Peptide properties

1Top 2Function-activity relationship 3Calculated physicochemical properties 4Peptide source & Food-borne protein(s) search 5Biological/Functional activity & target protein 6Taste properties & Structure 7Preparation method 8Stability & Cytotoxicity 9Additional information 10Database cross-references 11Reference(s)

List of peptide properties

DFBP ID - DFBPBBBP0002(Blood-brain barrier peptides)

DFBP ID	DFBPBBBP0002
Peptide sequence	CYFQNCPRG
Type	Native peptide
Peptide/Function name	Blood-brain barrier peptide, Vasopressin

Function-activity relationship

Main bioactivity	Penetrate blood-brain barrier
Otheir bioactivity	N.D

Calculated physicochemical properties

Three-letter amino acid

Cys-Tyr-Phe-Gln-Asn-Cys-Pro-Arg-Gly

Single-letter amino acid

CYFQNCPRG

Peptide length

Peptide mass

Experimental mass	Theoretical mass
N.D	1087.25 Da ^c

Net charge

0.00 ^c

Isoelectric point (pI)

8.25 ^c

IC₅₀

N.D

pIC₅₀

N.D

GRAVY

-0.7778^c

Hydrophilic residue ratio

33.33%^c

Peptide calculator

Peptide source & Food-borne protein(s) search

Classification	Animal
Organism/Source	Bovine hypothalamus
Precursor protein	N.D
Residue position	N.D
Precursor protein(s) search	Source.1: DFBPPR17506 ---- Animal proteins ---- Vasopressin-neurophysin 2-copeptin Source.2: DFBPPR13670 ---- Animal proteins ---- Vasopressin-neurophysin 2-copeptin
Link-research Inductive analysis	There are no literature reports on the discovery of this sequence in other food-source proteins.

Biological/Functional activity & target protein

Penetrate blood-barin barrier	The Nesfatin-1 is relatively stable in blood for the first 20 min after injection, and crosses the BBB by simple diffusion.
Specific target protein(s)	N.D

Taste properties & Structure

Bitterness

Literature report	N.D
Bitter prediction tools	Non-bitter taste ^prediction

SMILES

N.D

Preparation method

Mode of preparation	Separation
Enzyme(s)/starter culture	Nesfatin-1 is a peptide corresponding to amino acids 1–82 of the larger protein nucleobindin-2 (NUCB2, or DNA binding/EF-hand/acidic protein NEFA) that shows reduced expression in the paraventricular nucleus of the hypothalamus after fasting, and acts through melanocortin signaling to exert satiety effects in rats ^[1].

Stability & Cytotoxicity

Peptide stability

Literature report:	N.D
EHP-Tool:	Enzymatic Hydrolysis Prediction Tool (EHP-Tool)

Peptide cytotoxicity

Literature report:	N.D
Prediction:	ToxinPred

Additional information

The limited penetration under physiological conditions does not limit the pharmacological delivery of this satiety peptide (Nesfatin-1) as a potential therapeutic agent.

Database cross-references

[D1]

[D2]

[D3]

[D4]

Reference(s)

Primary literature	Pan W, Hsuchou H, Kastin AJ. Nesfatin-1 crosses the blood-brain barrier without saturation. Peptides. 2007 Nov;28(11):2223-8. PMID: 17950952 DOI: 10.1016/j.peptides.2007.09.005
Other literature(s)	[1] Oh-I S, Shimizu H, Satoh T, Okada S, Adachi S, Inoue K, Eguchi H, Yamamoto M, Imaki T, Hashimoto K, Tsuchiya T, Monden T, Horiguchi K, Yamada M, Mori M. Identification of nesfatin-1 as a satiety molecule in the hypothalamus. Nature. 2006 Oct 12;443(7112):709-12. doi: 10.1038/nature05162. Epub 2006 Oct 1. PMID: 17036007.
PubDate	2007