subject>Biology and Life Sciences ; BTK ; glucocorticoids ; ibrutinib ; Medicine and Health Sciences ; multiple myeloma ; therapy resistance ; withaferin A</subject><creationdate>2021</creationdate><rights>Creative Commons Attribution 4.0 International Public License (CC-BY 4.0) info:eu-repo/semantics/openAccess</rights><lds50>peer_reviewed</lds50><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,315,776,780,4010,27837</link.rule.ids></links><search><creatorcontrib>Logie, Emilie</creatorcontrib><creatorcontrib>Chirumamilla, Chandra S</creatorcontrib><creatorcontrib>Perez-Novo, Claudina</creatorcontrib><creatorcontrib>Shaw, Priyanka</creatorcontrib><creatorcontrib>Declerck, Ken</creatorcontrib><creatorcontrib>Palagani, Ajay</creatorcontrib><creatorcontrib>Rangarajan, Savithri</creatorcontrib><creatorcontrib>Cuypers, Bart</creatorcontrib><creatorcontrib>De Neuter, Nicolas</creatorcontrib><creatorcontrib>Mobashar Hussain Urf Turabe, Fazil</creatorcontrib><creatorcontrib>Kumar Verma, Navin</creatorcontrib><creatorcontrib>Bogaerts, Annemie</creatorcontrib><creatorcontrib>Laukens, Kris</creatorcontrib><creatorcontrib>Offner, Fritz</creatorcontrib><creatorcontrib>Van Vlierberghe, Pieter</creatorcontrib><creatorcontrib>Van Ostade, Xaveer</creatorcontrib><creatorcontrib>Berghe, Wim Vanden</creatorcontrib><title>Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells</title><description>Simple Summary Glucocorticoid therapy resistance in B-cell malignancies is often associated with constitutive activation of tyrosine kinases. Novel anticancer drugs targeting hyperactivated tyrosine kinases, such as Bruton's tyrosine kinase (BTK), have, therefore, gained much interest over the past few decades and have already been approved for clinical use. In this study, we compared the therapeutic efficacy of the phytochemical kinase inhibitor withaferin A with the clinically approved BTK inhibitor ibrutinib to target hyperactivated tyrosine kinase signaling in glucocorticoid-resistant multiple myeloma cells. Our results demonstrate that withaferin A-induced cell death of glucocorticoid-resistant MM1R cells involves covalent cysteine targeting of multiple Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including BTK. Multiple myeloma (MM) is a hematological malignancy characterized by plasma cells' uncontrolled growth. The major barrier in treating MM is the occurrence of primary and acquired therapy resistance to anticancer drugs. Often, this therapy resistance is associated with constitutive hyperactivation of tyrosine kinase signaling. Novel covalent kinase inhibitors, such as the clinically approved BTK inhibitor ibrutinib (IBR) and the preclinical phytochemical withaferin A (WA), have, therefore, gained pharmaceutical interest. Remarkably, WA is more effective than IBR in killing BTK-overexpressing glucocorticoid (GC)-resistant MM1R cells. To further characterize the kinase inhibitor profiles of WA and IBR in GC-resistant MM cells, we applied phosphopeptidome- and transcriptome-specific tyrosine kinome profiling. In contrast to IBR, WA was found to reverse BTK overexpression in GC-resistant MM1R cells. Furthermore, WA-induced cell death involves covalent cysteine targeting of Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including inhibition of the hyperactivated BTK. Covalent interaction between WA and BTK could further be confirmed by biotin-based affinity purification and confocal microscopy. Similarly, molecular modeling suggests WA preferably targets conserved cysteines in the Hinge-6 region of the kinase cysteinome classification, favoring inhibition of multiple B-cell receptors (BCR) family kinases. Altogether, we show that WA's promiscuous inhibition of multiple BTK family tyrosine kinases represents a highly effective strategy to overcome GC-therapy resistance in MM.</description><subject>Biology and Life Sciences</subject><subject>BTK</subject><subject>glucocorticoids</subject><subject>ibrutinib</subject><subject>Medicine and Health Sciences</subject><subject>multiple myeloma</subject><subject>therapy resistance</subject><subject>withaferin A</subject><issn>2072-6694</issn><issn>2072-6694</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2021</creationdate><recordtype>article</recordtype><sourceid>ADGLB</sourceid><recordid>eNqdj81KxEAMx4souOi-Q27qobDTlVaP7qIIsre9l3Q2baPTGZlkKn0XH9YWPHg2lwR-5P9xlq2KTVXkZfl4f_7nvszWIu-bebZbU5XVKvvehxEdeQU7iRJ7AsXYkbLvILSwi0mDvxHQKQZZ8Ad7FILb3fHtDloc2E3QTPDF2mNLkX3-BJFOyZKApDjyrL8odS7ZYENUtoFPeSRhUZyNh-SUPx3BMJELA8LhYMCSc3KdXbTohNa_-yorXp6P-9e86-fEteMmkkWtA3KN0fY8Up26BTVUP1TGmLnnv55-ANtZahk</recordid><startdate>2021</startdate><enddate>2021</enddate><creator>Logie, Emilie</creator><creator>Chirumamilla, Chandra S</creator><creator>Perez-Novo, Claudina</creator><creator>Shaw, Priyanka</creator><creator>Declerck, Ken</creator><creator>Palagani, Ajay</creator><creator>Rangarajan, Savithri</creator><creator>Cuypers, Bart</creator><creator>De Neuter, Nicolas</creator><creator>Mobashar Hussain Urf Turabe, Fazil</creator><creator>Kumar Verma, Navin</creator><creator>Bogaerts, Annemie</creator><creator>Laukens, Kris</creator><creator>Offner, Fritz</creator><creator>Van Vlierberghe, Pieter</creator><creator>Van Ostade, Xaveer</creator><creator>Berghe, Wim Vanden</creator><scope>ADGLB</scope></search><sort><creationdate>2021</creationdate><title>Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells</title><author>Logie, Emilie ; Chirumamilla, Chandra S ; Perez-Novo, Claudina ; Shaw, Priyanka ; Declerck, Ken ; Palagani, Ajay ; Rangarajan, Savithri ; Cuypers, Bart ; De Neuter, Nicolas ; Mobashar Hussain Urf Turabe, Fazil ; Kumar Verma, Navin ; Bogaerts, Annemie ; Laukens, Kris ; Offner, Fritz ; Van Vlierberghe, Pieter ; Van Ostade, Xaveer ; Berghe, Wim Vanden</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-ghent_librecat_oai_archive_ugent_be_87111033</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2021</creationdate><topic>Biology and Life Sciences</topic><topic>BTK</topic><topic>glucocorticoids</topic><topic>ibrutinib</topic><topic>Medicine and Health Sciences</topic><topic>multiple myeloma</topic><topic>therapy resistance</topic><topic>withaferin A</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Logie, Emilie</creatorcontrib><creatorcontrib>Chirumamilla, Chandra S</creatorcontrib><creatorcontrib>Perez-Novo, Claudina</creatorcontrib><creatorcontrib>Shaw, Priyanka</creatorcontrib><creatorcontrib>Declerck, Ken</creatorcontrib><creatorcontrib>Palagani, Ajay</creatorcontrib><creatorcontrib>Rangarajan, Savithri</creatorcontrib><creatorcontrib>Cuypers, Bart</creatorcontrib><creatorcontrib>De Neuter, Nicolas</creatorcontrib><creatorcontrib>Mobashar Hussain Urf Turabe, Fazil</creatorcontrib><creatorcontrib>Kumar Verma, Navin</creatorcontrib><creatorcontrib>Bogaerts, Annemie</creatorcontrib><creatorcontrib>Laukens, Kris</creatorcontrib><creatorcontrib>Offner, Fritz</creatorcontrib><creatorcontrib>Van Vlierberghe, Pieter</creatorcontrib><creatorcontrib>Van Ostade, Xaveer</creatorcontrib><creatorcontrib>Berghe, Wim Vanden</creatorcontrib><collection>Ghent University Academic Bibliography</collection></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Logie, Emilie</au><au>Chirumamilla, Chandra S</au><au>Perez-Novo, Claudina</au><au>Shaw, Priyanka</au><au>Declerck, Ken</au><au>Palagani, Ajay</au><au>Rangarajan, Savithri</au><au>Cuypers, Bart</au><au>De Neuter, Nicolas</au><au>Mobashar Hussain Urf Turabe, Fazil</au><au>Kumar Verma, Navin</au><au>Bogaerts, Annemie</au><au>Laukens, Kris</au><au>Offner, Fritz</au><au>Van Vlierberghe, Pieter</au><au>Van Ostade, Xaveer</au><au>Berghe, Wim Vanden</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells</atitle><date>2021</date><risdate>2021</risdate><issn>2072-6694</issn><eissn>2072-6694</eissn><abstract>Simple Summary Glucocorticoid therapy resistance in B-cell malignancies is often associated with constitutive activation of tyrosine kinases. Novel anticancer drugs targeting hyperactivated tyrosine kinases, such as Bruton's tyrosine kinase (BTK), have, therefore, gained much interest over the past few decades and have already been approved for clinical use. In this study, we compared the therapeutic efficacy of the phytochemical kinase inhibitor withaferin A with the clinically approved BTK inhibitor ibrutinib to target hyperactivated tyrosine kinase signaling in glucocorticoid-resistant multiple myeloma cells. Our results demonstrate that withaferin A-induced cell death of glucocorticoid-resistant MM1R cells involves covalent cysteine targeting of multiple Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including BTK. Multiple myeloma (MM) is a hematological malignancy characterized by plasma cells' uncontrolled growth. The major barrier in treating MM is the occurrence of primary and acquired therapy resistance to anticancer drugs. Often, this therapy resistance is associated with constitutive hyperactivation of tyrosine kinase signaling. Novel covalent kinase inhibitors, such as the clinically approved BTK inhibitor ibrutinib (IBR) and the preclinical phytochemical withaferin A (WA), have, therefore, gained pharmaceutical interest. Remarkably, WA is more effective than IBR in killing BTK-overexpressing glucocorticoid (GC)-resistant MM1R cells. To further characterize the kinase inhibitor profiles of WA and IBR in GC-resistant MM cells, we applied phosphopeptidome- and transcriptome-specific tyrosine kinome profiling. In contrast to IBR, WA was found to reverse BTK overexpression in GC-resistant MM1R cells. Furthermore, WA-induced cell death involves covalent cysteine targeting of Hinge-6 domain type tyrosine kinases of the kinase cysteinome classification, including inhibition of the hyperactivated BTK. Covalent interaction between WA and BTK could further be confirmed by biotin-based affinity purification and confocal microscopy. Similarly, molecular modeling suggests WA preferably targets conserved cysteines in the Hinge-6 region of the kinase cysteinome classification, favoring inhibition of multiple B-cell receptors (BCR) family kinases. Altogether, we show that WA's promiscuous inhibition of multiple BTK family tyrosine kinases represents a highly effective strategy to overcome GC-therapy resistance in MM.</abstract><oa>free_for_read</oa></addata></record> |
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| source | MDPI - Multidisciplinary Digital Publishing Institute; Ghent University Academic Bibliography; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; PubMed Central; PubMed Central Open Access |
| subjects | Biology and Life Sciences BTK glucocorticoids ibrutinib Medicine and Health Sciences multiple myeloma therapy resistance withaferin A |
| title | Covalent cysteine targeting of Bruton's tyrosine kinase (BTK) family by withaferin-A reduces survival of glucocorticoid-resistant multiple myeloma MM1 cells |
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