Peptide Database

Peptide NameSAMP H1

Function Ontology

Anticancer

Antimicrobial

Antimicrobial ▸ Antibacterial

Antimicrobial ▸ Antibacterial ▸ Anti-Gram-negative

Antimicrobial ▸ Antibacterial ▸ Anti-Gram-positive

Standard StatusStandard

Sequence Length30 amino acids

Chemical FormulaC126H217N37O34

DescriptionStandard

        AEVAPAPAAAAPAKAPKKKAAAKPKKAGPS
    

Molecular Weight2794.30 Da

Isoelectric Point (pI)10.40

Net Charge (pH 7.0)5.79

Net Charge (pH 7.4) 5.59

Charge Density (pH 7.0) 0.1931

GRAVY Index-0.47

Hydrophobic Moment 0.44

Boman Index-0.04

Instability Index58.51

Aliphatic Index 53.00

Aromaticity 0.0000

Extinction Coeff. Reduced 0.00

Extinction Coeff. Oxidized 0.00

The radar chart summarizes major physicochemical dimensions for quick comparison, while exact numerical values remain listed on the left.

Amino Acid Composition

TPSA 1094.15

LogP -12.20

H-bond Donors 34.0

H-bond Acceptors 40.0

Rotatable Bonds 86.0

Heavy Atoms 197.0

Ring Count 6.0

Amide Bonds 29.0

3D PDB MODEL

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2D CHEMICAL STRUCTURE

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RECORD: Rec_0118505 VERIFIED: YES

Provenance & Taxonomy

OrganismSalmo salar [Animal]

Structure & Mods

Configlinear peptide [Linear]

Chiralitynoncanonical stereochemical modification [Modified]

N-TermAcetylation

Other Modsderived from the N-terminal region of histone H1. Purified chromatographically. A 26-mer was initially found in 2001 (Patrzykat et al., 2001) but was inactive probably due to a lack of proline isomerase actiion (see activity section). Chemical modification: N-terminal acetylation (XXE)

Bio-Activity Profile

Function

Antimicrobial

TargetBacillus subtilis

Activity2 μM

MethodMIC

RECORD: Rec_0124349 VERIFIED: YES

Provenance & Taxonomy

OrganismSalmo salar [Animal]

Structure & Mods

Configtopology not specified [Not included yet]

Chiralitystereochemistry not specified [Other]

Bio-Activity Profile

Function

Antimicrobial Antibacterial Anti-Gram-positive Anti-Gram-negative

TargetBacillus subtilis

Activity2 μM

MethodMIC

RECORD: Rec_0164448 VERIFIED: YES

Provenance & Taxonomy

OrganismSalmo salar [Animal]

Structure & Mods

Configtopology not specified [Not included yet]

Chiralitystereochemistry not specified [Other]

Bio-Activity Profile

Function

Antimicrobial Antibacterial Anti-Gram-positive Anti-Gram-negative

TargetEscherichia coli

Activity2 μM

MethodMIC

RECORD: Rec_0170282 VERIFIED: YES

Provenance & Taxonomy

OrganismSalmo salar [Animal]

Structure & Mods

Configlinear peptide [Linear]

Chiralitynoncanonical stereochemical modification [Modified]

N-TermAcetylation

Other Modsderived from the N-terminal region of histone H1. Purified chromatographically. A 26-mer was initially found in 2001 (Patrzykat et al., 2001) but was inactive probably due to a lack of proline isomerase actiion (see activity section). Chemical modification: N-terminal acetylation (XXE)

Bio-Activity Profile

Function

Antimicrobial

TargetEscherichia coli

Activity2 μM

MethodMIC

RECORD: Rec_0187930 VERIFIED: YES

Provenance & Taxonomy

OrganismSalmo salar [Animal]

Structure & Mods

Configlinear peptide [Linear]

Chiralitynoncanonical stereochemical modification [Modified]

N-TermAcetylation

Other Modsderived from the N-terminal region of histone H1. Purified chromatographically. A 26-mer was initially found in 2001 (Patrzykat et al., 2001) but was inactive probably due to a lack of proline isomerase actiion (see activity section). Chemical modification: N-terminal acetylation (XXE)

Bio-Activity Profile

Function

Antimicrobial

TargetL. ivanovii

Activity4 μM

MethodMIC

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