2020
DOI: 10.1016/j.bbamem.2020.183264
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Design of human lactoferricin derived antitumor peptides-activity and specificity against malignant melanoma in 2D and 3D model studies

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Cited by 8 publications
(27 citation statements)
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“…Furthermore, the 10 amino acids at the N-terminal end of cecropin can be used and repeated three times to create the CB1 peptide [ 85 ]. Grissenberger et al (2020) obtained anticancer peptide fractions from lactoferrin residues 21 to31, including retro dipeptides DIM-LF11-322 and R-DIM-PLF11-215 characterized by a net charge of +9 and a potent activity and selectivity against cancer cells [ 94 ].…”
Section: Sequence Template Methods Of Rational Design Of Anticancementioning
confidence: 99%
“…Furthermore, the 10 amino acids at the N-terminal end of cecropin can be used and repeated three times to create the CB1 peptide [ 85 ]. Grissenberger et al (2020) obtained anticancer peptide fractions from lactoferrin residues 21 to31, including retro dipeptides DIM-LF11-322 and R-DIM-PLF11-215 characterized by a net charge of +9 and a potent activity and selectivity against cancer cells [ 94 ].…”
Section: Sequence Template Methods Of Rational Design Of Anticancementioning
confidence: 99%
“…Cationic antitumor peptides derived from the human host defense peptide Lactoferricin [22] studied in our lab (PCT/EP2014/050330; US 14/760,445; EP 14700349.5) have been shown to selectively kill cancer cells of different types, including malignant melanoma and their metastases [23][24][25][26] and glioblastoma [24] in 2D and 3D [26] in vitro and in vivo [25] by targeting the negatively charged lipid phosphatidylserine (PS), specifically exposed by cell membranes of cancer cells [27,28]. Cell death appeared by peptide-induced apoptosis [24], a process normally blocked, e.g., in melanoma by inhibition of Apaf-1 [29].…”
Section: Introductionmentioning
confidence: 99%
“…Cell death appeared by peptide-induced apoptosis [24], a process normally blocked, e.g., in melanoma by inhibition of Apaf-1 [29]. Several highly active and specific peptide derivatives with about 5-to 25-fold specificity for melanoma over normal dermal fibroblasts or melanocytes were designed with a similar pattern of a secondary structure comprising a mostly proline induced loop in the middle of the peptide flanked by two helices or two β-strands and a net charge of +9 and above [24,26].…”
Section: Introductionmentioning
confidence: 99%
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