PAK: An essential motif for forming β-turn structures and exhibiting the thrombolytic effect of P6A and its analogs

Ming Zhao; Xin Jia; Chao Wang; Qin Li; Kexiang Zhou; Lili Wang; Hu Liu; Shiqi Peng

doi:10.1139/O07-143

PAK: An essential motif for forming β-turn structures and exhibiting the thrombolytic effect of P6A and its analogs

Ming Zhao
, Xin Jia
, Chao Wang
, Qin Li
, Kexiang Zhou
, Lili Wang
, Hu Liu^*
, Shiqi Peng

^*Corresponding author for this work

Capital Medical University
Peking University
Memorial University of Newfoundland

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Ala-Arg-Pro-Ala-Lys (ARPAK; also known as P6A) and 19 of its analogs were synthesized, and their thrombolytic activities were assessed in vitro and in vivo. The solution structures of 12 of the P6A analogs were determined using nuclear magnetic resonance (NMR) spectroscopy. The thrombolytic activity and conformational structure relationship was analyzed. We found that the Pro-Ala-Lys (PAK) sequence was essential for thrombolytic activity and was also responsible for the β-turn structure found in the P6A analogs studied. The well defined β turn may act as a binding head with the protruding lysine side-chain (positively charged) found at the target site for target recognition. Additionally, the N-terminal residue may be critical for thrombolytic activity, which for PAK-containing peptides, is likely achieved via a plasminogen-dependent pathway.

Original language	English
Pages (from-to)	730-740
Number of pages	11
Journal	Biochemistry and Cell Biology
Volume	85
Issue number	6
DOIs	https://doi.org/10.1139/O07-143
State	Published - Dec 2007
Externally published	Yes

Keywords

β-turn
Fibrinolysis
Peptide 6A, NMR structure
Plasminogen
Thrombolysis

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10.1139/O07-143

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@article{e1ca32b8681e4e0c97c69b075bf6d113,

title = "PAK: An essential motif for forming β-turn structures and exhibiting the thrombolytic effect of P6A and its analogs",

abstract = "Ala-Arg-Pro-Ala-Lys (ARPAK; also known as P6A) and 19 of its analogs were synthesized, and their thrombolytic activities were assessed in vitro and in vivo. The solution structures of 12 of the P6A analogs were determined using nuclear magnetic resonance (NMR) spectroscopy. The thrombolytic activity and conformational structure relationship was analyzed. We found that the Pro-Ala-Lys (PAK) sequence was essential for thrombolytic activity and was also responsible for the β-turn structure found in the P6A analogs studied. The well defined β turn may act as a binding head with the protruding lysine side-chain (positively charged) found at the target site for target recognition. Additionally, the N-terminal residue may be critical for thrombolytic activity, which for PAK-containing peptides, is likely achieved via a plasminogen-dependent pathway.",

keywords = "β-turn, Fibrinolysis, Peptide 6A, NMR structure, Plasminogen, Thrombolysis",

author = "Ming Zhao and Xin Jia and Chao Wang and Qin Li and Kexiang Zhou and Lili Wang and Hu Liu and Shiqi Peng",

year = "2007",

month = dec,

doi = "10.1139/O07-143",

language = "英语",

volume = "85",

pages = "730--740",

journal = "Biochemistry and Cell Biology",

issn = "0829-8211",

publisher = "National Research Council of Canada",

number = "6",

}

TY - JOUR

T1 - PAK

T2 - An essential motif for forming β-turn structures and exhibiting the thrombolytic effect of P6A and its analogs

AU - Zhao, Ming

AU - Jia, Xin

AU - Wang, Chao

AU - Li, Qin

AU - Zhou, Kexiang

AU - Wang, Lili

AU - Liu, Hu

AU - Peng, Shiqi

PY - 2007/12

Y1 - 2007/12

N2 - Ala-Arg-Pro-Ala-Lys (ARPAK; also known as P6A) and 19 of its analogs were synthesized, and their thrombolytic activities were assessed in vitro and in vivo. The solution structures of 12 of the P6A analogs were determined using nuclear magnetic resonance (NMR) spectroscopy. The thrombolytic activity and conformational structure relationship was analyzed. We found that the Pro-Ala-Lys (PAK) sequence was essential for thrombolytic activity and was also responsible for the β-turn structure found in the P6A analogs studied. The well defined β turn may act as a binding head with the protruding lysine side-chain (positively charged) found at the target site for target recognition. Additionally, the N-terminal residue may be critical for thrombolytic activity, which for PAK-containing peptides, is likely achieved via a plasminogen-dependent pathway.

AB - Ala-Arg-Pro-Ala-Lys (ARPAK; also known as P6A) and 19 of its analogs were synthesized, and their thrombolytic activities were assessed in vitro and in vivo. The solution structures of 12 of the P6A analogs were determined using nuclear magnetic resonance (NMR) spectroscopy. The thrombolytic activity and conformational structure relationship was analyzed. We found that the Pro-Ala-Lys (PAK) sequence was essential for thrombolytic activity and was also responsible for the β-turn structure found in the P6A analogs studied. The well defined β turn may act as a binding head with the protruding lysine side-chain (positively charged) found at the target site for target recognition. Additionally, the N-terminal residue may be critical for thrombolytic activity, which for PAK-containing peptides, is likely achieved via a plasminogen-dependent pathway.

KW - β-turn

KW - Fibrinolysis

KW - Peptide 6A, NMR structure

KW - Plasminogen

KW - Thrombolysis

UR - https://www.scopus.com/pages/publications/38849090525

U2 - 10.1139/O07-143

DO - 10.1139/O07-143

M3 - 文章

C2 - 18059531

AN - SCOPUS:38849090525

SN - 0829-8211

VL - 85

SP - 730

EP - 740

JO - Biochemistry and Cell Biology

JF - Biochemistry and Cell Biology

IS - 6

ER -

PAK: An essential motif for forming β-turn structures and exhibiting the thrombolytic effect of P6A and its analogs

Abstract

Keywords

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