An anticancer C-Kit kinase inhibitor is reengineered to make it more active and less cardiotoxic

Fernández, Ariel; Sanguino, Ángela; Peng, Zhenghong; Öztürk, Emel; Chen, Jianping; Crespo, Alejandro; Wulf, Sarah; Shavrin, Aleksander; Qin, Chaoping; Ma, Jianpeng; Trent, Jonathan C.; Lin, Yvonne G.; Han, Hee Dong; Mangala, Lingegowda S.; Bankson, James A.; Gelovani, Juri G.; Samarel, Allen M.; Bornmann, William G.; Sood, Anil K.; López-Berestein, Gabriel

doi:10.1172/jci32373

Cited by 148 publications

(159 citation statements)

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“…If it protects cardiomyocytes from oxidant stress, then its inhibition by imatinib explains its toxic effect. Recently, a modification to the molecule of imatinib to include an additional target, JNK, led to significant reduction of cardiotoxicity without any negative effect in the drug's potency [15]. This reengineered molecule, WBZ_4 is a methylated variant of imatinib.…”

Section: Imatinib Mesylatementioning

confidence: 99%

Cardiotoxicity induced by tyrosine kinase inhibitors

2009

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Section: Imatinib Mesylatementioning

confidence: 99%

Cardiotoxicity induced by tyrosine kinase inhibitors

2009

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“…Incidence of cardiotoxicity was cited as similar to onset of heart failure incidence in the general population, estimated at 0.2% per year, as evidenced by new-onset heart failure or left ventricular dysfunction [5]. While the impact of imatinib cardiotoxicity for GIST has been debated, molecular re-engineering of anticancer C-kit kinase inhibitors and cellular data on mitochondrial dysfunction and adenosine triphosphate (ATP) production deficit in murine models suggest a relationship, despite advocates for imatinib safety [11–14]. Prospective data on cardiac function and long-term follow-up data are needed to confirm murine observation in humans.…”

Section: Discussionmentioning

confidence: 99%

Rapidly progressive dyspnea in gastrointestinal stromal tumor (GIST) with imatinib cardiac toxicity

Ghias

Bhayani

Gemmel

et al. 2018

Journal of Community Hospital Internal Medicine Perspectives

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Gastrointestinal stromal tumors (GISTs) are rare and current estimates range from 4,000 to 6,000 number of GIST cases in the USA annually. Imatinib, a tyrosine kinase inhibitor, has shown a survival benefit in GISTs, and the presence of KIT mutation status is predictive of response. The current case discusses rapidly progressive dyspnea and heart failure in an elderly male with metastatic GIST who was started on imatinib. Although reported as a rare and sporadic side effect of imatinib, the current case illustrates rapidity and the clinical significance of cardiotoxicity, with onset at 2 weeks.Cases of imatinib-induced cardiotoxicity can range from being mild ventricular dysfunction to overt heart failure. Prior to starting imatinib, our patient had a history of hypertension. He subsequently ended up developing heart failure as acknowledged by the echocardiogram (ECHO). In general, elderly with preexisting cardiovascular comorbidity are at greater risk. The goal in such situations is immediate discontinuation or reduction of the imatinib dosage. The case prompts for awareness of imatinib cardiotoxicity. Moreover, a pretreatment cardiac assessment along with monitoring throughout therapy is therefore advisable. Also, imatinib-induced cardiotoxicity should be differentiated from imatinib-associated fluid retention, in which ECHO findings can be normal. This case report raises the concern for accelerated cardiotoxicity profile of imatinib. Further prospective studies with multidisciplinary input are needed to establish this association further.

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“…As noted in 2007 [4], labile hydration patterns in the target protein provide suitable "epistructural" (around the structure) blueprints. Thus, it has been shown that water becomes easily removable when found in the vicinity of certain packing defects in proteins known as dehydrons [1].…”

mentioning

confidence: 99%

“…Lead optimization has been increasingly influenced by the identification of labile water molecules at the interface with the target protein [4][5][6][7]. These molecules are expected to be displaced upon drug binding.…”

mentioning

confidence: 99%

“…The emerging design principle resulting from this simple observation was originally introduced in 2007 [4] in what constitutes a precursor to the WaterMap® software (Schrödinger, Inc.) [5,7]. Thus, the maps of "local de-wetting propensities" scanning the protein interface are regarded as epistructural blueprints for drug discovery [4,6], and in fact provide the guidance and inspiration to Water Map computations. The latter estimate the free energy cost associated with the transferring of water molecules from the protein interface to bulk solvent [7].…”

mentioning

confidence: 99%

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