6,843 research outputs found

    Asian tauiwi and tangata whenua: Māori-Asian relationships and their implications for Aotearoa New Zealandā€™s constitutional future

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    This article traces the history of migration by Asian peoples to Aotearoa New Zealand and examines how their relationships with Māori has evolved and been influenced by the social, economic and political climate. Although Asian and Māori communities have often been pitted against each other by mainstream narratives, they share many common values and are natural allies ā€“ including in constitutional transformation. Despite perceptions to the contrary, there is strong compatibility between recognising te Tiriti and supporting Aotearoaā€™s ethnically and culturally diverse population. I argue that honouring te Tiriti is a foundational step towards addressing injustice and supporting all those who live in Aotearoa

    Identification and characterization of human plasma prekallikrein-prolylcarboxypeptidase interaction sites

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    Prolylcarboxypeptidase isoform1 (PRCP1, also known as angiotensinase C, PCP, PRCP, PrCP) is a widely distributed serine protease found throughout the human body. PRCP1 removes the C-terminal amino acid which is next to a proline residue of a peptide. Through this activity, PRCP1 is postulated to play distinct biological roles including the regulation of vascular homeostasis, the induction of inflammation and the adjustment of metabolism. Compelling evidence indicates that human PRCP1 activates plasma prekallikrein (PK) to kallikrein on endothelial cells. However, the mechanism of this activation is yet unknown. The formation of kallikrein leads to the generation of proinflammatory factors and the activation of the blood coagulation intrinsic pathway, both of which are deeply involved in human diseases such as angioedema, disseminated intravascular coagulation, acute respiratory distress syndrome and sepsis. Therefore, the identification of PRCP/PK binding sites, and PRCP cleavage sites on PK, may be of clinical significance which would aid drug design. To address this issue, a combination of peptide mapping and site-directed mutagenesis approaches were employed to investigate the regulation of PK by PRCP1. The synthetic peptide corresponding to the last 10 amino acids of PK C-terminus inhibited PRCP1 activity. Three recombinant PKs (rPK), which are only distinct from each other at the extreme C-terminus, exhibited elevated susceptibility to PRCP1-induced activation. Our results demonstrate that the PK C-terminus participates in PRCP1-induced activation of PK. However, due to the fact that PRCP1 can still activate the rPKs which have modified C-termini, the C-terminus of PK may not be a major cleavage site for PRCP1. Using synthetic peptides corresponding to the N-terminus or the catalytic region of PRCP1, two sites were identified to be involved in binding of PRCP1 to PK, one of which lies in the N-terminus of PRCP1, whereas the other one locates adjacent to the opening of the active site. In summary, our results indicate that the C-terminus of PK is involved in, but not necessary for PRCP1-induced PK activation. The interaction between PK and PRCP1 occurs at multiple sites on PRCP1, including both the N-terminal region and a portion adjacent to the catalytic domain

    Greening Supply Chains in China: Practical Lessons From China-Based Suppliers in Achieving Environmental Performance

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    Presents case studies of how five China-based suppliers are meeting international buyers' environmental requirements. Examines management processes; effective low-cost ways to reduce water pollution; and the roles of multistakeholders and third parties
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