Author(s): Beller U, Quinn MA, Benedet JL, Creasman WT, Ngan HY
Anthracyclines are important for the treatment of gynecological malignancies, but their effects are modest, and one of the major reasons is the lack of a tumor-targeting property. To overcome this drawback, a poly (hydroxypropyl meta-acrylamide) conjugated with tetrahydropyraryl doxorubicin (P-THP) has been developed, which exhibits a highly tumor-specific accumulation owing to the enhanced permeability and retention effect. The effect of P-THP has been confirmed by using various cell lines and solid tumor models, while its effect on gynecological malignancies have not been investigated. In this regard, human uterine sarcoma cell line with metastatic potential MEA-SA C9 high, epithelial ovarian cancer cell line A2780 and its cisplatin-resistant line A2780cis, and DOX-resistant line A2780ADR were used in this study, and the therapeutic effect as well as the safety profiles of P-THP were investigated compared to native THP, cisplatin, and paclitaxel, which are commonly used for gynecological malignancies, both in vitro and in vivo. Similar to native THP, a dose-dependent toxicity of P-THP was identified in all cell lines. Moreover, the IC50 values in the 3 h following P-THP were 1.5-10 times higher than those at 72 h, though the intracellular uptake of P-THP in all cells were 2-10-fold less than THP. In vivo studies using xenograft tumor models revealed that P-THP significantly suppressed the MES-SA C9 high, A2780, and A2780cis tumor growth at the dose of 15 mg/kg (THP equivalent), which is three times above the maximal tolerance dose of native THP, while no body weight loss or acute death occurred. However, in A2780ADR cells and the xenograft model, no significant difference in the therapeutic effect was observed between THP and P-THP, suggesting that P-THP exhibits its effect depending on the release of the active free THP in tumor tissues, and thus the internalization into tumor cells. These findings indicates that P-THP has the potential as a therapeutic for gynecological malignancies to improve the therapeutic outcomes and survival rates of patients, even in refractory patients.
Referred From: https://pubmed.ncbi.nlm.nih.gov/35629236/
Author(s): Judson PL, Habermann EB, Baxter NN, Durham SB, Virnig BA
Author(s): Hampl M, Deckers-Figiel S, Hampl JA, Rein D, Bender HG
Author(s): Jones RW, Baranyai J, Stables S
Author(s): Taussig FJ
Author(s): Falconer AD, Hirschowitz L, Weeks J, Murdoch J; South West Gynaecology Tumour Panel
Author(s): Rhodes CA, Cummins C, Shafi MI
Author(s): Levenback C, Morris M, Burke TW, Gershenson DM, Wolf JK, et al.
Author(s): Micheletti L, Preti M, Zola P, Zanotto Valentino MC, Bocci C, et al.
Author(s): [No authors listed]
Author(s): Benedet JL, Bender H, Jones H 3rd, Ngan HY, Pecorelli S
Author(s): Rutledge F, Smith JP, Franklin EW
Author(s): Boutselis JG
Author(s): Japaze H, Garcia-Bunuel R, Woodruff JD
Author(s): Benedet JL, Turko M, Fairey RN, Boyes DA
Author(s): Cavanagh D, Shepherd JH
Author(s): Cavanagh D, Roberts WS, Bryson SC, Marsden DE, Ingram JM, et al.
Author(s): Hacker NF, Berek JS, Lagasse LD, Leuchter RS, Moore JG
Author(s): Homesley HD, Bundy BN, Sedlis A, Yordan E, Berek JS
Author(s): Rodolakis A, Diakomanolis E, Voulgaris Z, Akrivos T, Vlachos G, et al.
Author(s): Raspagliesi F, Hanozet F, Ditto A, Solima E, Zanaboni F, et al.
Author(s): Chan JK, Sugiyama V, Pham H, Gu M, Rutgers J, et al.
Author(s): Dhar KK, Woolas RP
Author(s): Saito T, Kato K
Author(s): Marsden DE, Hacker NF
Author(s): Hoffman JS, Kumar NB, Morley GW
Author(s): Hacker NF, Berek JS, Lagasse LD, Nieberg RK, Leuchter RS
Author(s): Monaghan JM, Hammond IG
Author(s): Lingard D, Free K, Wright RG, Battistutta D et al.
Author(s): Atamdede F, Hoogerland D
Author(s): Van Der Velden J, Kooyman CD, Van Lindert AC, Heintz A
Author(s): Rhodes CA, Cummins C, Shafi MI
Author(s): Reuben DB, Mor V, Hiris J
Author(s): Barnes EA, Thomas G
Author(s): Barbera L, Thomas G, Elit L, Covens A, Fyles A, et al.
