Pseudomonas Exotoxin A Based Toxins Targeting Epidermal Growth Factor Receptor for the Treatment of Prostate Cancer

被引:16
作者
Fischer, Alexandra [1 ,2 ]
Wolf, Isis [1 ,2 ]
Fuchs, Hendrik [3 ,4 ,5 ,6 ]
Masilamani, Anie Priscilla [1 ,2 ]
Wolf, Philipp [1 ,2 ]
机构
[1] Univ Freiburg, Fac Med, D-79106 Freiburg, Germany
[2] Univ Freiburg, Dept Urol Antibody Based Diagnost & Therapies, Med Ctr, Breisacher Str 66, D-79106 Freiburg, Germany
[3] Charite Univ Med Berlin, Inst Lab Med Clin Chem & Pathobiochem, D-13353 Berlin, Germany
[4] Free Univ Berlin, D-13353 Berlin, Germany
[5] Humboldt Univ, D-13353 Berlin, Germany
[6] Berlin Inst Hlth, D-13353 Berlin, Germany
关键词
prostate cancer; targeted toxins; epidermal growth factor; epidermal growth factor receptor; Pseudomonas Exotoxin A; PHASE-II TRIAL; IN-VITRO; EGFR; IMMUNOTOXIN; EXPRESSION; CETUXIMAB; ANTIGEN; OVEREXPRESSION; IMMUNOGENICITY; PROGRESSION;
D O I
10.3390/toxins12120753
中图分类号
TS2 [食品工业];
学科分类号
0832 ;
摘要
The epidermal growth factor receptor (EGFR) was found to be a valuable target on prostate cancer (PCa) cells. However, EGFR inhibitors mostly failed in clinical studies with patients suffering from PCa. We therefore tested the targeted toxins EGF-PE40 and EGF-PE24mut consisting of the natural ligand EGF as binding domain and PE40, the natural toxin domain of Pseudomonas Exotoxin A, or PE24mut, the de-immunized variant thereof, as toxin domains. Both targeted toxins were expressed in the periplasm of E.coli and evoked an inhibition of protein biosynthesis in EGFR-expressing PCa cells. Concentration- and time-dependent killing of PCa cells was found with IC50 values after 48 and 72 h in the low nanomolar or picomolar range based on the induction of apoptosis. EGF-PE24mut was found to be about 11- to 120-fold less toxic than EGF-PE40. Both targeted toxins were more than 600 to 140,000-fold more cytotoxic than the EGFR inhibitor erlotinib. Due to their high and specific cytotoxicity, the EGF-based targeted toxins EGF-PE40 and EGF-PE24mut represent promising candidates for the future treatment of PCa.
引用
收藏
页数:13
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