ISDA: 2JP8

Deposition Date 2007-04-27

Release Date 2007-10-30

Last Version Date 2023-12-20

Entry Detail

PDB ID:

2JP8

Keywords:

SIGNALING PROTEIN

Title:

Angiotensin 1-7

Method Details:

Experimental Method:

SOLUTION NMR

Conformers Calculated:

100

Conformers Submitted:

Selection Criteria:

structures with the lowest energy

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Macromolecular Entities

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:Angiotensin-(1-7)
Gene (Uniprot):AGT
Chain IDs:A (auth: P)
Chain Length:7
Number of Molecules:1
Biological Source:

UniProt ID:P01019

Ligand Molecules

Primary Citation

Study of angiotensin-(1-7) vasoactive peptide and its beta-cyclodextrin inclusion complexes: complete sequence-specific NMR assignments and structural studies

Lula, I, Denadai, A.L, Resende, J.M, de Sousa, F.B, de Lima, G.F, Pilo-Veloso, D, Heine, T, Duarte, H.A, Santos, R.A, Sinisterra, R.D.Show

Peptides 28 2199 2210 (2007)

PMID: 17904691 DOI: 10.1016/j.peptides.2007.08.011

Abstact

We report the complete sequence-specific hydrogen NMR assignments of vasoactive peptide angiotensin-(1-7) (Ang-(1-7)). Assignments of the majority of the resonances were accomplished by COSY, TOCSY, and ROESY peak coordinates at 400MHz and 600MHz. Long-side-chain amino acid spin system identification was facilitated by long-range coherence transfer experiments (TOCSY). Problems with overlapped resonance signals were solved by analysis of heteronuclear 2D experiments (HSQC and HMBC). Nuclear Overhauser effects (NOE) results were used to probe peptide conformation. We show that the inclusion of the angiotensin-(1-7) tyrosine residue is favored in inclusion complexes with beta-cyclodextrin. QM/MM simulations at the DFTB/UFF level confirm the experimental NMR findings and provide detailed structural information on these compounds in aqueous solution.

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Primary Citation of related structures

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