Your search keyword '"Masci PP"' showing total 69 results

1. Anti-Coagulant and Anti-Thrombotic Properties of Blacklip Abalone (Haliotis rubra): In Vitro and Animal Studies

Author

Suleria, HAR, Masci, PP, Zhao, K-N, Addepalli, R, Chen, W, Osborne, SA, Gobe, GC, Suleria, HAR, Masci, PP, Zhao, K-N, Addepalli, R, Chen, W, Osborne, SA, and Gobe, GC

Abstract

Sulphated polysaccharides with anti-thrombotic and anti-coagulant activities have been found in various marine biota. In this study, a previously characterised anti-thrombotic and anti-coagulant extract from blacklip abalone was fractionated by anion exchange chromatography (AEC), pooled (on a sulphated polysaccharide basis) and administered to Wistar rats via oral gavage (N = 8) for assessment as an oral therapeutic. To ensure that the preparation had anti-coagulant activity prior to oral administration, it was assessed in rat blood by thromboelastography (TEG) significantly increasing reaction (R) time (or time until clot formation). Following in vitro confirmation of anti-coagulant activity, 40 mg of the preparation was orally administered to rats with blood samples collected at 2, 4, and 6 h post-gavage. Assessment of all blood samples by TEG showed some prolongation of R time from 355 to 380 s after 4 h. Dosing of the post-gavage blood samples with the abalone preparation to confirm anti-thrombotic activity in vitro revealed residual anti-coagulant activity, further suggesting that oral administration did increase anti-coagulant potential in the collected blood but that bioavailability was low. Assessment of tissues and haematological parameters showed no obvious harmful effects of the abalone preparation in animals. In summary, even though oral administration of fractionated and pooled blacklip abalone extract to rats delayed clotting after 4 h, bioavailability of the preparation appeared to be low and may be more appropriate for intravenous administration as an anti-thrombotic or anti-coagulant therapeutic.

Published

2017

2. Rapid Radiations and the Race to Redundancy: An Investigation of the Evolution of Australian Elapid Snake Venoms

Author

Jackson, TNW, Koludarov, I, Ali, SA, Dobson, J, Zdenek, CN, Dashevsky, D, op den Brouw, B, Masci, PP, Nouwens, A, Josh, P, Goldenberg, J, Cipriani, V, Hay, C, Hendrikx, I, Dunstan, N, Allen, L, Fry, BG, Jackson, TNW, Koludarov, I, Ali, SA, Dobson, J, Zdenek, CN, Dashevsky, D, op den Brouw, B, Masci, PP, Nouwens, A, Josh, P, Goldenberg, J, Cipriani, V, Hay, C, Hendrikx, I, Dunstan, N, Allen, L, and Fry, BG

Abstract

Australia is the stronghold of the front-fanged venomous snake family Elapidae. The Australasian elapid snake radiation, which includes approximately 100 terrestrial species in Australia, as well as Melanesian species and all the world's sea snakes, is less than 12 million years old. The incredible phenotypic and ecological diversity of the clade is matched by considerable diversity in venom composition. The clade's evolutionary youth and dynamic evolution should make it of particular interest to toxinologists, however, the majority of species, which are small, typically inoffensive, and seldom encountered by non-herpetologists, have been almost completely neglected by researchers. The present study investigates the venom composition of 28 species proteomically, revealing several interesting trends in venom composition, and reports, for the first time in elapid snakes, the existence of an ontogenetic shift in the venom composition and activity of brown snakes (Pseudonaja sp.). Trends in venom composition are compared to the snakes' feeding ecology and the paper concludes with an extended discussion of the selection pressures shaping the evolution of snake venom.

Published

2016

3. Oral administration of dermatan sulphate reduces venous thrombus formation in vivo: potential use as a formulation for venous thromboembolism.

Author

Osborne SA, Masci PP, Du QS, Daniel RA, Desilva K, Vitetta L, Zhao KN, and Seymour RB

Subjects

Administration, Oral, Animals, Anticoagulants administration & dosage, Cattle, Collagen metabolism, Dermatan Sulfate administration & dosage, Disease Models, Animal, Enoxaparin pharmacology, Male, Rabbits, Thrombelastography, Venous Thromboembolism drug therapy, Venous Thromboembolism pathology, Venous Thrombosis pathology, Anticoagulants pharmacology, Dermatan Sulfate pharmacology, Venous Thrombosis drug therapy

Abstract

Dermatan sulphate (DS) is a sulphated polysaccharide that displays complexity in constituent sulphated disaccharides and interacts with proteins and signalling molecules to modulate numerous biological processes, including inhibition of the coagulation cascade and regulation of blood clotting and fibrinolysis. This study shows the antithrombotic and anticoagulant effects of DS prepared from bovine collagen waste liquor following oral and intravenous administrations in a deep vein thrombosis (DVT) rabbit model. In vitro, the prothrombin time, activated partial thromboplastin time, and thrombin citrated plasma clotting assays revealed that bovine DS had strong antithrombotic and anticoagulant effects comparable to low-molecular-weight heparin [Clexane ® (enoxaparin sodium)]. In a DVT rabbit model, animals received intravenous and oral administrations of bovine DS and Clexane ® providing further evidence that both agents had strong antithrombotic and anticoagulant effects by significantly reducing or preventing clot formation. Thromboelastography (TEG) assays revealed further that both bovine DS and Clexane ® substantially prolonged the clotting time of recalcified citrated whole blood, but only bovine DS could retain clot strength suggesting that bovine DS had less effect on platelet-fibrin interactions. In conclusion, this is the first report that oral administration of DS from bovine collagen waste liquor reduces experimental venous thrombus formation warranting further research into bovine DS as an oral antithrombotic therapeutic.

Published

2021

4. PAR2 Activation on Human Kidney Tubular Epithelial Cells Induces Tissue Factor Synthesis, That Enhances Blood Clotting.

Author

Iyer A, Humphries TLR, Owens EP, Zhao KN, Masci PP, Johnson DW, Nikolic-Paterson D, Gobe GC, Fairlie DP, and Vesey DA

Abstract

Coagulation abnormalities and increased risk of atherothrombosis are common in patients with chronic kidney diseases (CKD). Mechanisms that alter renal hemostasis and lead to thrombotic events are not fully understood. Here we show that activation of protease activated receptor-2 (PAR2) on human kidney tubular epithelial cells (HTECs), induces tissue factor (TF) synthesis and secretion that enhances blood clotting. PAR-activating coagulation-associated protease (thrombin), as well as specific PAR2 activators (matriptase, trypsin, or synthetic agonist 2f-LIGRLO-NH 2 (2F), induced TF synthesis and secretion that were potently inhibited by PAR2 antagonist, I-191. Thrombin-induced TF was also inhibited by a PAR1 antagonist, Vorapaxar. Peptide activators of PAR1, PAR3, and PAR4 failed to induce TF synthesis. Differential centrifugation of the 2F-conditoned medium sedimented the secreted TF, together with the exosome marker ALG-2 interacting protein X (ALIX), indicating that secreted TF was associated with extracellular vesicles. 2F-treated HTEC conditioned medium significantly enhanced blood clotting, which was prevented by pre-incubating this medium with an antibody for TF. In summary, activation of PAR2 on HTEC stimulates synthesis and secretion of TF that induces blood clotting, and this is attenuated by PAR2 antagonism. Thrombin-induced TF synthesis is at least partly mediated by PAR1 transactivation of PAR2. These findings reveal how underlying hemostatic imbalances might increase thrombosis risk and subsequent chronic fibrin deposition in the kidneys of patients with CKD and suggest PAR2 antagonism as a potential therapeutic strategy for intervening in CKD progression., Competing Interests: DJ has received consultancy fees, research grants, speaker’s honoraria and travel sponsorships from Baxter Healthcare and Fresenius Medical Care, consultancy fees from Astra Zeneca and AWAK, speaker’s honoraria and travel sponsorships from ONO, and travel sponsorships from Amgen. DJ is a current recipient of an Australian National Health and Medical Research Council Practitioner Fellowship. DF is an inventor on a patent (AU20109033378) covering PAR2 agonists and antagonists that is owned by The University of Queensland. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Iyer, Humphries, Owens, Zhao, Masci, Johnson, Nikolic-Paterson, Gobe, Fairlie and Vesey.)

Published

2021

5. Progress curve analysis of microtitre plate plasma clotting assays. Assessment of tissue factor levels.

Author

Humphries TLR, Johnson LA, Masci PP, Gobe GC, and Vesey DA

Subjects

Humans, Models, Theoretical, Plasma, Reproducibility of Results, Sensitivity and Specificity, Thrombelastography methods, Thromboplastin urine, Blood Coagulation, Blood Coagulation Tests methods, Thromboplastin analysis

Abstract

MTP plasma clotting assays monitor the time course of fibrin formation in re-calcified plasma by absorbance measurements and are increasingly used as alternatives to traditional one-point clot time assays employed in clinical laboratories to detect thrombotic disorders. The parameters derived from these analyses are analogous to thromboelastography viz. time, rate and maximum extent of clot formation. The derived parameters, based on the whole course of the clotting reaction are more robust, informative and quantitative than single-point clot time assays. However, the parameters themselves are usually obtained arbitrarily by crude graphical analysis of subjectively selected points of progress curves. The current work aimed to investigate the sensitivity and reproducibility of an MTP clotting assay and examine its suitability for measuring tissue factor (TF) levels in cell culture medium and patient urine. The results demonstrate that progress curves can be analysed by fitting a logistic equation, derived from a simplified autocatalytic clot formation model. The parameters, maximum amplitude (Fm), rate constant (k), time to half-maximum amplitude (tm) and maximum rate of clot formation (vm), fit a power curve showing limiting effects with increasing TF concentration. Log/log plots of tm and k against TF concentration provide standard curves for assessment of unknowns., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2021

6. Progress Curve Analysis of the one stage chromogenic assay for ecarin.

Author

Johnson LA, de Jersey J, Masci PP, Zhao KN, Bennett NC, Dimeski G, Grant M, and Lavin MF

Subjects

Aniline Compounds chemistry, Animals, Humans, Hydrolysis, Kinetics, Limit of Detection, Linear Models, Prothrombin chemistry, Reference Standards, Reproducibility of Results, Thrombin chemistry, Chromogenic Compounds chemistry, Dipeptides chemistry, Endopeptidases analysis, Enzyme Assays methods

Abstract

Snake venom prothrombin activators such as Ecarin are readily assayed by continuous spectrophotometric monitoring of p-nitroaniline production in a one step assay containing prothrombin and a p-nitroanilide peptide substrate for thrombin. The coupled reactions result in accelerating p-nitroaniline (pNA) production over the course of the assay giving non-linear progress curves, from which initial velocities are not readily obtained. Most studies therefore resort to approximate estimates of activity, based on the absorbance reached at an arbitrary time. A simple kinetic analysis of the coupled reactions shows that the early points of such curves should be fitted by second order polynomials, representing the accelerating reaction rate in μmol pNA/min/min. The first derivative of the polynomial then gives the increasing velocity of pNA production in μmol pNA/min over the time course of the assay. We demonstrate here that, with the substrate S2238, these rates can be converted to absolute thrombin concentrations using the Michaelis-Menten equation, substituted with values for kcat and Km. These thrombin concentrations increase linearly over the time course of the assay allowing the activity to be expressed in units, defined as μmol product/min, most commonly used to report enzyme activity., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

7. Rapid serum tube technology overcomes problems associated with use of anticoagulants.

Author

Zhao KN, Dimeski G, de Jersey J, Johnson LA, Grant M, Masci PP, and Lavin MF

Subjects

Blood Coagulation drug effects, Blood Coagulation Tests, Heparin pharmacology, Humans, Anticoagulants pharmacology, Prothrombin pharmacology

Abstract

Introduction: Failure to obtain complete blood clotting in serum is a common laboratory problem. Our aim was to determine whether snake proth-rombin activators are effective in clotting blood and producing quality serum for analyte measurement in anticoagulated patients., Materials and Methods: Whole blood clotting was studied in a total of 64 blood samples (41 controls, 20 Warfarin patients, 3 anticoagulated patients using snake venom prothrombin activator (OsPA)) with plain tubes. Coagulation was analysed using a visual assay, Hyland-Clotek and thromboelastography. Healthy control blood was spiked with a range of anticoagulants to determine the effectiveness of OsPa-induced clotting. A paired analysis of a Dabigatran patient and a control investigated the effectiveness of the OsPA clotting tubes. Biochemical analytes (N = 31) were determined for 7 samples on chemistry and immunoassay analysers and compared with commercial tubes., Results: Snake venom prothrombin activators efficiently coagulated blood and plasma spiked with heparin and commonly used anticoagulants. Clotting was observed in the presence of anticoagulants whereas no clotting was observed in BDRST tubes containing 3 U/mL of heparin. Snake venom prothrombin activator enhanced heparinised blood clotting by shortening substantially the clotting time and improving significantly the strength of the clot. Comparison of 31 analytes from the blood of five healthy and two anticoagulated participants gave very good agreement between the analyte concentrations determined., Conclusions: Our results showed that the snake venom prothrombin activators OsPA and PtPA efficiently coagulated recalcified and fresh bloods with or without added anticoagulants. These procoagulants produced high quality serum for accurate analyte measurement., Competing Interests: Potential conflict of interest: The project was in part funded by a Development grant from the National Health and Medical Research Council of Australia and by Q-Sera Pty Ltd, Australia., (©Croatian Society of Medical Biochemistry and Laboratory Medicine.)

Published

2019

8. Next-generation rapid serum tube technology using prothrombin activator coagulant: fast, high-quality serum from normal samples.

Author

Zhao KN, Dimeski G, de Jersey J, Johnson LA, Grant M, Masci PP, and Lavin MF

Subjects

Animals, Healthy Volunteers, Humans, Snake Venoms chemistry, Blood Coagulation drug effects, Blood Coagulation Tests, Blood Specimen Collection, Coagulants pharmacology, Prothrombin pharmacology

Abstract

Background Incomplete blood clotting or latent clotting in serum is a common laboratory problem, especially for patients on anticoagulant therapy or when serum tubes are centrifuged before clotting is completed. We describe a novel approach to producing high-quality serum using snake venom prothrombin activator complex (OsPA) as an additive in blood collection tubes for non-anticoagulated (normal) individuals. Methods Plasma clotting assays were performed using a Hyland-Clotek instrument. Blood clotting was visually observed, and thromboelastography was also performed to determine the important parameters of coagulation. Thrombin generation was assayed using the chromogenic substrate S-2238, and biochemical analytes in the serum were determined on chemistry and immunoassay analysers. Fibrinogen was determined by either ELISA or Clauss fibrinogen assay. Results We initially showed that OsPA had strong coagulation activity in clotting not only recalcified citrated plasma and recalcified citrated whole blood, but also fresh whole blood in a clinical setting. The use of TEG clearly showed improved speed of clotting and generation of a firmer clot. We also showed that the use of OsPA to produce serum did not interfere with the determination of commonly measured biochemical analytes. The underlying clotting mechanism involves a burst of thrombin production at the initial stages of the clotting process upon contact with prothrombin in blood. Conclusions These results demonstrate rapid generation of high-quality serum, contributing to faster turnaround times with standardised quality samples, for accurate analyte determinations in normal individuals.

Published

2019

9. Anti-Coagulant and Anti-Thrombotic Properties of Blacklip Abalone (Haliotis rubra): In Vitro and Animal Studies.

Author

Suleria HAR, Masci PP, Zhao KN, Addepalli R, Chen W, Osborne SA, and Gobe GC

Subjects

Animals, Anticoagulants chemistry, Blood Coagulation Tests, Fibrinolytic Agents chemistry, In Vitro Techniques, Polysaccharides, Rats, Rats, Wistar, Anticoagulants isolation & purification, Anticoagulants pharmacology, Fibrinolytic Agents isolation & purification, Fibrinolytic Agents pharmacology, Gastropoda chemistry, Seafood

Abstract

Sulphated polysaccharides with anti-thrombotic and anti-coagulant activities have been found in various marine biota. In this study, a previously characterised anti-thrombotic and anti-coagulant extract from blacklip abalone was fractionated by anion exchange chromatography (AEC), pooled (on a sulphated polysaccharide basis) and administered to Wistar rats via oral gavage (N = 8) for assessment as an oral therapeutic. To ensure that the preparation had anti-coagulant activity prior to oral administration, it was assessed in rat blood by thromboelastography (TEG) significantly increasing reaction (R) time (or time until clot formation). Following in vitro confirmation of anti-coagulant activity, 40 mg of the preparation was orally administered to rats with blood samples collected at 2, 4, and 6 h post-gavage. Assessment of all blood samples by TEG showed some prolongation of R time from 355 to 380 s after 4 h. Dosing of the post-gavage blood samples with the abalone preparation to confirm anti-thrombotic activity in vitro revealed residual anti-coagulant activity, further suggesting that oral administration did increase anti-coagulant potential in the collected blood but that bioavailability was low. Assessment of tissues and haematological parameters showed no obvious harmful effects of the abalone preparation in animals. In summary, even though oral administration of fractionated and pooled blacklip abalone extract to rats delayed clotting after 4 h, bioavailability of the preparation appeared to be low and may be more appropriate for intravenous administration as an anti-thrombotic or anti-coagulant therapeutic., Competing Interests: The authors have no conflict of interest.

Published

2017

10. Evaluation of the Greiner Bio-One serum separator BCA Fast Clot tube.

Author

Dimeski G, Johnston J, Masci PP, Zhao KN, and Brown N

Subjects

Humans, Thrombelastography, Time Factors, Blood Coagulation, Blood Specimen Collection instrumentation, Serum

Abstract

Background: Current commercial tubes have difficulties in producing "true" serum from all blood samples even within the recommended clotting times. Hence, Becton Dickinson (BD) and now Greiner have produced tubes containing thrombin as the procoagulant to reduce the clotting time and increase the possibility of producing serum from anticoagulated blood samples., Methods: The Greiner BCA Fast Clot (GBBCAFC) tube was evaluated in a hospital environment using 40 participants, (30 healthy and 10 undergoing renal dialysis) for 32 analytes against the Greiner lithium heparin tube and the BD Rapid Serum Tubes (BD RST) tube measured on Beckman DxC 800 and DxI 800 analyzers. Clotting strength was also examined using thromboelastography (TEG)., Results: The analytes results showed there was a very close agreement between the BD RST tube and GBBCAFC tube in comparison with lithium heparin plasma. The result comparison data showed equivalent performance with lower levels of hemolysis. The prolonged storage study also showed very similar agreement between the BD RST and the GBBCAFC tubes. Likewise, the TEG data showed there was very little difference in clotting ability between the tubes, and neither was capable of producing true serum from blood spiked with 2 U heparin/mL of blood., Conclusions: The study showed the GBBCAFC tube with the combination of the two procoagulants blood clotting activator and thrombin produced comparable performance with the lithium heparin plasma and the BD RST serum samples.

Published

2017

11. In vitro anti-thrombotic and anti-coagulant properties of blacklip abalone (Haliotis rubra) viscera hydrolysate.

Author

Suleria HAR, Masci PP, Addepalli R, Chen W, Gobe GC, and Osborne SA

Subjects

Animals, Anticoagulants isolation & purification, Anticoagulants pharmacology, Fibrinolytic Agents isolation & purification, Fibrinolytic Agents pharmacology, Humans, Hydrolysis, Partial Thromboplastin Time, Polysaccharides isolation & purification, Polysaccharides pharmacology, Prothrombin Time, Sulfates chemistry, Sulfates pharmacology, Thrombelastography, Anticoagulants chemistry, Blood Coagulation drug effects, Fibrinolytic Agents chemistry, Gastropoda chemistry, Polysaccharides chemistry

Abstract

Abalone viscera contain sulphated polysaccharides with anti-thrombotic and anti-coagulant activities. In this study, a hydrolysate was prepared from blacklip abalone (Haliotis rubra) viscera using papain and bromelain and fractionated using ion exchange and size exclusion chromatography. Hydrolysates and fractions were investigated for in vitro thrombin inhibition mediated through heparin cofactor II (HCII) as well as anti-coagulant activity in plasma and whole blood. On the basis of sulphated polysaccharide concentration, the hydrolysate inhibited thrombin through HCII with an inhibitor concentration at 50% (IC50) of 16.5 μg/mL compared with 2.1 μg/mL for standard heparin. Fractionation concentrated HCII-mediated thrombin inhibition down to an IC50 of 1.8 μg/mL and improved anti-coagulant activities by significantly delaying clotting time. This study confirmed the presence of anti-thrombotic and anti-coagulant molecules in blacklip abalone viscera and demonstrated that these activities can be enriched with a simple chromatography regime. Blacklip abalone viscera warrant further investigation as a source of nutraceutical or functional food ingredients. Graphical abstract Schematic showing preparation of bioactive extracts and fractions from blacklip abalone.

Published

2017

12. Therapeutic potential of abalone and status of bioactive molecules: A comprehensive review.

Author

Suleria HA, Masci PP, Gobe GC, and Osborne SA

Subjects

Animals, Anti-Infective Agents chemistry, Anti-Infective Agents pharmacology, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Anticoagulants chemistry, Anticoagulants pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Antioxidants chemistry, Antioxidants pharmacology, Aquaculture, Dietary Supplements, Fibrinolytic Agents chemistry, Fibrinolytic Agents pharmacology, Food Handling, Aquatic Organisms chemistry, Gastropoda chemistry, Shellfish analysis

Abstract

Marine organisms are increasingly being investigated as sources of bioactive molecules with therapeutic applications as nutraceuticals and pharmaceuticals. In particular, nutraceuticals are gaining popularity worldwide owing to their therapeutic potential and incorporation in functional foods and dietary supplements. Abalone, a marine gastropod, contains a variety of bioactive compounds with anti-oxidant, anti-thrombotic, anti-inflammatory, anti-microbial, and anti-cancer activities. For thousands of years different cultures have used abalone as a traditional functional food believing consumption provides health benefits. Abalone meat is one of the most precious commodities in Asian markets where it is considered a culinary delicacy. Recent research has revealed that abalone is composed of many vital moieties like polysaccharides, proteins, and fatty acids that provide health benefits beyond basic nutrition. A review of past and present research is presented with relevance to the therapeutic potential of bioactive molecules from abalone.

Published

2017

13. Rapid Radiations and the Race to Redundancy: An Investigation of the Evolution of Australian Elapid Snake Venoms.

Author

Jackson TN, Koludarov I, Ali SA, Dobson J, Zdenek CN, Dashevsky D, Op den Brouw B, Masci PP, Nouwens A, Josh P, Goldenberg J, Cipriani V, Hay C, Hendrikx I, Dunstan N, Allen L, and Fry BG

Subjects

Animals, Australia, Blood Coagulation drug effects, Elapidae genetics, Elapidae physiology, Evolution, Molecular, Female, Humans, Male, Predatory Behavior, Elapid Venoms chemistry, Elapid Venoms genetics, Elapid Venoms toxicity

Abstract

Australia is the stronghold of the front-fanged venomous snake family Elapidae. The Australasian elapid snake radiation, which includes approximately 100 terrestrial species in Australia, as well as Melanesian species and all the world's sea snakes, is less than 12 million years old. The incredible phenotypic and ecological diversity of the clade is matched by considerable diversity in venom composition. The clade's evolutionary youth and dynamic evolution should make it of particular interest to toxinologists, however, the majority of species, which are small, typically inoffensive, and seldom encountered by non-herpetologists, have been almost completely neglected by researchers. The present study investigates the venom composition of 28 species proteomically, revealing several interesting trends in venom composition, and reports, for the first time in elapid snakes, the existence of an ontogenetic shift in the venom composition and activity of brown snakes ( Pseudonaja sp.). Trends in venom composition are compared to the snakes' feeding ecology and the paper concludes with an extended discussion of the selection pressures shaping the evolution of snake venom., Competing Interests: The authors declare no conflict of interest.

Published

2016

14. Alteration of blood clot structures by interleukin-1 beta in association with bone defects healing.

Author

Wang X, Friis TE, Masci PP, Crawford RW, Liao W, and Xiao Y

Subjects

Animals, Biomechanical Phenomena, Blood Coagulation physiology, Disease Models, Animal, Fibrinolysis, Hematoma blood, Hematoma pathology, Humans, Interleukin-1beta blood, Microscopy, Electron, Scanning, Rats, Rats, Inbred F344, S-Nitrosoglutathione pharmacology, Thrombosis blood, Thrombosis pathology, Fibrin metabolism, Fracture Healing physiology, Hematoma physiopathology, Interleukin-1beta metabolism, Thrombosis physiopathology

Abstract

The quality of hematomas are crucial for successful early bone defect healing, as the structure of fibrin clots can significantly influence the infiltration of cells, necessary for bone regeneration, from adjacent tissues into the fibrin network. This study investigated if there were structural differences between hematomas from normal and delayed healing bone defects and whether such differences were linked to changes in the expression of IL-1β. Using a bone defect model in rats, we found that the hematomas in the delayed healing model had thinner fibers and denser clot structures. Moreover, IL-1β protein levels were significantly higher in the delayed healing hematomas. The effects of IL-1β on the structural properties of human whole blood clots were evaluated by thrombelastograph (TEG), scanning electronic microscopy (SEM), compressive study, and thrombolytic assays. S-nitrosoglutathione (GSNO) was applied to modulate de novo hematoma structure and the impact on bone healing was evaluated in the delayed healing model. We found that GSNO produced more porous hematomas with thicker fibers and resulted in significantly enhanced bone healing. This study demonstrated that IL-1β and GSNO had opposing effects on clot architecture, the structure of which plays a pivotal role in early bone healing.

Published

2016

15. Characterization and structural analysis of a potent anticoagulant phospholipase A2 from Pseudechis australis snake venom.

Author

Du QS, Trabi M, Richards RS, Mirtschin P, Madaras F, Nouwens A, Zhao KN, de Jersey J, Lavin MF, Guddat LW, and Masci PP

Subjects

Amino Acid Sequence, Animals, Blood Proteins chemistry, Humans, Models, Molecular, Oculomotor Nerve Diseases, Protein Conformation, Prothrombin Time, Rabbits, Thrombelastography, Blood Proteins pharmacology, Elapid Venoms chemistry, Elapidae physiology, Phospholipases A2 metabolism

Abstract

Pseudechis australis is one of the most venomous and lethal snakes in Australia. Numerous phospholipase A2 (PLA2) isoforms constitute a major portion of its venom, some of which have previously been shown to exhibit not only enzymatic, but also haemolytic, neurotoxic and anticoagulant activities. Here, we have purified a potent anticoagulant PLA2 (identified as PA11) from P. australis venom to investigate its phospholipase, anticoagulant, haemolytic and cytotoxic activities and shown that addition of 11 nM PA11 resulted in a doubling of the clotting time of recalcified whole blood. We have also demonstrated that PA11 has high PLA2 enzymatic activity (10.9 × 10(4) Units/mg), but low haemolytic activity (0.6% of red blood cells hydrolysed in the presence of 1 nM PA11). PA11 at a concentration lower than 600 nM is not cytotoxic towards human cultured cells. Chemical modification experiments using p-bromophenacyl bromide have provided evidence that the catalytic histidine of PA11 is critical for the anticoagulant activity of this PLA2. PA11 that was subjected to trypsin digestion without previous reduction and alkylation of the disulfide bonds maintained enzymatic and anticoagulant activity, suggesting that proteolysis alone cannot abolish these properties. Consistent with these results, administration of PA11 by gavage in a rabbit stasis thrombosis model increased the clotting time of recalcified citrated whole blood by a factor of four. These data suggest that PA11 has potential to be developed as an anticoagulant in a clinical setting., (Copyright © 2015. Published by Elsevier Ltd.)

Published

2016

16. Influence of Interleukin-1 Beta on Platelet-Poor Plasma Clot Formation: A Potential Impact on Early Bone Healing.

Author

Wang X, Luo Y, Masci PP, Crawford R, and Xiao Y

Subjects

Animals, Hematoma pathology, Humans, Rats, Rats, Inbred F344, Blood Coagulation, Fracture Healing, Hematoma metabolism, Interleukin-1beta metabolism

Abstract

Objectives: Hematoma quality (especially the fibrin matrix) plays an important role in the bone healing process. Here, we investigated the effect of interleukin-1 beta (IL-1β) on fibrin clot formation from platelet-poor plasma (PPP)., Methods: Five-milliliter of rat whole-blood samples were collected from the hepatic portal vein. All blood samples were firstly standardized via a thrombelastograph (TEG), blood cell count, and the measurement of fibrinogen concentration. PPP was prepared by collecting the top two-fifths of the plasma after centrifugation under 400 × g for 10 min at 20°C. The effects of IL-1β cytokines on artificial fibrin clot formation from PPP solutions were determined by scanning electronic microscopy (SEM), confocal microscopy (CM), turbidity, and clot lysis assays., Results: The lag time for protofibril formation was markedly shortened in the IL-1β treatment groups (243.8 ± 76.85 in the 50 pg/mL of IL-1β and 97.5 ± 19.36 in the 500 pg/mL of IL-1β) compared to the control group without IL-1β (543.8 ± 205.8). Maximal turbidity was observed in the control group. IL-1β (500 pg/mL) treatment significantly decreased fiber diameters resulting in smaller pore sizes and increased density of the fibrin clot structure formed from PPP (P < 0.05). The clot lysis assay revealed that 500 pg/mL IL-1β induced a lower susceptibility to dissolution due to the formation of thinner and denser fibers., Conclusion: IL-1β can significantly influence PPP fibrin clot structure, which may affect the early bone healing process.

Published

2016

17. TGFβ isoforms and receptors mRNA expression in breast tumours: prognostic value and clinical implications.

Author

Chen C, Zhao KN, Masci PP, Lakhani SR, Antonsson A, Simpson PT, and Vitetta L

Subjects

Adult, Aged, Aged, 80 and over, Biomarkers, Tumor analysis, Breast Neoplasms diagnosis, Breast Neoplasms genetics, Female, Gene Expression Regulation, Neoplastic, Humans, Prognosis, Protein Isoforms analysis, Protein Isoforms genetics, RNA, Messenger metabolism, Receptors, Transforming Growth Factor beta analysis, Receptors, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta analysis, Transforming Growth Factor beta metabolism, Breast Neoplasms metabolism, Receptors, Transforming Growth Factor beta genetics, Transforming Growth Factor beta genetics

Abstract

Background: Transforming growth factor beta (TGFβ) signalling is involved in both tumour suppression and tumour progression. The mRNA expression levels of the TGFβ isoforms and receptors in breast tumours may have prognostic value and clinical implications., Methods: The mRNA levels of TGFB1, TGFB2, TGFB3, TGFBR1 and TGFBR2 were analysed in primary breast tumours and adjacent normal breast tissues, and the associations with tumour characteristics and patients' overall and relapse-free survival were evaluated, using the public gene expression microarray data from The Cancer Genome Atlas (n = 520) and the Gene Expression Omnibus (four datasets) and our quantitative real-time PCR validation data (n = 71)., Results: Significantly higher TGFB1 and TGFB3 mRNA levels and lower TGFBR2 mRNA levels were observed in primary tumours compared with their paired normal tissues. TGFB1 mRNA expression was seemly lower in triple-negative tumours and in tumours from lymph node-negative patients. TGFB3 mRNA expression was significantly lower in estrogen receptor-negative/progesterone receptor-negative/Basal-like/Grade 3 tumours. High TGFB2, TGFB3 and TGFBR2 mRNA levels in tumours were generally associated with better prognosis for patients, especially those diagnosed with lymph node-negative diseases. High TGFBR1 mRNA levels in tumours were associated with poorer clinical outcomes for patients diagnosed with small (diameter ≤ 2 cm) tumours., Conclusions: The results indicate a reduced responsiveness of tumour cells to TGFβ, a preferential up-regulation of TGFB1 in malignant tumours and a preferential up-regulation of TGFB3 in premalignant tumours. The results may not only provide prognostic value for patients but also assist in classifying tumours according to their potential responses to TGFβ and selecting patients for TGFβ signalling pathway targeted therapies.

Published

2015

18. β-Adducin siRNA disruption of the spectrin-based cytoskeleton in differentiating keratinocytes prevented by calcium acting through calmodulin/epidermal growth factor receptor/cadherin pathway.

Author

Wu J, Masci PP, Chen C, Chen J, Lavin MF, and Zhao KN

Subjects

Animals, Cadherins metabolism, Calmodulin metabolism, Calmodulin-Binding Proteins genetics, Cell Differentiation drug effects, Cell Shape drug effects, ErbB Receptors metabolism, Gene Knockdown Techniques, Humans, Intracellular Signaling Peptides and Proteins metabolism, Keratinocytes drug effects, Keratinocytes metabolism, Keratins metabolism, Membrane Proteins metabolism, Mice, Myristoylated Alanine-Rich C Kinase Substrate, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation drug effects, Phosphotyrosine metabolism, Protein Binding drug effects, Protein Precursors metabolism, Proto-Oncogene Proteins c-akt metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Transfection, src-Family Kinases metabolism, Calcium pharmacology, Calmodulin-Binding Proteins metabolism, Cytoskeleton metabolism, Keratinocytes cytology, RNA, Small Interfering metabolism, Signal Transduction drug effects, Spectrin metabolism

Abstract

Here, we report that siRNA transfection of β-adducin significantly disrupted the spectrin-based cytoskeleton and cytoskeletal arrangements of both β-adducin and PKCδ by substantially inhibiting the expression of β-adducin, spectrin and PKCδ proteins in differentiating keratinocytes. However, extracellular Ca2+ treatment blocked the inhibitory effects of the β-adducin siRNA. Ca2+ also prevented the significant down-regulation of two differentiation markers involucrin and K1/10 and the distinct up-regulation of proliferation marker K14 in β-adducin siRNA transfected keratinocytes. In addition, β-adducin knockdown resulted in a substantial reduction of epidermal growth factor receptor (EGFR), cadherin and β-catenin and enhanced phosphorylation of EGFR on tyrosine 1173 and Ca2+ prevented these changes. Furthermore, Ca2+ blocked the inhibitory effects of β-adducin siRNA on the expression of calmodulin, phosphorylated-calmodulin (P-CaM((Tyr138))) and myristoylated alanine-rich C-kinase substrate (MARCKS) in keratinocytes. Co-immunoprecipitation studies further revealed that calmodulin, not MARCKS, strongly interacted with EGFR, cadherin and β-catenin. Our data suggest that Ca2+ plays an important role in regulating the expression and function of β-adducin to sustain normal organization of the spectrin-based cytoskeleton and the differentiation properties in keratinocytes through the calmodulin/EGFR/cadherin signaling pathway., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2015

19. Four major factors regulate phosphatidylinositol 3-kinase signaling pathway in cancers induced by infection of human papillomaviruses.

Author

Wu J, Chen J, Zhang L, Masci PP, and Zhao KN

Subjects

Animals, Cell Proliferation, Humans, Neoplasms etiology, Neoplasms pathology, Phosphatidylinositol 3-Kinases metabolism, Receptors, Growth Factor metabolism, Neoplasms metabolism, Papillomavirus Infections complications, Signal Transduction

Abstract

Epidemiological surveys and molecular studies have indicated that infection of human papillomavirus (HPV)itself is necessary but insufficient for completing transformation of the human epithelial cells in vivo to lead to different cancers. Mounting evidence exists that HPV E6/E7 oncoproteins indeed alter the cellular and molecular events in their transformed cells to induce cancers through a phosphatidylinositol 3-kinase (PI3K)/AKT/mammalian target of rapamycin (mTOR) signaling pathway. The PI3K/AKT/mTOR signaling pathway is, nonetheless, of the central importance, which tightly modulates many cellular events that occur in cells to lead them to be cancerous under the action of oncogenic factors. The cancinogenic roles of the PI3K/AKT/mTOR signaling in HPV-induced cancers are generally regulated by different upstream signaling molecules such as upstream receptor tyrosine kinases. In this article, we review that the four major upstream signaling molecules (growth factor receptor, notch receptor, Ras and PI3KCA genes) regulate PI3K/AKT/mTOR pathway to confer oncogenicity in HPV-immortalized epithelial cells and various transformed phenotypes.

Published

2014

20. Nutraceuticals and chemotherapy induced peripheral neuropathy (CIPN): a systematic review.

Author

Schloss JM, Colosimo M, Airey C, Masci PP, Linnane AW, and Vitetta L

Subjects

Acetylcarnitine therapeutic use, Acetylcysteine therapeutic use, Fatty Acids, Omega-3 therapeutic use, Glutamine therapeutic use, Glutathione therapeutic use, Humans, Peripheral Nervous System Diseases chemically induced, Randomized Controlled Trials as Topic, Thioctic Acid therapeutic use, Trace Elements therapeutic use, Vitamins therapeutic use, Antineoplastic Agents adverse effects, Dietary Supplements, Peripheral Nervous System Diseases therapy

Abstract

Chemotherapy induced peripheral neuropathy [CIPN] is a common significant and debilitating side effect resulting from the administration of neurotoxic chemotherapeutic agents. These pharmaco-chemotherapeutics can include taxanes, vinca alkaloids and others. Moderate to severe CIPN significantly decreases the quality of life and physical abilities of cancer patients and current pharmacotherapy for CIPN e.g. Amifostine and antidepressants have had limited efficacy and may themselves induce adverse side effects. To determine the potential use of nutraceuticals i.e. vitamin E, acetyl-L-carnitine, glutamine, glutathione, vitamin B6, omega-3 fatty acids, magnesium, calcium, alpha lipoic acid and n-acetyl cysteine as adjuvants in cancer treatments a systematic literature review was conducted. Revised clinical studies comprised of randomized clinical trials that investigated the anti-CIPN effect of nutraceuticals as the adjuvant intervention in patients administered chemotherapy. Twenty-four studies were assessed on methodological quality and limitations identified. Studies were mixed in their recommendations for nutraceuticals. Currently no agent has shown solid beneficial evidence to be recommended for the treatment or prophylaxis of CIPN. The standard of care for CIPN includes dose reduction and/or discontinuation of chemotherapy treatment. The management of CIPN remains an important challenge and future studies are warranted before recommendations for the use of supplements can be made., (Copyright © 2013 Elsevier Ltd and European Society for Clinical Nutrition and Metabolism. All rights reserved.)

Published

2013

21. Calcium prevents retinoic acid-induced disruption of the spectrin-based cytoskeleton in keratinocytes through the Src/PI3K-p85α/AKT/PKCδ/β-adducin pathways.

Author

Zhao KN, Masci PP, Chen J, and Lavin MF

Subjects

Animals, Calmodulin-Binding Proteins metabolism, Cells, Cultured, Class Ia Phosphatidylinositol 3-Kinase metabolism, Cyclin D2 metabolism, Gene Expression drug effects, Keratinocytes cytology, Keratinocytes drug effects, Keratinocytes metabolism, Mice, Phosphorylation drug effects, Protein Kinase C beta metabolism, Protein Kinase C-delta metabolism, Proto-Oncogene Proteins c-akt metabolism, Up-Regulation drug effects, src-Family Kinases metabolism, Calcium pharmacology, Cell Differentiation drug effects, Cytoskeleton metabolism, Signal Transduction drug effects, Spectrin metabolism, Tretinoin pharmacology

Abstract

We have previously reported that spectrin increases dramatically in amount and is assembled into the cytoskeleton in differentiating keratinocytes both in vitro and in vivo (Zhao et al., PLoS ONE 6 (12) (2011) e28267). We demonstrate here that extracellular calcium (Ca2+) enhances differentiation of keratinocytes and that this is associated with increased spectrin expression and formation of a spectrin-based cytoskeleton. While Retinoic acid (RA) also enhanced keratinocyte differentiation, it abrogated the spectrin-based cytoskeleton in keratinocytes. Furthermore, RA substantially inhibited expression of both Src and PI3K-p85α and consequently the amounts of specific phosphorylation of both of these proteins. RA also enhanced AKT expression and dramatically induced phosphorylation of AKT((Thr308)), accompanied by phosphorylation of both PKCδ((Thr505)) and β-adducin((Ser662)) and upregulated cyclin D2 and down-regulated cyclin B1. On the other hand, Ca2+ overcame the inhibitory effects of RA on expression of Src, PI3K-p85α and cyclin B1 by maintaining high levels of phosphorylation of both Src((Tyr527)) and PI3K-p85α and preventing phosphorylation of AKT((Thr308)), PKCδ((Thr505)) and β-adducin((Ser662)). These data highlight the importance of Ca2+ in both spectrin expression and the organizational integrity of the spectrin-based cytoskeleton in differentiating keratinocytes and assist in elucidating the signalling pathways involved., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

22. The structure of human microplasmin in complex with textilinin-1, an aprotinin-like inhibitor from the Australian brown snake.

Author

Millers EK, Johnson LA, Birrell GW, Masci PP, Lavin MF, de Jersey J, and Guddat LW

Subjects

Amino Acid Sequence, Animals, Aprotinin pharmacology, Crystallography, X-Ray, Elapid Venoms pharmacology, Fibrinolysin analysis, Fibrinolysin antagonists & inhibitors, Humans, Molecular Docking Simulation, Molecular Sequence Data, Peptide Fragments antagonists & inhibitors, Plasma Kallikrein antagonists & inhibitors, Protein Binding, Protein Conformation, Sequence Alignment, Snake Venoms pharmacology, Trypsin chemistry, Trypsin metabolism, Elapid Venoms chemistry, Fibrinolysin chemistry, Macromolecular Substances chemistry, Peptide Fragments chemistry, Snake Venoms chemistry

Abstract

Textilinin-1 is a Kunitz-type serine protease inhibitor from Australian brown snake venom. Its ability to potently and specifically inhibit human plasmin (K(i) = 0.44 nM) makes it a potential therapeutic drug as a systemic anti-bleeding agent. The crystal structures of the human microplasmin-textilinin-1 and the trypsin-textilinin-1 complexes have been determined to 2.78 Å and 1.64 Å resolution respectively, and show that textilinin-1 binds to trypsin in a canonical mode but to microplasmin in an atypical mode with the catalytic histidine of microplasmin rotated out of the active site. The space vacated by the histidine side-chain in this complex is partially occupied by a water molecule. In the structure of microplasminogen the χ(1) dihedral angle of the side-chain of the catalytic histidine is rotated by 67° from its "active" position in the catalytic triad, as exemplified by its location when microplasmin is bound to streptokinase. However, when textilinin-1 binds to microplasmin the χ(1) dihedral angle of this amino acid residue changes by -157° (i.e. in the opposite rotation direction compared to microplasminogen). The unusual mode of interaction between textilinin-1 and plasmin explains textilinin-1's selectivity for human plasmin over plasma kallikrein. This difference can be exploited in future drug design efforts.

Published

2013

23. Drug development from Australian elapid snake venoms and the Venomics pipeline of candidates for haemostasis: Textilinin-1 (Q8008), Haempatch™ (Q8009) and CoVase™ (V0801).

Author

Earl ST, Masci PP, de Jersey J, Lavin MF, and Dixon J

Subjects

Animals, Australia, Drug Discovery, Factor Xa pharmacology, Hemorrhage drug therapy, Hemostatics pharmacology, Humans, Antifibrinolytic Agents pharmacology, Elapid Venoms pharmacology, Elapidae, Hemostasis drug effects, Reptilian Proteins pharmacology, Serine Endopeptidases pharmacology

Abstract

Snake venoms are attractive for drug discovery and development, with a number of therapeutics derived from snake venom either in clinical use or in development. Recognising this opportunity, Australian biopharmaceutical company QRxPharma Ltd and its subsidiary Venomics Pty Ltd (VPL) has partnered with the University of Queensland (UQ) to screen and develop drug candidates from Australian elapid snake venoms. VPL has three haemostasis candidates in early preclinical development. Textilinin-1 (Q8008) is a 7 kDa potent and selective plasmin inhibitor that has application as an anti-fibrinolytic agent to reduce blood loss associated with complex surgeries. Haempatch™ (Q8009) is a Factor Xa-like protein that displays potent procoagulant effects and is being developed as a topical haemostatic agent to reduce blood loss resulting from surgery or trauma. CoVase™ (V0801) is a procoagulant cofactor that may have application as a systemic anti-bleeding agent in the treatment of internal bleeding and non-compressible haemorrhage. This review focuses on drug discovery from Australian elapid snake venoms, with emphasis on the QRxPharma/VPL drug discovery project undertaken in collaboration with UQ and candidates at further stages of development., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

24. Identification and characterisation of Kunitz-type plasma kallikrein inhibitors unique to Oxyuranus sp. snake venoms.

Author

Earl ST, Richards R, Johnson LA, Flight S, Anderson S, Liao A, de Jersey J, Masci PP, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Australia, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Fibrinolysis drug effects, Kinetics, Molecular Sequence Data, Molecular Weight, Plasma Kallikrein metabolism, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Recombinant Proteins pharmacology, Sequence Alignment, Substrate Specificity, Thrombelastography, Whole Blood Coagulation Time, Elapid Venoms chemistry, Elapidae physiology, Enzyme Inhibitors isolation & purification, Plasma Kallikrein antagonists & inhibitors

Abstract

As part of a wider study on Australian snake venom components, we have identified and characterised Kunitz-type protease inhibitors from the venoms of Oxyuranus scutellatus and Oxyuranus microlepidotus (Australian taipans) with plasma kallikrein inhibitory activity. Each inhibitor had a mass of 7 kDa and was purified from the venom as part of a protein complex. Mass spectrometry and N-terminal sequencing was employed to obtain amino acid sequence information for each inhibitor and a recombinant form of the O. scutellatus inhibitor, termed TSPI, was subsequently expressed and purified. TSPI was investigated for inhibition against a panel of 12 enzymes involved in haemostasis and estimates of the K(i) value determined for each enzyme. TSPI was found to be a broad spectrum inhibitor with most potent inhibitory activity observed against plasma kallikrein that corresponded to a K(i) of 0.057 ± 0.019 nM. TSPI also inhibited fibrinolysis in whole blood and prolonged the intrinsic clotting time. These inhibitors are also unique in that they appear to be found only in Oxyuranus sp. venoms., (Copyright © 2011. Published by Elsevier Masson SAS.)

Published

2012

25. Cloning and characterisation of novel cystatins from elapid snake venom glands.

Author

Richards R, St Pierre L, Trabi M, Johnson LA, de Jersey J, Masci PP, and Lavin MF

Subjects

Agkistrodon genetics, Agkistrodon metabolism, Amino Acid Sequence, Animals, Australia, Base Sequence, Cloning, Molecular, Cystatins biosynthesis, Cysteine Proteinase Inhibitors biosynthesis, Elapid Venoms genetics, Elapidae genetics, Elapidae metabolism, Molecular Sequence Data, Protein Isoforms chemistry, Protein Isoforms genetics, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Salivary Cystatins isolation & purification, Salivary Glands metabolism, Sequence Alignment, Cystatins chemistry, Cystatins genetics, Cysteine Proteinase Inhibitors chemistry, Cysteine Proteinase Inhibitors genetics, Elapid Venoms chemistry, Salivary Cystatins chemistry

Abstract

Snake venoms contain a complex mixture of polypeptides that modulate prey homeostatic mechanisms through highly specific and targeted interactions. In this study we have identified and characterised cystatin-like cysteine-protease inhibitors from elapid snake venoms for the first time. Novel cystatin sequences were cloned from 12 of 13 elapid snake venom glands and the protein was detected, albeit at very low levels, in a total of 22 venoms. One highly conserved isoform, which displayed close sequence identity with family 2 cystatins, was detected in each elapid snake. Crude Austrelaps superbus (Australian lowland copperhead) snake venom inhibited papain, and a recombinant form of A. superbus cystatin inhibited cathepsin L ≅ papain > cathepsin B, with no inhibition observed for calpain or legumain. While snake venom cystatins have truncated N-termini, sequence alignment and structural modelling suggested that the evolutionarily conserved Gly-11 of family 2 cystatins, essential for cysteine protease inhibition, is conserved in snake venom cystatins as Gly-3. This was confirmed by mutagenesis at the Gly-3 site, which increased the dissociation constant for papain by 10(4)-fold. These data demonstrate that elapid snake venom cystatins are novel members of the type 2 family. The widespread, low level expression of type 2 cystatins in snake venom, as well as the presence of only one highly conserved isoform in each species, imply essential housekeeping or regulatory roles for these proteins., (Copyright © 2010 Elsevier Masson SAS. All rights reserved.)

Published

2011

26. Characterisation of a mannose-binding C-type lectin from Oxyuranus scutellatus snake venom.

Author

Earl ST, Robson J, Trabi M, de Jersey J, Masci PP, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Antibodies immunology, Cloning, Molecular, DNA, Complementary genetics, Mannose-Binding Lectin genetics, Mannose-Binding Lectin isolation & purification, Models, Molecular, Molecular Sequence Data, Species Specificity, Substrate Specificity, Elapid Venoms genetics, Elapidae genetics, Mannose-Binding Lectin chemistry, Mannose-Binding Lectin metabolism

Abstract

C-type lectins are calcium-dependent sugar binding proteins and are distributed ubiquitously amongst vertebrate organisms. As part of a wider study on Australian snake venom components, we have identified and characterised a C-type lectin from the venom of Oxyuranus scutellatus (Australian coastal taipan) with mannose-binding activity. This protein exhibited a subunit molecular mass of 15 kDa and was found to bind mannose and also bind to and agglutinate erythrocytes in a Ca(2+)-dependent manner. cDNA transcripts coding for C-lectin proteins were cloned and sequenced from six Australian elapid snake species and an antibody generated against the O. scutellatus mannose-binding C-lectin identified C-lectin proteins in the venom of 13 Australian elapid snakes by immunoblotting. Experimental evidence and molecular modelling also suggest that this protein exhibits a unique dimeric structure. This is the first confirmed example of a snake venom C-lectin with mannose-binding activity., (Copyright © 2010 Elsevier Masson SAS. All rights reserved.)

Published

2011

27. Disruption of spectrin-like cytoskeleton in differentiating keratinocytes by PKCδ activation is associated with phosphorylated adducin.

Author

Zhao KN, Masci PP, and Lavin MF

Subjects

Actins chemistry, Animals, Cells, Cultured, Cytoplasm metabolism, Cytoskeleton chemistry, Genetic Techniques, Humans, Mice, Microtubules metabolism, Phosphorylation, RNA, Small Interfering metabolism, Skin metabolism, Calmodulin-Binding Proteins chemistry, Calmodulin-Binding Proteins genetics, Calmodulin-Binding Proteins metabolism, Cytoskeleton metabolism, Keratinocytes cytology, Protein Kinase C-delta metabolism, Spectrin chemistry

Abstract

Spectrin is a central component of the cytoskeletal protein network in a variety of erythroid and non-erythroid cells. In keratinocytes, this protein has been shown to be pericytoplasmic and plasma membrane associated, but its characteristics and function have not been established in these cells. Here we demonstrate that spectrin increases dramatically in amount and is assembled into the cytoskeleton during differentiation in mouse and human keratinocytes. The spectrin-like cytoskeleton was predominantly organized in the granular and cornified layers of the epidermis and disrupted by actin filament inhibitors, but not by anti-mitotic drugs. When the cytoskeleton was disrupted PKCδ was activated by phosphorylation on Thr505. Specific inhibition of PKCδ(Thr505) activation with rottlerin prevented disruption of the spectrin-like cytoskeleton and the associated morphological changes that accompany differentiation. Rottlerin also inhibited specific phosphorylation of the PKCδ substrate adducin, a cytoskeletal protein. Furthermore, knock-down of endogenous adducin affected not only expression of adducin, but also spectrin and PKCδ, and severely disrupted organization of the spectrin-like cytoskeleton and cytoskeletal distribution of both adducin and PKCδ. These results demonstrate that organization of a spectrin-like cytoskeleton is associated with keratinocytes differentiation, and disruption of this cytoskeleton is mediated by either PKCδ(Thr505) phosphorylation associated with phosphorylated adducin or due to reduction of endogenous adducin, which normally connects and stabilizes the spectrin-actin complex.

Published

2011

28. Evaluation of the Becton-Dickinson rapid serum tube: does it provide a suitable alternative to lithium heparin plasma tubes?

Author

Dimeski G, Masci PP, Trabi M, Lavin MF, and de Jersey J

Subjects

Blood Chemical Analysis, Humans, Anticoagulants chemistry, Blood Specimen Collection instrumentation, Heparin chemistry, Lithium chemistry

Abstract

Background: Obtaining a suitable specimen for analysis in a timely manner is pivotal in clinical chemistry service provision. Serum is recognized as the preferred specimen for most assays, but because of time constraints for completion of clotting and an increasing number of patients on anti-coagulant therapy, latent clotting or no clotting is an outcome which can lead to errors and delay in delivery of critical results. Although lithium heparin plasma has unique problems, it has become an alternative in hospital-based laboratories., Methods: The Becton-Dickinson (BD) rapid serum tube (RST) was evaluated in a hospital environment using a total of 53 participants, both healthy and anticoagulated, for 31 analytes against BD PST II and BD SST II tubes measured with Beckman DxC800 and DxI800 analyzers., Results: Most results from the RST tube were comparable with those from the SST II tube. Potassium results were closer to the PST II plasma concentrations. Incomplete and latent clotting was encountered in the RST specimens from participants (cardiac and dialysis) who had received a total of >7000 units of heparin [activated partial thromboplastin time (APTT) >150 s], warfarin/heparin combination, and specimens from cardiac surgery patients who had received a total of >25,000 units of heparin (APTT >200 s) at the time of collection of specimens., Conclusions: The RST tube provides a suitable alternative to lithium heparin plasma tubes for most patients in a hospital environment. However, latent clotting continued to occur in specimens collected from participants who had received high concentrations of anticoagulants.

Published

2010

29. Altered clot kinetics in patients with non-alcoholic fatty liver disease.

Author

Hickman IJ, Sullivan CM, Flight S, Campbell C, Crawford DH, Masci PP, O'Moore-Sullivan TM, Prins JB, and Macdonald GA

Subjects

Adult, Biopsy, Body Mass Index, Case-Control Studies, Female, Homeostasis physiology, Humans, Liver pathology, Male, Metabolic Syndrome physiopathology, Middle Aged, Obesity physiopathology, Risk Factors, Thrombelastography, Blood Coagulation physiology, Cardiovascular Diseases epidemiology, Fatty Liver blood, Fatty Liver complications

Abstract

Background: Emerging evidence has linked the presence of non-alcoholic fatty liver disease (NAFLD) with an increased risk for cardiovascular events. We hypothesised that altered clot kinetics and platelet function may contribute to this increased risk. This study compared whole blood clotting kinetics in patients with 1) non-cirrhotic NAFLD (n = 28) and 2) healthy control subjects (n = 22)., Methods: Clotting kinetics were assessed in whole blood using thromboelastography (TEG) and assessed for correlations with cardiovascular risk factors., Results: Clot kinetics in patients with NAFLD showed significantly stronger clot development (maximum amplitude (MA); 58.3 +/- 6.3 mm vs. 52.0 +/- 10.1 mm, p = 0.01) and reduced clot lysis in the presence of thrombin (35 +/- 30% vs. 51 +/- 26% clot lysis 30 minutes after MA, p = 0.03) compared to control subjects. Clot strength was independently positively associated with body mass index in NAFLD, but not in control subjects. There was a greater platelet contribution to clot strength in patients with NAFLD compared to controls despite similar platelet counts. There was no association between clot kinetics and features of the metabolic syndrome or presence of type 2 diabetes., Conclusion: Patients with NAFLD have disturbances in ex-vivo clot kinetics including increased clot strength and clots that are more resistant to thrombin-stimulated lysis.

Published

2009

30. Prothrombinase complexes with different physiological roles.

Author

Lavin MF and Masci PP

Subjects

Animals, Anticoagulants chemistry, Evolution, Molecular, Factor V chemistry, Factor X chemistry, Humans, Models, Biological, Protein C chemistry, Protein Isoforms, Protein Structure, Tertiary, Recombinant Proteins chemistry, Snake Venoms, Snakes, Thromboplastin chemistry

Published

2009

31. Venom factor V from the common brown snake escapes hemostatic regulation through procoagulant adaptations.

Author

Bos MH, Boltz M, St Pierre L, Masci PP, de Jersey J, Lavin MF, and Camire RM

Subjects

Animals, Factor V chemistry, Factor Xa, Hemostasis, Humans, Protein Stability, Sequence Alignment, Snakes, Blood Coagulation, Factor V physiology, Snake Venoms enzymology, Thromboplastin chemistry

Abstract

Venomous snakes produce an array of toxic compounds, including procoagulants to defend themselves and incapacitate prey. The Australian snake Pseudonaja textilis has a venom-derived prothrombin activator homologous to coagulation factors V (FV) and Xa (FXa). Here we show that the FV component (pt-FV) has unique biologic properties that subvert the normal regulatory restraints intended to restrict an unregulated procoagulant response. Unlike human FV, recombinant pt-FV is constitutively active and does not require proteolytic processing to function. Sequence comparisons show that it has shed a large portion of the central B-domain, including residues that stabilize the inactive procofactor state. Remarkably, pt-FV functions in the absence of anionic membranes as it binds snake-FXa with high affinity in solution. Furthermore, despite cleavage in the heavy chain, pt-FV is functionally resistant to activated protein C, an anticoagulant. We speculate this stability is the result of noncovalent interactions and/or a unique disulfide bond in pt-FV linking the heavy and light chains. Taken together, these findings provide a biochemical rationale for the strong procoagulant nature of venom prothrombinase. Furthermore, they illustrate how regulatory mechanisms designed to limit the hemostatic response can be uncoupled to provide a sustained, disseminated procoagulant stimulus for use as a biologic toxin.

Published

2009

32. Crystal structure of textilinin-1, a Kunitz-type serine protease inhibitor from the venom of the Australian common brown snake (Pseudonaja textilis).

Author

Millers EK, Trabi M, Masci PP, Lavin MF, de Jersey J, and Guddat LW

Subjects

Amino Acid Sequence, Animals, Australia, Binding Sites, Crystallography, X-Ray, Elapid Venoms genetics, Elapid Venoms isolation & purification, Fibrinolysin antagonists & inhibitors, Models, Molecular, Molecular Sequence Data, Protein Structure, Secondary, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Serine Proteinase Inhibitors isolation & purification, Elapid Venoms chemistry, Elapidae metabolism, Serine Proteinase Inhibitors chemistry

Abstract

Textilinin-1 is a Kunitz-type serine protease inhibitor isolated from the venom of the Australian common brown snake, Pseudonaja textilis. This molecule binds to and blocks the activity of a range of serine proteases, including plasmin and trypsin. Textilinin-1's ability to inhibit plasmin, a protease involved in fibrinolysis, has raised the possibility that it could be used as an alternative to aprotinin (Trasylol) as a systemic antibleeding agent in surgery. Here, the crystal structure of free recombinant textilinin-1 has been determined to 1.63 A, with three molecules observed in the asymmetric unit. All of these have a similar overall fold to aprotinin, except that the canonical loop for one of the molecules is inverted such that the side chain of the P1' residue, Val18, is partially buried by intramolecular contacts to Pro15, Thr13, and Ile36. In aprotinin, the P1' residue is Ala16, whose side chain is too small to form similar contacts. The loop inversion in textilinin-1 is facilitated by changes in backbone dihedral angles for the P1 and P2' residues, such that they alternate between values in the beta-sheet and alpha-helical regions of the Ramachandran plot. In a comparison with the structures of all other known Kunitz-type serine protease inhibitors, no such conformational variability has been observed. The presence of the bulkier valine as the P1' residue in textilinin-1 appears to be a major contributor to reducing the binding affinity for plasmin as compared to aprotinin (3.5 nm versus 0.053 nm) and could also account for an observed narrower binding specificity.

Published

2009

33. Textilinin-1, an alternative anti-bleeding agent to aprotinin: Importance of plasmin inhibition in controlling blood loss.

Author

Flight SM, Johnson LA, Du QS, Warner RL, Trabi M, Gaffney PJ, Lavin MF, de Jersey J, and Masci PP

Subjects

Analysis of Variance, Animals, Fibrinolysis drug effects, Hemostasis, Mice, Time Factors, Aprotinin therapeutic use, Blood Loss, Surgical prevention & control, Elapid Venoms therapeutic use, Fibrinolysin antagonists & inhibitors, Serine Proteinase Inhibitors therapeutic use

Abstract

Aprotinin has been used widely in surgery as an anti-bleeding agent but is associated with a number of side effects. We report that textilinin-1, a serine protease inhibitor from Pseudonaja textilis venom with sequence relatedness to aprotinin, is a potent but reversible plasmin inhibitor and has a narrower range of protease inhibition compared to aprotinin. Like aprotinin, textilinin-1 at 5 micromol/l gave almost complete inhibition of tissue plasminogen activator-induced fibrinolysis of whole blood clots. The activated partial thromboplastin time for plasma was markedly increased by aprotinin but unaffected by textilinin-1. In a mouse tail-vein bleeding model, intravenous textilinin-1 and aprotinin caused similar decreases in blood loss but time to haemostasis in the textilinin-treated animals was significantly shorter than in aprotinin-treated mice. Based on these data, textilinin-1 merits further investigation as a therapeutic alternative to aprotinin.

Published

2009

34. Common evolution of waprin and kunitz-like toxin families in Australian venomous snakes.

Author

St Pierre L, Earl ST, Filippovich I, Sorokina N, Masci PP, De Jersey J, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Australia, Base Sequence, DNA, Complementary genetics, Elapid Venoms chemistry, Genome, Immunoblotting, Molecular Sequence Data, Peptides chemistry, Sequence Alignment, Elapid Venoms genetics, Evolution, Molecular, Peptides genetics, Protease Inhibitors chemistry

Abstract

The venoms of Australian snakes contain a myriad of pharmacologically active toxin components. This study describes the identification and comparative analysis of two distinct toxin families, the kunitztype serine protease inhibitors and waprins, and demonstrates a previously unknown evolutionary link between the two. Multiple cDNA and full-length gene isoforms were cloned and shown to be composed of three exons separated by two introns. A high degree of identity was observed solely within the first exon which coded for the propeptide sequence and its cleavage site, and indicates that each toxin family has arisen from a gene duplication event followed by diversification only within the portion of the gene coding for the functional toxin. It is proposed that while the mechanism of toxin secretion is highly conserved, diversification of mature toxin sequences allows for the existence of multiple protein isoforms in the venom to adapt to variations within the prey environment.

Published

2008

35. Distinct activities of novel neurotoxins from Australian venomous snakes for nicotinic acetylcholine receptors.

Author

St Pierre L, Fischer H, Adams DJ, Schenning M, Lavidis N, de Jersey J, Masci PP, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Australia, Base Sequence, Bufo marinus, DNA Primers genetics, DNA, Complementary genetics, Elapid Venoms genetics, Elapid Venoms isolation & purification, Elapidae genetics, Electrophysiology, In Vitro Techniques, Molecular Sequence Data, Neurotoxins genetics, Neurotoxins isolation & purification, Nicotinic Antagonists isolation & purification, Nicotinic Antagonists toxicity, Receptors, Nicotinic metabolism, Recombinant Proteins genetics, Recombinant Proteins toxicity, Sequence Homology, Amino Acid, Elapid Venoms toxicity, Neurotoxins toxicity, Receptors, Nicotinic drug effects

Abstract

Envenomation from Australian elapid snakes results in a myriad of neurological effects due to post-synaptic neurotoxins that bind and inhibit nicotinic acetylcholine receptors (nAChRs) of neurons and muscle fibres. However, despite the significant physiological effects of these toxins, they have remained largely undercharacterised at the molecular level. This study describes the identification and comparative analysis of multiple neurotoxin isoforms from ten Australian snakes, including functional characterisation of two of these isoforms, Os SNTX-1 from Oxyuranus scutellatus and the more potent Pt LNTX-1 from Pseudonaja textilis. Electrophysiological recordings from adrenal chromaffin cells demonstrate that both neurotoxins act as competitive antagonists of nAChRs in a concentration-dependent manner. Their effects upon spontaneous and nerve-evoked membrane responses at the amphibian neuromuscular junction provide further evidence that both toxins bind muscle nAChRs in an irreversible manner. This study represents one of the most comprehensive descriptions to date of the sequences and activity of individual Australian elapid neurotoxins.

Published

2007

36. Diversity of toxic components from the venom of the evolutionarily distinct black whip snake, Demansia vestigiata.

Author

St Pierre L, Birrell GW, Earl ST, Wallis TP, Gorman JJ, de Jersey J, Masci PP, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Molecular Sequence Data, Proteome metabolism, Species Specificity, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Evolution, Molecular, Reptilian Proteins analysis, Snake Venoms analysis, Snakes metabolism

Abstract

Included among the more than 300 species of elapid snakes worldwide is the Australian genus Demansia, or whip snakes. Despite evidence to suggest adverse clinical outcomes from envenomation by these snakes, together with confusion on their true phylogenetic relationship to other Australian elapids, not a single toxin sequence has previously been reported from the venom of a Demansia species. We describe here a combined proteomic and transcriptomic approach characterizing the venom from the black whip snake, Demansia vestigiata. A total of 13 distinct toxin families were identified, including homologues of all of the major toxic components previously reported from the venom of other Australian elapids, such as factor X-like prothrombin activators, neurotoxins, phospholipases, cysteine rich secretory proteins, textilinin-like molecules, nerve growth factors, l-amino acid oxidases, vespryns, 5' nucleotidases, metalloproteinases, and C-type lectins as well as a novel dipeptidyl peptidase family. Phylogenetic analysis of these sequences revealed an early evolutionary split of the black whip snake from all other characterized Australian snakes, with a low degree of sequence identity between D. vestigiata and the other snakes, across all toxin families. The results of this study have important implications not only for the further characterization of venom from whip snakes, but also for our understanding of the evolutionary relationship of Australian snake species.

Published

2007

37. The diversity of bioactive proteins in Australian snake venoms.

Author

Birrell GW, Earl ST, Wallis TP, Masci PP, de Jersey J, Gorman JJ, and Lavin MF

Subjects

Animals, Australia, Electrophoresis, Gel, Two-Dimensional, Glycosylation, Lectins metabolism, Mass Spectrometry, Phosphorylation, Protein Binding, Protein Processing, Post-Translational, Reptilian Proteins chemistry, Reptilian Proteins isolation & purification, Elapid Venoms chemistry, Reptilian Proteins analysis

Abstract

Australian elapid snakes are among the most venomous in the world. Their venoms contain multiple components that target blood hemostasis, neuromuscular signaling, and the cardiovascular system. We describe here a comprehensive approach to separation and identification of the venom proteins from 18 of these snake species, representing nine genera. The venom protein components were separated by two-dimensional PAGE and identified using mass spectrometry and de novo peptide sequencing. The venoms are complex mixtures showing up to 200 protein spots varying in size from <7 to over 150 kDa and in pI from 3 to >10. These include many proteins identified previously in Australian snake venoms, homologs identified in other snake species, and some novel proteins. In many cases multiple trains of spots were typically observed in the higher molecular mass range (>20 kDa) (indicative of post-translational modification). Venom proteins and their post-translational modifications were characterized using specific antibodies, phosphoprotein- and glycoprotein-specific stains, enzymatic digestion, lectin binding, and antivenom reactivity. In the lower molecular weight range, several proteins were identified, but the predominant species were phospholipase A2 and alpha-neurotoxins, both represented by different sequence variants. The higher molecular weight range contained proteases, nucleotidases, oxidases, and homologs of mammalian coagulation factors. This information together with the identification of several novel proteins (metalloproteinases, vespryns, phospholipase A2 inhibitors, protein-disulfide isomerase, 5'-nucleotidases, cysteine-rich secreted proteins, C-type lectins, and acetylcholinesterases) aids in understanding the lethal mechanisms of elapid snake venoms and represents a valuable resource for future development of novel human therapeutics.

Published

2007

38. Surfactant protein expression in human skin: evidence and implications.

Author

Mo YK, Kankavi O, Masci PP, Mellick GD, Whitehouse MW, Boyle GM, Parsons PG, Roberts MS, and Cross SE

Subjects

Aged, 80 and over, Cells, Cultured, DNA, Complementary metabolism, Female, Fetus metabolism, Fibroblasts metabolism, Humans, Immunohistochemistry, Infant, Newborn, Keratinocytes metabolism, Male, Melanocytes metabolism, Pulmonary Surfactant-Associated Protein A metabolism, Pulmonary Surfactant-Associated Protein B metabolism, Pulmonary Surfactant-Associated Protein C metabolism, Pulmonary Surfactant-Associated Protein D metabolism, Pulmonary Surfactant-Associated Proteins genetics, Pulmonary Surfactant-Associated Proteins pharmacology, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Sebum chemistry, Sebum drug effects, Skin cytology, Skin embryology, Surface Tension, Pulmonary Surfactant-Associated Proteins metabolism, Skin metabolism

Abstract

The presence of surfactant proteins (SPs), critical to local barrier and defense functions and usually associated with the lung, was revealed in adult and fetal human skin complementary deoxyribonucleic acid, in skin samples from three adult female donors and also in cultured fibroblasts, keratinocytes, and melanocytes. Using reverse transcription-PCR, SP-A, SP-B, SP-C, and SP-D messenger ribonucleic acid expression was detected to varying extents in the different skin sources. The stronger expression of SP-C in fetal skin, compared to adult skin, suggested that the role of this protein alters with age. Immunohistochemical studies showed variable distribution of SPs in human epidermis and dermis, confirming that these proteins are indeed translated and expressed in skin tissue. In vitro studies showed that the surface tension of SP-deficient artificial sebum is (a) lowered by skin-extracted SP-B and (b) further reduced to a level comparable to normal sebum by the additional presence of skin-extracted SP-A and SP-D, consistent with their surface tension-lowering capabilities in lung. The possible roles of SPs in skin, based on their known functions in the lung are discussed. However, their potential as therapeutic targets or diagnostic markers of skin disease remains to be elucidated.

Published

2007

39. Cloning and characterisation of natriuretic peptides from the venom glands of Australian elapids.

Author

St Pierre L, Flight S, Masci PP, Hanchard KJ, Lewis RJ, Alewood PF, de Jersey J, and Lavin MF

Subjects

Amino Acid Sequence, Angiotensin-Converting Enzyme Inhibitors pharmacology, Animals, Cell Line, Cloning, Molecular, Cyclic GMP metabolism, DNA, Complementary chemistry, DNA, Complementary genetics, Dose-Response Relationship, Drug, Elapid Venoms metabolism, Elapid Venoms pharmacology, Electrophoresis, Polyacrylamide Gel, Humans, Molecular Sequence Data, Natriuretic Peptides metabolism, Natriuretic Peptides pharmacology, Peptidyl-Dipeptidase A metabolism, Platelet Aggregation drug effects, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Recombinant Proteins pharmacology, Sequence Alignment, Sequence Analysis, DNA, Elapid Venoms genetics, Elapidae genetics, Natriuretic Peptides genetics

Abstract

The venom from Australian elapid snakes contains a complex mixture of polypeptide toxins that adversely affect multiple homeostatic systems within their prey in a highly specific and targeted manner. Included in these toxin families are the recently described venom natriuretic peptides, which display similar structure and vasoactive functions to mammalian natriuretic peptides. This paper describes the identification and detailed comparative analysis of the cDNA transcripts coding for the mature natriuretic peptide from a total of nine Australian elapid snake species. Multiple isoforms were identified in a number of species and represent the first description of a natriuretic peptide from the venom gland for most of these snakes. Two distinct natriuretic peptide isoforms were selected from the common brown snake (Pseudonaja textilis), PtNP-a, and the mulga (Pseudechis australis), PaNP-c, for recombinant protein expression and functional analysis. Only one of these peptides, PtNP-a, displayed cGMP stimulation indicative of normal natriuretic peptide activity. Interestingly, both recombinant peptides demonstrated a dose-dependent inhibition of angiotensin converting enzyme (ACE) activity, which is predictive of the vasoactive effects of the toxin. The natriuretic peptides, however, did not possess any coagulopathic activity, nor did they inhibit or potentiate thrombin, adenosine diphosphate or arachidonic acid induced platelet aggregation. The data presented in this study represent a significant resource for understanding the role of various natriuretic peptides isoforms during the envenomation process by Australian elapid snakes.

Published

2006

40. Post-translational modification accounts for the presence of varied forms of nerve growth factor in Australian elapid snake venoms.

Author

Earl ST, Birrell GW, Wallis TP, St Pierre LD, Masci PP, de Jersey J, Gorman JJ, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Australia, Base Sequence, Biological Assay, Cloning, Molecular, DNA, Complementary genetics, Elapid Venoms genetics, Elapidae genetics, Elapidae metabolism, Electrophoresis, Gel, Two-Dimensional, Glycosylation, Molecular Sequence Data, Nerve Growth Factor genetics, PC12 Cells, Protein Processing, Post-Translational, Proteomics, Rats, Sequence Homology, Amino Acid, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Tandem Mass Spectrometry, Elapid Venoms chemistry, Elapid Venoms metabolism, Nerve Growth Factor chemistry, Nerve Growth Factor metabolism

Abstract

The Australian elapid snakes are amongst the most venomous snakes in the world, but much less is known about the overall venom composition in comparison to Asian and American snakes. We have used a combined approach of cDNA cloning and 2-DE with MS to identify nerve growth factor (NGF) in venoms of the Australian elapid snakes and demonstrate its neurite outgrowth activity. While a single 730 nucleotide ORF, coding for a 243 amino acid precursor protein was detected in all snakes, use of 2-DE identified NGF proteins with considerable variation in molecular size within and between the different snakes. The variation in size can be explained at least in part by N-linked glycosylation. It is possible that these modifications alter the stability, activity and other characteristics of the snake NGFs. Further characterisation is necessary to delineate the function of the individual NGF isoforms.

Published

2006

41. Crystallization and preliminary X-ray analysis of a Kunitz-type inhibitor, textilinin-1 from Pseudonaja textilis textilis.

Author

Millers EK, Masci PP, Lavin MF, de Jersey J, and Guddat LW

Subjects

Amino Acid Sequence, Animals, Cattle, Crystallization, Crystallography, X-Ray, Elapid Venoms isolation & purification, Elapidae, Fibrinolysin antagonists & inhibitors, Sequence Homology, Amino Acid, Trypsin chemistry, Trypsin isolation & purification, X-Ray Diffraction, Aprotinin chemistry, Elapid Venoms chemistry

Abstract

Textilinin-1 (Txln-1), a Kunitz-type serine protease inhibitor, is a 59-amino-acid polypeptide isolated from the venom of the Australian Common Brown snake Pseudonaja textilis textilis. This molecule has been suggested as an alternative to aprotinin, also a Kunitz-type serine protease inhibitor, for use as an anti-bleeding agent in surgical procedures. Txln-1 shares only 47% amino-acid identity to aprotinin; however, six cysteine residues in the two peptides are in conserved locations. It is therefore expected that the overall fold of these molecules is similar but that they have contrasting surface features. Here, the crystallization of recombinant textilinin-1 (rTxln-1) as the free molecule and in complex with bovine trypsin (229 amino acids) is reported. Two organic solvents, phenol and 1,4-butanediol, were used as additives to facilitate the crystallization of free rTxln-1. Crystals of the rTxln-1-bovine trypsin complex diffracted to 2.0 angstroms resolution, while crystals of free rTxln-1 diffracted to 1.63 angstroms resolution.

Published

2006

42. Resistance of porcine blood clots to lysis relates to poor activation of porcine plasminogen by tissue plasminogen activator.

Author

Flight SM, Masci PP, Lavin MF, and Gaffney PJ

Subjects

Animals, Enzyme Activation drug effects, Enzyme Activation physiology, Fibrinolytic Agents metabolism, Humans, Models, Animal, Plasminogen metabolism, Recombinant Proteins pharmacology, Serum Globulins chemistry, Serum Globulins metabolism, Swine, Thrombelastography, Tissue Plasminogen Activator pharmacology, Fibrinolysis drug effects, Fibrinolytic Agents pharmacology, Thrombosis prevention & control, Tissue Plasminogen Activator therapeutic use

Abstract

In-vitro experimentation was performed on porcine and human blood to determine their comparative responsiveness to a novel fibrinolytic inhibitor and thereby assess whether the pig is a suitable animal model for subsequent in-vivo testing of this inhibitor. Thromboelastography showed the clots formed from porcine whole blood to be highly resistant to tissue plasminogen activator (t-PA)-catalyzed lysis, and this communication offers the resistance of porcine plasminogen to activation by t-PA as an explanation. Porcine blood containing 100 and 1500 IU/ml added t-PA lysed very slowly, having LY30 values of 1.9 +/- 1.4 and 2.9 +/- 1.9%, respectively. In contrast, the LY30 values for the human clots containing 100 and 1500 IU/ml t-PA were 77.1 +/- 6.3 and 93.3 +/- 1.3%, respectively. Moreover, purified porcine plasminogen was activated very slowly by added t-PA in the presence of both human and porcine fibrin. Activation of plasminogen by the endogenous activators, as measured by the euglobulin clot lysis time, was greatly prolonged for the pig (22 +/- 3 h) compared with the human (3.5 +/- 1.5 h). These results suggest caution in using the pig as an experimental model when studying the effects of various agents on fibrinolysis.

Published

2006

43. Comparison of active venom components between Eastern brown snakes collected from South Australia and Queensland.

Author

Flight S, Mirtschin P, and Masci PP

Subjects

Animals, Elapid Venoms analysis, Factor Xa metabolism, Humans, Queensland, South Australia, Species Specificity, Blood Coagulation drug effects, Elapid Venoms pharmacology, Elapidae, Fibrinolysin antagonists & inhibitors

Abstract

The abundance and activity of the prothrombin activator (pseutarin C) within the venom of the Eastern brown snake (Pseudonaja textilis textilis) is the primary determinant of its coagulation potency. Textilinin-1, also in this venom, is a plasmin inhibitor which is thought to exert its toxic effects through the slowing of fibrinolysis. The aim of this report is to determine if there are differences in the potency of the venom from Eastern brown snakes collected from South Australia (SA) compared to those from Queensland (QLD). A concentration of 0.4 microg/ml venom protein from six QLD specimens clotted citrated plasma in an average time of 21.4+/-3.3 s compared to 68.7+/-2.4 s for the same amount of SA venom (averaged for six individuals). The more potent procoagulant activity of the QLD venom was measured between 0.4 and 94 microg/ml venom protein in plasma. The anti-plasmin activity of textilinin was also greater in the venom of the snakes collected from QLD, causing full inhibition of plasmin at approximately 1.88 microg/ml of venom protein compared to approximately 7.5 microg/ml for the SA venoms. It is concluded that geographic differentiation of the Eastern brown snakes results in significant differences venom potency.

Published

2006

44. Molecular diversity in venom from the Australian Brown snake, Pseudonaja textilis.

Author

Birrell GW, Earl S, Masci PP, de Jersey J, Wallis TP, Gorman JJ, and Lavin MF

Subjects

Animals, Australia, Electrophoresis, Gel, Two-Dimensional, Geography, Glycosylation, Immunoblotting, Lectins metabolism, Mass Spectrometry, Protein Binding, Elapid Venoms chemistry, Elapidae, Reptilian Proteins analysis, Reptilian Proteins chemistry

Abstract

Venom from the Australian elapid Pseudonaja textilis (Common or Eastern Brown snake), is the second most toxic snake venom known and is the most common cause of death from snake bite in Australia. This venom is known to contain a prothrombin activator complex, serine proteinase inhibitors, various phospholipase A2s, and pre- and postsynaptic neurotoxins. In this study, we performed a proteomic identification of the venom using two-dimensional gel electrophoresis, mass spectrometry, and de novo peptide sequencing. We identified most of the venom proteins including proteins previously not known to be present in the venom. In addition, we used immunoblotting and post-translational modification-specific enzyme stains and antibodies that reveal the complexity and regional diversity of the venom. Modifications observed include phosphorylation, gamma-carboxylation, and glycosylation. Glycoproteins were further characterized by enzymatic deglycosylation and by lectin binding specificity. The venom contains an abundance of glycoproteins with N-linked sugars that include glucose/mannose, N-acetylgalactosamine, N-acetylglucosamine, and sialic acids. Additionally there are multiple isoforms of mammalian coagulation factors that comprise a significant proportion of the venom. Indeed two of the identified proteins, a procoagulant and a plasmin inhibitor, are currently in development as human therapeutic agents.

Published

2006

45. Identification and analysis of venom gland-specific genes from the coastal taipan (Oxyuranus scutellatus) and related species.

Author

St Pierre L, Woods R, Earl S, Masci PP, and Lavin MF

Subjects

Amino Acid Oxidoreductases genetics, Amino Acid Sequence, Animals, Crotalid Venoms genetics, DNA, Complementary, Elapid Venoms metabolism, Elapidae metabolism, Gene Expression Profiling, Molecular Sequence Data, Oligonucleotide Array Sequence Analysis, Phospholipases A genetics, Phospholipases A metabolism, Phylogeny, RNA, Messenger metabolism, Sequence Alignment, Snake Venoms genetics, Elapid Venoms genetics, Elapidae genetics

Abstract

Australian terrestrial elapid snakes contain amongst the most potently toxic venoms known. However, despite the well-documented clinical effects of snake bite, little research has focussed on individual venom components at the molecular level. To further characterise the components of Australian elapid venoms, a complementary (cDNA) microarray was produced from the venom gland of the coastal taipan (Oxyuranus scutellatus) and subsequently screened for venom gland-specific transcripts. A number of putative toxin genes were identified, including neurotoxins, phospholipases, a pseudechetoxin-like gene, a venom natriuretic peptide and a nerve growth factor together with other genes involved in cellular maintenance. Venom gland-specific components also included a calglandulin-like protein implicated in the secretion of toxins from the gland into the venom. These toxin transcripts were subsequently identified in seven other related snake species, producing a detailed comparative analysis at the cDNA and protein levels. This study represents the most detailed description to date of the cloning and characterisation of different genes associated with envenomation from Australian snakes.

Published

2005

46. Cloning and functional expression of venom prothrombin activator protease from Pseudonaja textilis with whole blood procoagulant activity.

Author

Filippovich I, Sorokina N, St Pierre L, Flight S, de Jersey J, Perry N, Masci PP, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blood Coagulation Factors metabolism, Blood Coagulation Tests, CHO Cells, Cloning, Molecular, Cricetinae, Elapid Venoms metabolism, Enzyme Activation, Factor X genetics, Humans, Molecular Sequence Data, Peptide Hydrolases metabolism, Recombinant Fusion Proteins metabolism, Sequence Alignment, Sheep, Blood Coagulation, Blood Coagulation Factors genetics, Elapid Venoms genetics, Elapidae, Peptide Hydrolases genetics, Prothrombin, Serine Endopeptidases genetics

Abstract

The snake venom group C prothrombin activators contain a number of components that enhance the rate of prothrombin activation. The cloning and expression of full-length cDNA for one of these components, an activated factor X (factor Xa)-like protease from Pseudonaja textilis as well as the generation of functional chimeric constructs with procoagulant activity were described. The complete cDNA codes for a propeptide, light chain, activation peptide (AP) and heavy chain related in sequence to mammalian factor X. Efficient expression of the protease was achieved with constructs where the AP was deleted and the cleavage sites between the heavy and light chains modified, or where the AP was replaced with a peptide involved in insulin receptor processing. In human kidney cells (H293F) transfected with these constructs, up to 80% of the pro-form was processed to heavy and light chains. Binding of the protease to barium citrate and use of specific antibodies demonstrated that gamma-carboxylation of glutamic acid residues had occurred on the light chain in both cases, as observed in human factor Xa and the native P. textilis protease. The recombinant protease caused efficient coagulation of whole citrated blood and citrated plasma that was enhanced by the presence of Ca2+. This study identified the complete cDNA sequence of a factor Xa-like protease from P. textilis and demonstrated for the first time the expression of a recombinant form of P. textilis protease capable of blood coagulation.

Published

2005

47. Comparative analysis of prothrombin activators from the venom of Australian elapids.

Author

St Pierre L, Masci PP, Filippovich I, Sorokina N, Marsh N, Miller DJ, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Australia, DNA, Complementary, Elapid Venoms chemistry, Elapidae classification, Enzyme Activation, Factor Va isolation & purification, Factor Xa isolation & purification, Gene Amplification, Molecular Sequence Data, Prothrombin metabolism, Prothrombin Time, Sequence Alignment, Elapid Venoms pharmacology, Elapidae genetics, Factor Va genetics, Factor Xa genetics, Phylogeny, Prothrombin genetics

Abstract

A key component of the venom of many Australian snakes belonging to the elapid family is a toxin that is structurally and functionally similar to that of the mammalian prothrombinase complex. In mammals, this complex is responsible for the cleavage of prothrombin to thrombin and is composed of factor Xa in association with its cofactors calcium, phospholipids, and factor Va. The snake prothrombin activators have been classified on the basis of their requirement for cofactors for activity. The two major subgroups described in Australian elapid snakes, groups C and D, are differentiated by their requirement for mammalian coagulation factor Va. In this study, we describe the cloning, characterization, and comparative analysis of the factor X- and factor V-like components of the prothrombin activators from the venom glands of snakes possessing either group C or D prothrombin activators. The overall domain arrangement in these proteins was highly conserved between all elapids and with the corresponding mammalian clotting factors. The deduced protein sequence for the factor X-like protease precursor, identified in elapids containing either group C or D prothrombin activators, demonstrated a remarkable degree of relatedness to each other (80%-97%). The factor V-like component of the prothrombin activator, present only in snakes containing group C complexes, also showed a very high degree of homology (96%-98%). Expression of both the factor X- and factor V-like proteins determined by immunoblotting provided an additional means of separating these two groups at the molecular level. The molecular phylogenetic analysis described here represents a new approach for distinguishing group C and D snake prothrombin activators and correlates well with previous classifications.

Published

2005

48. Increased platelet-derived microparticles in the coronary circulation of percutaneous transluminal coronary angioplasty patients.

Author

Craft JA, Masci PP, Roberts MS, Brighton TA, Garrahy P, Cox S, and Marsh NA

Subjects

Antithrombin III analysis, Cardiovascular Agents therapeutic use, Combined Modality Therapy, Coronary Circulation, Coronary Restenosis etiology, Coronary Stenosis drug therapy, Coronary Stenosis therapy, Coronary Vessels, Female, Humans, Integrin beta3 analysis, L-Lactate Dehydrogenase blood, Leukocyte Count, Male, Middle Aged, Particle Size, Peptide Hydrolases analysis, Platelet Adhesiveness, Platelet Count, Stents, Thromboxane B2 blood, Angioplasty, Balloon, Coronary, Blood Platelets ultrastructure, Coronary Stenosis blood

Abstract

Platelet-derived microparticles that are produced during platelet activation are capable of adhesion and aggregation. Endothelial trauma that occurs during percutaneous transluminal coronary angioplasty (PTCA) may support platelet-derived microparticle adhesion and contribute to development of restenosis. We have previously reported an increase in platelet-derived microparticles in peripheral arterial blood with angioplasty. This finding raised concerns regarding the role of platelet-derived microparticles in restenosis, and therefore the aim of this study was to monitor levels in the coronary circulation. The study population consisted of 19 angioplasty patients. Paired coronary artery and sinus samples were obtained following heparinization, following contrast administration, and subsequent to all vessel manipulation. Platelet-derived microparticles were identified with an anti-CD61 (glycoprotein IIIa) fluorescence-conjugated antibody using flow cytometry. There was a significant decrease in arterial platelet-derived microparticles from heparinization to contrast administration (P = 0.001), followed by a significant increase to the end of angioplasty (P = 0.004). However, there was no significant change throughout the venous samples. These results indicate that the higher level of platelet-derived microparticles after angioplasty in arterial blood remained in the coronary circulation. Interestingly, levels of thrombin-antithrombin complexes did not rise during PTCA. This may have implications for the development of coronary restenosis post-PTCA, although this remains to be determined.

Published

2004

49. Fatty acid binding protein is a major determinant of hepatic pharmacokinetics of palmitate and its metabolites.

Author

Hung DY, Burczynski FJ, Chang P, Lewis A, Masci PP, Siebert GA, Anissimov YG, and Roberts MS

Subjects

Albumins metabolism, Algorithms, Animals, Biomarkers, Biotransformation, Clofibrate pharmacology, Cytochrome P-450 Enzyme System metabolism, Cytoplasm metabolism, Diffusion, Fatty Acid-Binding Protein 7, Fatty Acid-Binding Proteins, Glutathione metabolism, Hypolipidemic Agents pharmacology, In Vitro Techniques, Male, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Perfusion, Proteins metabolism, Rats, Rats, Wistar, Tissue Distribution, Carrier Proteins metabolism, Liver metabolism, Neoplasm Proteins, Nerve Tissue Proteins, Palmitates pharmacokinetics

Abstract

Disposition kinetics of [(3)H]palmitate and its low-molecular-weight metabolites in perfused rat livers were studied using the multiple-indicator dilution technique, a selective assay for [(3)H]palmitate and its low-molecular-weight metabolites, and several physiologically based pharmacokinetic models. The level of liver fatty acid binding protein (L-FABP), other intrahepatic binding proteins (microsomal protein, albumin, and glutathione S-transferase) and the outflow profiles of [(3)H]palmitate and metabolites were measured in four experimental groups of rats: 1) males; 2) clofibrate-treated males; 3) females; and 4) pregnant females. A slow-diffusion/bound model was found to better describe the hepatic disposition of unchanged [(3)H]palmitate than other pharmacokinetic models. The L-FABP levels followed the order: pregnant female > clofibrate-treated male > female > male. Levels of other intrahepatic proteins did not differ significantly. The hepatic extraction ratio and mean transit time for unchanged palmitate, as well as the production of low-molecular-weight metabolites of palmitate and their retention in the liver, increased with increasing L-FABP levels. Palmitate metabolic clearance, permeability-surface area product, retention of palmitate by the liver, and cytoplasmic diffusion constant for unchanged [(3)H]palmitate also increased with increasing L-FABP levels. It is concluded that the variability in hepatic pharmacokinetics of unchanged [(3)H]palmitate and its low-molecular-weight metabolites in perfused rat livers is related to levels of L-FABP and not those of other intrahepatic proteins.

Published

2003

50. A family of textilinin genes, two of which encode proteins with antihaemorrhagic properties.

Author

Filippovich I, Sorokina N, Masci PP, de Jersey J, Whitaker AN, Winzor DJ, Gaffney PJ, and Lavin MF

Subjects

Amino Acid Sequence, Animals, Artificial Gene Fusion, Cloning, Molecular, Consensus Sequence, Elapid Venoms pharmacology, Hemostatics pharmacology, Mice, Models, Animal, Molecular Sequence Data, Recombinant Proteins pharmacology, Reverse Transcriptase Polymerase Chain Reaction, Sequence Alignment, Snake Venoms, Tail blood supply, Blood Loss, Surgical prevention & control, DNA, Complementary genetics, Elapid Venoms genetics

Abstract

Two peptides, textilinins 1 and 2, isolated from the venom of the Australian common brown snake, Pseudonaja textilis textilis, are effective in preventing blood loss. To further investigate the potential of textilinins as antihaemorrhagic agents, we cloned cDNAs encoding these proteins. The isolated full-length cDNA (430 bp in size) was shown to code for a 59 amino acid protein, corresponding in size to the native peptide, plus an additional 24 amino acid propeptide. Six such cDNAs were identified, differing in nucleotide sequence in the coding region but with an identical propeptide. All six sequences predicted peptides containing six conserved cysteines common to Kunitz-type serine protease inhibitors. When expressed as glutathione S-transferase (GST) fusion proteins and released by cleavage with thrombin, only those peptides corresponding to textilinin 1 and 2 were active in inhibiting plasmin with Ki values similar to those of their native counterparts and in binding to plasmin less tightly than aprotinin by two orders of magnitude. Similarly, in the mouse tail vein blood loss model only recombinant textilinin 1 and 2 were effective in reducing blood loss. These recombinant textilinins have potential as therapeutic agents for reducing blood loss in humans, obviating the need for reliance on aprotinin, a bovine product with possible risk of transmissible disease, and compromising the fibrinolytic system in a less irreversible manner.

Published

2002