dbACP: A Comprehensive Database of Anti-Cancer Peptides

dbacp04853

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General Description

Peptide name : NK-11

Source/Organism : NK2 derived iNot foundctive control peptide

Linear/Cyclic : Linear

Chirality : L

Sequence Information

Sequence : KISKRILTGKK

Peptide length: 11

C-terminal modification: Linear

N-terminal modification : Amidation

Non-natural peptide information: None

Activity Information

Assay type : MTT/MTS assay

Assay time : 2h

Activity : IC50 : > 100 µM

Cell line : E42/02

Cancer type : Skin cancer

Other activity : Hemolytic activity

Physicochemical Properties

Amino acid composition bar chart :

Molecular mass : 1271.5955 Dalton

Aliphatic index : 1.063

Instability index : 33.0818

Hydrophobicity (GRAVY) : -0.836

Isoelectric point : 11.333

Charge (pH 7) : 4.7561

Aromaticity : 0

Molar extinction coefficient (cysteine, cystine): (0, 0)

Hydrophobic/hydrophilic ratio : 0.57142857

hydrophobic moment : -1.107

Missing amino acid : C,W,H,Q,P,M,E,F,D,Y,N,A,V

Most occurring amino acid : K

Most occurring amino acid frequency : 4

Least occurring amino acid : S

Least occurring amino acid frequency : 1

Structural Information

3D structure :

Secondary structure fraction (Helix, Turn, Sheet): (0.4, 0.1, 0.3)

SMILES Notation: CC[C@H](C)[C@H](NC(=O)[C@H](CCCNC(=N)N)NC(=O)[C@H](CCCCN)NC(=O)[C@H](CO)NC(=O)[C@@H](NC(=O)[C@@H](N)CCCCN)[C@@H](C)CC)C(=O)N[C@@H](CC(C)C)C(=O)N[C@H](C(=O)NCC(=O)N[C@@H](CCCCN)C(=O)N[C@@H](CCCCN)C(=O)O)[C@@H](C)O

Secondary Structure :

Method Prediction
GOR HHHHHHHHTCC
Chou-Fasman (CF) CEECEEECCCC
Neural Network (NN) CCCHHHHCCCC
Joint/Consensus CCCHHHHCCCC

Molecular Descriptors and ADMET Properties

Molecular Descriptors: Click here to download

ADMET Properties: Click here to download

Cross Referencing databases

Pubmed Id : 23893605

Uniprot : Not available

PDB : Not available

CancerPPD : Click here

ApIAPDB : Not available

CancerPPD2 ID : Not available

Reference

1 : Gross S, et al. Design of NK-2-derived peptides with improved activity against equine sarcoid cells. J Pept Sci. 2013; 19:619-28. doi: 10.1002/psc.2540

Literature

Paper title : Design of NK-2-derived peptides with improved activity against equine sarcoid cells.

Doi : https://doi.org/10.1002/psc.2540

Abstract : Equine sarcoid is a topically accessible model for the evaluation of anticancer peptides acting by physical membrane disruption avoiding the complexity of a systemic application. We aim at evaluating and improving natural peptides for host defence as lead structures, where we focus on the cationic and amphipathic peptide NK-2. Cytotoxicity tests, fluorescence microscopy and a chip-based biosensor, which enabled real-time monitoring of cell metabolism, were applied. Cancer cell killing was dynamic with an initial phase of increased cellular respiration, followed by membrane destruction. NK-2 was substantially improved and shortened. Novel peptides exhibited a fivefold improved activity against sarcoid cells, while haemolysis remained almost unaltered. Similar Zeta potential and similar amount of surface phosphatidylserine of sarcoid and normal skin cells are responsible for a lack of selectivity between these two cell types.