Synthesis and antiproliferative activities of doxorubicin thiol conjugates and doxorubicin-SS-cyclic peptide

Shaban Darwish; Neda Sadeghiani; Shirley Fong; Saghar Mozaffari; Parinaz Hamidi; Thimanthi Withana; Sun Yang; Rakesh Kumar Tiwari; Keykavous Parang

doi:10.1016/j.ejmech.2018.10.042

Synthesis and antiproliferative activities of doxorubicin thiol conjugates and doxorubicin-SS-cyclic peptide

Eur J Med Chem. 2019 Jan 1:161:594-606. doi: 10.1016/j.ejmech.2018.10.042. Epub 2018 Oct 23.

Authors

Shaban Darwish¹, Neda Sadeghiani², Shirley Fong², Saghar Mozaffari², Parinaz Hamidi², Thimanthi Withana³, Sun Yang³, Rakesh Kumar Tiwari⁴, Keykavous Parang⁵

Affiliations

¹ Center for Targeted Drug Delivery, Department of Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, Irvine, CA, 92618, United States; Organometallic and Organometalloid Chemistry Department, National Research Centre, El Bohouth st, Dokki, Giza, Egypt.
² Center for Targeted Drug Delivery, Department of Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, Irvine, CA, 92618, United States.
³ Department of Pharmacy Practice, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, Irvine, CA, 92618, United States.
⁴ Center for Targeted Drug Delivery, Department of Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, Irvine, CA, 92618, United States. Electronic address: tiwari@chapman.edu.
⁵ Center for Targeted Drug Delivery, Department of Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, Irvine, CA, 92618, United States. Electronic address: parang@chapman.edu.

Abstract

Myocardial toxicity and drug resistance caused by drug efflux are major limitations of doxorubicin (Dox)-based chemotherapy. Dox structure modification could be used to develop conjugates with an improved biological profile, such as antiproliferative activity and higher cellular retention. Thus, Dox thiol conjugates, Dox thiol (Dox-SH), thiol-reactive Dox-SS-pyridine (SS = disulfide), and a Dox-SS-cell-penetrating cyclic peptide, Dox-SS-[C(WR)₄K], were synthesized. Dox was reacted with Traut's reagent to generate Dox-SH. The thiol group was activated by the reaction with dithiodipyridine to afford the corresponding Dox-SS-Pyridine (Dox-SS-Pyr). A cyclic cell-penetrating peptide containing a cysteine residue [C(WR)₄K] was prepared using Fmoc solid-phase strategy. Dox-SS-Py was reacted with the free sulfhydryl of cysteine in [C(WR)₄K] to generate Dox-SS-[C(WR)₄K] as a Dox-cyclic peptide conjugate. Cytotoxicity of the compounds was examined in human embryonic kidney (HEK-293), human ovarian cancer (SKOV-3), human fibrosarcoma (HT-1080), and human leukemia (CCRF-CEM) cells. Dox-SH and Dox-SS-pyridine were found to have significantly higher or comparable cytotoxicity when compared to Dox in HEK-293, HT-1080, and CCRF-CEM cells after 24 h and 72 incubation, presumably because of higher activity and retention of the compounds in these cells. Furthermore, Dox-SS-[C(WR)₄K] showed significantly higher cytotoxic activity in HEK-293, HT-1080, and SKOV-3 cells when compared with Dox after 72 h incubation. Dox-SS-Pyr exhibited higher cellular uptake than Dox-SS-[C(WR)₄K] in HT-1080 and HEK-293 cells as shown by flow cytometry. Fluorescence microscopy exhibited that Dox-SS-Pyr, Dox-SH, and Dox-SS-[C(WR)₄K] localized in the nucleus as shown in four cell lines, HT-1080, SKOV-3, MDA-MB-468, and MCF-7. Of note, Dox-SS-[C(WR)₄K] was significantly less toxic in mouse myoblast cells compared to Dox at the same concentration. Further mechanistic study demonstrated that the level of intracellular reactive oxygen species (ROS) in myoblast cells exposed to Dox-SS-[C(WR)₄K] was reduced in comparison of Dox when co-treated with FeCl₂. These data indicate that Dox-SH, Dox-SS-Pyr, and Dox-SS-[C(WR)₄K] have the potential to be further examined as Dox alternatives and anticancer agents.

Keywords: Anticancer; Cardiotoxicity; Cellular uptake; Cyclic peptide; Disulfide; Doxorubicin; Thiol.

MeSH terms

Animals
Antineoplastic Agents / chemical synthesis
Antineoplastic Agents / chemistry
Antineoplastic Agents / pharmacology*
Cell Proliferation / drug effects
Cell Survival / drug effects
Cells, Cultured
Disulfides / chemistry
Disulfides / pharmacology*
Dose-Response Relationship, Drug
Doxorubicin / chemistry
Doxorubicin / pharmacology*
Drug Screening Assays, Antitumor
Flow Cytometry
HEK293 Cells
Humans
Mice
Molecular Conformation
Peptides, Cyclic / chemistry
Peptides, Cyclic / pharmacology*
Reactive Oxygen Species / analysis
Reactive Oxygen Species / metabolism
Structure-Activity Relationship
Sulfhydryl Compounds / chemistry
Sulfhydryl Compounds / pharmacology*

Substances

Antineoplastic Agents
Disulfides
Peptides, Cyclic
Reactive Oxygen Species
Sulfhydryl Compounds
Doxorubicin

Grants and funding

K08 CA179084/CA/NCI NIH HHS/United States