Pharmaceutical compositions and methods for countering chemotherapy induced cardiotoxicity

a technology of chemotherapy and compositions, applied in the direction of drug compositions, enzyme inhibitor ingredients, antibody medical ingredients, etc., can solve the problems of high incidence of heart failure, cell death in both cancer and normal cells, severe limits of the therapeutic potential of these anticancer agents, etc., to reduce the risk of potentially devastating heart failure, prevent heart failure, and improve efficacy and safety

Inactive Publication Date: 2017-08-10
STEM CELL THERANOSTICS INC +1
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

[0038]This disclosure provides composition, kits, and methods for protecting the heart and for preventing heart failure in patients treated with anthracyclines, protein kinase inhibitors and / or biologic agents. By minimizing the risk of potentially devastating heart failure in cancer patient under chemotherapy, conventional cancer treatment can achieve improved efficacy and safety with the invention described herein.
[0039]The compositions include one or more protective agents with or without an anticancer agent. The kits often include one or more protective agents, and sometimes anticancer agents as well. The methods include methods of reducing, preventing, or eliminating cardiotoxicity induced by a drug or other therapy including cancer treatments.

Problems solved by technology

Certain reductions in heart failure rates have been achieved by capping the maximal doses of anthracyclines and by changing their administration schedules, all of which severely limits the therapeutic potentials of these anticancer agents.
A common side effect of anthracycline use is associated with cardiotoxicity, which is dose dependent and may also result from cumulative exposures.
The reactive oxygen species (ROS) may activate apoptotic pathways, leading to cell death in both cancer and normal cells.
Some protein kinase inhibitors-including small molecule and biologic inhibitors may also cause cardiotoxicity.
Several monoclonal antibodies target receptor protein kinases that play an important role in heart function and thus may cause cardiotoxicity as a result.
DEX is not approved for use in children and adolescents, it is particularly disheartening to find reports of high incidences of heart failure in anthracycline-treated young children in their later life of post-cancer.
Further, the limited indication approval and use are also testament of DEX's shortcomings, which include interfering with antitumor efficacy of anthracyclines, inducing secondary malignancies, and causing blood and bone marrow disorders.

Method used

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  • Pharmaceutical compositions and methods for countering chemotherapy induced cardiotoxicity
  • Pharmaceutical compositions and methods for countering chemotherapy induced cardiotoxicity
  • Pharmaceutical compositions and methods for countering chemotherapy induced cardiotoxicity

Examples

Experimental program
Comparison scheme
Effect test

example 1

Provides Long-Term Cardioprotection (Cell Viability)

[0220]Cell samples were prepared by differentiating induced pluripotent stem cells into cardiomyocytes. Cells were cultured for 4 days post-differentiation, changing media at day 3, before performing experiments. Samples were either mock-treated, treated with 1.25 μM doxorubicin, treated with myricetin, or co-treated with 1.25 μM of doxorubicin and myricetin for 72 hours. Following treatment, the samples were incubated Hoeschst 33342 to indicate cell nuclei. Cells were imaged using the INCell Analyzer2200, and images were analyzed to quantify the total number of cells and plotted as a percentage of total cells normalized to control (left), where each data point was obtained from three biological replicates. Representative images (FIG. 3, right) are presented for each sample, where an increase in Hoechst 33342 signal represents an increase ion cell viability.

[0221]Cardiomyocytes were either mock-treated, treated with 1.25 μM doxorub...

example 2

f Myricetin on Doxorubicin-Induced Cardiotoxicity 2 Days Following Treatment (Mitochondrial Toxicity)

[0222]Human iPSC-derived cardiomyocytes were prepared by differentiating induced pluripotent stem cells into cardiomyocytes. Cells were cultured for 4 days post-differentiation, changing media at day 3, before performing experiments. Cardiomyocytes were treated with 1.25 μM doxorubicin (FIG. 4A), or co-treated with 1.25 μM of doxorubicin and 79 μM myricetin (FIG. 4B) for 2 days. Following treatment, the samples were incubated with a tetramethylrhodamine methyl ester (TMRM) dye to indicate mitochondrial health, and Hoechst 33342 to identify cell nuclei. Cells were imaged using the INCell Analyzer2200. Representative images are presented for each sample, wherein a decrease in TMRM signal indicates an increase in mitochondrial toxicity. Myricetin was a potent protector against doxorubicin-induced mitochondrial toxicity, as indicated by a greater TMRM signal in cells co-treated with 1.25...

example 3

f Myricetin on Doxorubicin-Induced Cardiotoxicity 3 Days Following Treatment (Contractility)

[0223]Human iPSC-derived cardiomyocytes were prepared as described above. Samples were either mock-treated, treated with 1.25 μM doxorubicin, treated with 79 μM myricetin, or co-treated with 1.25 μM of doxorubicin and 79 μM myricetin for 72 hours. Following treatment, videos of beating cardiomyocytes were captured using Pulse, and analyzed to quantify beat rate (FIG. 5; left) from plots of cell contraction, where each data point was obtained from three biological replicates. Representative plots of cell contraction (FIG. 5; right) are presented for each sample. Myricetin was a potent protector of cell contractility. Mock-treated cardiomyocytes contracted at 33.33 beats per minute, whereas treatment with 1.25 μM doxorubicin, in the absence of myricetin, completely inhibited contraction. Cardiomyocytes treated with myricetin, or co-treated with myricetin and 1.25 μM doxorubicin, contracted at 3...

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Abstract

This disclosure provides methods and pharmaceutical compositions for reducing or eliminating cardiotoxicity, particularly cardiotoxicity induced by a cancer treatment or other therapy. In some cases, the methods and compositions prevent or reduce cardiotoxicity caused by anthracycline treatment. The methods provided herein often comprise administering a protective agent such as myricetin, tricetin, robinetin, ficetin, vitexin, quercetin, dihydrorobinetin, kaempferol, 7,3′,4′,5′-tetrahydroxyflavone, and myricitrin in conjunction with the administration of a cancer drug or other treatment. They may comprise administering a protective agent in combination with dexrazoxane. The compositions provided herein include co-formulations of a protective agent with a different protective agent or with a cancer treatment (e.g., anthracycline drug).

Description

CROSS-REFERENCE TO RELATED APPLICATIONS[0001]This application claims the priority of U.S. provisional application Ser. No. 62 / 291,480, filed Feb. 4, 2016, and U.S. provisional application Ser. No. 62 / 348,102, filed Jun. 9, 2016, each of which is hereby incorporated by reference herein in its entirety for all purposes.BACKGROUND[0002]Cardiotoxicity and congestive heart failure are serious side-effects of oncological therapies, most prominently those comprising anthracyclines, which are administered to greater than one million cancer patients per year and half of all childhood cancer patients. Adverse cardiac side effects are also observed in patients treated with protein kinase inhibitors and antibody-based biologics that target protein kinase. Certain reductions in heart failure rates have been achieved by capping the maximal doses of anthracyclines and by changing their administration schedules, all of which severely limits the therapeutic potentials of these anticancer agents. The...

Claims

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Application Information

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Patent Type & Authority Applications(United States)
IPC IPC(8): A61K31/352A61K31/704A61K38/05A61K9/00A61K31/404A61K39/395C07K16/32A61K31/496A61K9/20A61K31/4412
CPCA61K31/352A61K9/20A61K31/704A61K38/05A61K31/4412C07K2317/24A61K39/3955C07K16/32A61K31/496A61K9/0053A61K9/0019A61K31/404A61K9/127A61K9/48A61K31/136A61K31/353A61K31/4439A61K31/4545A61K31/47A61K31/506A61K31/517A61K31/7048A61P9/00A61P35/00A61K31/44A61K38/005A61K2300/00A61K39/395A61K45/06
Inventor ARMSTRONG, CHRISTOPHER G.KIM, KEVIN J.PHAM, LISA MARIA LUCIAPARK, EUNHYEZHONG, ZHONGHUANG, GUANYIWU, JOSEPH C.ELMER, SIDNEY PAULVISUTHIKRAISEE, VIWATCADAG, EITHON MICHAEL GFREEMAN, THOMAS BERNARDLUM, PEK YEE
Owner STEM CELL THERANOSTICS INC
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