Heparin Cofactor II: Discovery, Properties, and Role in Controlling Vascular Homeostasis

Rau, Jill C.; Mitchell, Jennifer W.; Fortenberry, Yolanda M.; Church, Frank C.

doi:10.1055/s-0031-1276582

Cited by 31 publications

(21 citation statements)

References 85 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Pathway analysis revealed a strong activation of the coagulation system, indicative of damage to the endothelial lining of microvessels. The up-regulation of genes coding anticoagulant factors such as Serpinc1 (ATIII) and Serpind1 (heparin cofactor II) may suggest a link of activated anticoagulant factors to intestinal bleeding [12]–[14]. The increased expression of the procoagulant factors F8 [15] and Bdkrb1 [16], [17] as well as an inhibitor of a wide variety of proteases Serpina1 (alpha-1 antiproteinase) [18] could be explained as a compensatory response to achieve a balanced hemostasis and protect the tissue from degradation.…”

Section: Discussionmentioning

confidence: 99%

Laser Capture Microdissected Mucosa versus Whole Tissue Specimens for Assessment of Radiation-Induced Dynamic Molecular and Pathway Changes in the Small Intestine

et al. 2013

View full text Add to dashboard Cite

BackgroundThe intestinal mucosa is the compartment that sustains the most severe injury in response to radiation and is therefore of primary interest. The use of whole gut extracts for analysis of gene expression may confound important changes in the mucosa. On the other hand, laser capture microdissection (LCM) is hampered by the unstable nature of RNA and by a more complicated collection process. This study assessed, in parallel samples from a validated radiation model, the indications for use of LCM for intestinal gene expression analysis.Methodology/Principal FindingsRNA was extracted from mouse whole intestine and from mucosa by LCM at baseline and 4 h, 24 h, and 3.5 d after total body irradiation and subjected to microarray analysis. Among mucosal genes that were altered > = 2-fold, less than 7% were present in the whole gut at 4 and 24 h, and 25% at 3.5 d. As expected, pathway analysis of mucosal LCM samples showed that radiation activated the coagulation system, lymphocyte apoptosis, and tight junction signaling, and caused extensive up-regulation of cell cycle and DNA damage repair pathways. Using similar stringent criteria, regulation of these pathways, with exception of the p53 pathway, was undetectable in the whole gut. Radiation induced a dramatic increase of caspase14 and ectodysplasin A2 receptor (Eda2r), a TNFα receptor, in both types of samples.Conclusions/SignificanceLCM-isolated mucosal specimens should be used to study cellular injury, cell cycle control, and DNA damage repair pathways. The remarkable increase of caspase14 and Eda2r suggests a novel role for these genes in regulating intestinal radiation injury. Comparative gene expression data from complex tissues should be interpreted with caution.

show abstract

Section: Discussionmentioning

confidence: 99%

Laser Capture Microdissected Mucosa versus Whole Tissue Specimens for Assessment of Radiation-Induced Dynamic Molecular and Pathway Changes in the Small Intestine

et al. 2013

View full text Add to dashboard Cite

show abstract

“…Vascular endothelium has strategic location between the plasma and the underlying tissue and is an active paracrine, endocrine, and autocrine organ that is indispensable for the regulation of vascular tone and the maintenance of vascular homeostasis (36)(37)(38)(39)(40)(41). Macrophages, fibroblasts, and endothelial cells all move into wounds at the same time.…”

Section: Fig 1 Pathogenesis Ofatherosclerosismentioning

confidence: 99%

Endothelial Cells, Cholesterol, Cytokines, and Aging

Tetè

Tripodi

Rosati

et al. 2012

Int J Immunopathol Pharmacol

View full text Add to dashboard Cite

It has been reported that high levels of cholesterol and triglycerides are associated with increased risk of developing atherosclerosis and shorter life. In fact, vascular endothelial dysfunction occurs during the human aging process. Accumulation of lipids in vascular endothelium activates leukocytes to produce cytokines and chemokines which recruit macrophages. On the other hand, macrophages augment inflammatory response and secrete vascular endothelial growth factor, a key cytokine that mediates angiogenesis and inflammatory response. In addition, hyperlipidaemia is one of the main risk factors for aging, hypertension and diabetes. Here, we review the interrelationship between endothelial cells, high level of cholesterol, and aging.

show abstract

“…Heparin cofactor II (HCII) is a 66 kDa plasma protein and member of the serpin superfamily of protease inhibitors [1,2] (reviewed in [3]). It regulates the key coagulation protease thrombin by trapping it in a covalently-linked denaturation-resistant complex.…”

Section: Introductionmentioning

confidence: 99%

The complete N-terminal extension of heparin cofactor II is required for maximal effectiveness as a thrombin exosite 1 ligand

et al. 2013

View full text Add to dashboard Cite

BackgroundHeparin cofactor II (HCII) is a circulating protease inhibitor, one which contains an N-terminal acidic extension (HCII 1-75) unique within the serpin superfamily. Deletion of HCII 1-75 greatly reduces the ability of glycosaminoglycans (GAGs) to accelerate the inhibition of thrombin, and abrogates HCII binding to thrombin exosite 1. While a minor portion of HCII 1-75 can be visualized in a crystallized HCII-thrombin S195A complex, the role of the rest of the extension is not well understood and the affinity of the HCII 1-75 interaction has not been quantitatively characterized. To address these issues, we expressed HCII 1-75 as a small, N-terminally hexahistidine-tagged polypeptide in E. coli.ResultsImmobilized purified HCII 1-75 bound active α-thrombin and active-site inhibited FPR-ck- or S195A-thrombin, but not exosite-1-disrupted γT-thrombin, in microtiter plate assays. Biotinylated HCII 1-75 immobilized on streptavidin chips bound α-thrombin and FPR-ck-thrombin with similar KD values of 330-340 nM. HCII 1-75 competed thrombin binding to chip-immobilized HCII 1-75 more effectively than HCII 54-75 but less effectively than the C-terminal dodecapeptide of hirudin (mean Ki values of 2.6, 8.5, and 0.29 μM, respectively). This superiority over HCII 54-75 was also demonstrated in plasma clotting assays and in competing the heparin-catalysed inhibition of thrombin by plasma-derived HCII; HCII 1-53 had no effect in either assay. Molecular modelling of HCII 1-75 correctly predicted those portions of the acidic extension that had been previously visualized in crystal structures, and suggested that an α-helix found between residues 26 and 36 stabilizes one found between residues 61-67. The latter region has been previously shown by deletion mutagenesis and crystallography to play a crucial role in the binding of HCII to thrombin exosite 1.ConclusionsAssuming that the KD value for HCII 1-75 of 330-340 nM faithfully predicts that of this region in intact HCII, and that 1-75 binding to exosite 1 is GAG-dependent, our results support a model in which thrombin first binds to GAGs, followed by HCII addition to the ternary complex and release of HCII 1-75 for exosite 1 binding and serpin mechanism inhibition. They further suggest that, in isolated or transferred form, the entire HCII 1-75 region is required to ensure maximal binding of thrombin exosite 1.

show abstract

Heparin Cofactor II: Discovery, Properties, and Role in Controlling Vascular Homeostasis

Cited by 31 publications

References 85 publications

Laser Capture Microdissected Mucosa versus Whole Tissue Specimens for Assessment of Radiation-Induced Dynamic Molecular and Pathway Changes in the Small Intestine

Laser Capture Microdissected Mucosa versus Whole Tissue Specimens for Assessment of Radiation-Induced Dynamic Molecular and Pathway Changes in the Small Intestine

Endothelial Cells, Cholesterol, Cytokines, and Aging

The complete N-terminal extension of heparin cofactor II is required for maximal effectiveness as a thrombin exosite 1 ligand

Contact Info

Product

Resources

About