Development Of Second Generation Thiol Isomerase Inhibitors To Prevent Thrombus Formation

Kennedy, Daniel R.; Nag, Partha P.; Galinski, Christian; Bowley, Sheryl R.; Bekendam, Roelof H.; Dilks, James R.; Scalise, Alissa A.; Hessem, Lotte van; Pu, Jun; Pilyugina, Tatiana; Dandapani, Sivaraman; Muñoz, Benito; Flaumenhaft, Robert

doi:10.1182/blood.v122.21.926.926

Cited by 3 publications

(2 citation statements)

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“…The precise mechanisms of this action conferred by ADTM would be another interesting question that is worth investigating in the future. Recently there are accumulating reports that the inhibition of protein disulfide isomerases including PDI and ERp57 could block thrombus formation in various in vivo models and suggest that this protein family represents an important novel class of anti-thrombotic target 39 40 41 42 43 . Preclinical studies demonstrate that deficiency in platelet ERp57 resulted in the increased tail bleeding times and delayed thrombus formation 20 , while PDI is unable to compensate for the absence of platelet ERp57 20 and other study also showed that the blockade of ERp57 with specific antibody further inhibited platelet aggregation in PDI deficient platelets 16 .…”

Section: Discussionmentioning

confidence: 99%

Novel anti-thrombotic agent for modulation of protein disulfide isomerase family member ERp57 for prophylactic therapy

Cui

Shan

Guo

et al. 2015

Sci Rep

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Protein disulfide isomerase (PDI) family members including PDI and ERp57 emerge as novel targets for anti-thrombotic treatments, but chemical agents with selectivity remain to be explored. We previously reported a novel derivative of danshensu (DSS), known as ADTM, displayed strong cardioprotective effects against oxidative stress-induced cellular injury in vitro and acute myocardial infarct in vivo. Herein, using chemical proteomics approach, we identified ERp57 as a major target of ADTM. ADTM displayed potent inhibitory effects on the redox activity of ERp57, inhibited the adenosine diphosphate (ADP)-induced expressions of P-selectin and αIIbβ3 integrin, and disrupted the interaction between ERp57 and αIIbβ3. In addition, ADTM inhibited both arachidonic acid (AA)-induced and ADP-induced platelet aggregation in vitro. Furthermore, ADTM significantly inhibited rat platelet aggregation and thrombus formation in vivo. Taken together, ADTM represents a promising candidate for anti-thrombotic therapy targeting ERp57.

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Section: Discussionmentioning

confidence: 99%

Novel anti-thrombotic agent for modulation of protein disulfide isomerase family member ERp57 for prophylactic therapy

Cui

Shan

Guo

et al. 2015

Sci Rep

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“…Inhibition of PDI can affect both platelet aggregation and fibrin generation. Moreover, it is a safe target for the inhibition of thrombus formation ( Flaumenhaft, 2013 ; Kennedy et al, 2013 ). Quercetin-3-rutinoside (rutin) is a kind of flavonoid glycoside, which is abundant in buckwheat, tea, fruits, and berries ( Gullon et al, 2017 ).…”

Section: Introductionmentioning

confidence: 99%

Rutin-Loaded Silver Nanoparticles With Antithrombotic Function

Jin

et al. 2020

Front. Bioeng. Biotechnol.

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In this paper, we fabricated rutin-loaded silver nanoparticles (Rutin@AgNPs) as the nano-anticoagulant with antithrombotic function. The serum stability, anticoagulation activity, and bleeding risk of Rutin@AgNPs were evaluated. The results showed Rutin@AgNPs had good serum stability, hemocompatibility, and cytocompatibility. The anticoagulation activity of rutin was maintained, and its stability and aqueous solubility were improved. The Rutin@AgNPs could provide a sustained release to prolong the half-life of rutin. The results of the coagulation parameter assay and thrombus formation test in mice model showed that the activated partial thromboplastin time and prothrombin time were prolonged, and Rutin@AgNPs inhibited the thrombosis in the 48 h period. Moreover, the limited bleeding time indicated that the Rutin@AgNPs significantly minimized the hemorrhage risk of rutin. This Rutin@AgNPs is a potential anticoagulant for antithrombotic therapy.

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Biocompatibility assessment of Rutin and PEG loaded novel nanoceria on human erythrocytes and human myeloid leukemia (U937) cells

Ganeshkar,

Gaddigal,

Shivappa

et al. 2023

Journal of Drug Delivery Science and Technology

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Development Of Second Generation Thiol Isomerase Inhibitors To Prevent Thrombus Formation

Cited by 3 publications

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Novel anti-thrombotic agent for modulation of protein disulfide isomerase family member ERp57 for prophylactic therapy

Novel anti-thrombotic agent for modulation of protein disulfide isomerase family member ERp57 for prophylactic therapy

Rutin-Loaded Silver Nanoparticles With Antithrombotic Function

Biocompatibility assessment of Rutin and PEG loaded novel nanoceria on human erythrocytes and human myeloid leukemia (U937) cells

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