Agnieszka Potęga - Dane badawcze - MOST Wiedzy

dr inż. Agnieszka Potęga

Zatrudnienie

Adiunkt w Katedra Technologii Leków i Biochemii

Obszary badawcze

Non-enzymatic glutathione-mediated conjugation of unsymmetrical bisacridine C-2028 with anticancer activity
Dane Badawcze
- A. Potęga
- D. Rafalska
- E. Paluszkiewicz
- K. Kozłowska-Tylingo
The presented data complement the studies on the interplay between C-2028 (anticancer-active unsymmetrical bisacridine) and the glutathione S-transferase/glutathione (GST/GSH) system.
Glutathione conjugation of the antitumor-active 1-nitroacridine derivatives compounds C-857 and C-1748 – the major role of glutathione S-transferase M1-1
Dane Badawcze
- A. Potęga
- A. Mierzejewska
- J. Pasztelan
Objectives: C-857 and C-1748 are antitumor-active agents, monomers of unsymmetrical bisacridine derivatives. The aim of this study was to analyze their glutathione (GSH) conjugation in vitro in the presence of glutathione S-transferase (GST) M1-1.
Involvement of human glutathione S-transferase M1-1 in the glutathione conjugation of the antitumor unsymmetrical bisacridine derivative C-2028.
Dane Badawcze
- A. Potęga
- A. Mierzejewska
- J. Pasztelan
- K. Kozłowska-Tylingo
Unsymmetrical bisacridines (UAs) are a novel potent class of antitumor-active therapeutics. The aim of this study was to investigate the possible role of human glutathione S-transferase M1-1 (hGSTM1-1) in the glutathione (GSH) conjugation of a representative UA, C‑2028.

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