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British Journal of Pharmacology | 1983

Effects of a pyridine derivative thromboxane synthetase inhibitor and its inactive isomer in endotoxic shock in the rat.

Katherine Anderegg; Peter Anzeveno; James A. Cook; P. V. Halushka; James R. McCarthy; Eugene R. Wagner; Wise Wc

1 We investigated the effects of a pyridine derivative thromboxane synthetase inhibitor and its inactive ortho isomer on arachidonic acid metabolism and pathophysiological sequelae of endotoxic shock. In vehicle‐treated rats, 30 min after intravenous S. enteritidis endotoxin (15 mg/kg), plasma iTxB2 (the stable metabolite of thromboxane A2) increased from non‐detectable levels (< 100 pg/ml) to 763 ± 250 pg/ml (n = 10). Plasma i6‐keto‐PGF1α (the stable metabolite of prostacyclin, PGI2) increased to 1850 ± 426 pg/ml, (n = 9) and plasma iPGE increased to 2350 = 560 (n = 5). Pretreatment with the pyridine active (PA) meta isomer (30 mg/kg i.p.) significantly (P < 0.05) suppressed iTxB2 to 390 ± 31 pg/ml (n = 10) although 6‐keto‐PGF1α levels (1294 ± 358 pg/ml, n = 5) and plasma iPGE (2847 ± 1103 pg/ml, n = 5) were not significantly different from the shocked control values. In contrast, pretreatment with, the pyridine inactive (PI) ortho isomer did not significantly affect endotoxin‐induced iTxB2 (1431 ± 194 pg/ml, n = 5) or i6‐keto‐PGF1α synthesis (628 ± 266 pg/ml, n = 5). 2 Pretreatment of rats with the Tx synthetase inhibitor, PA, significantly enhanced (P < 0.05) survival and prevented splanchnic infarction relative to both endotoxin shocked control rats and those pretreated with the PI isomer. 3 Significantly reduced lysosomal labilization, hepatocellular dysfunction and elevations in serum fibrin/fibrinogen degradation products were seen only in groups pretreated with the PA isomer. 4 The beneficial effects of the latter compound in Endotoxic shock thus appear to be due to inhibition of Tx synthesis, since its ortho isomer did not inhibit TxA2 synthesis nor did it protect against endotoxic shock.


Archive | 2016

production by macrophages from endotoxin-tolerant rats stimulated cAMP 2 Increased prostacyclin and PGE

James A. Cook; M. Makhlouf; Lawrence P. Fernando; Thomas W. Gettys; P. V. Halushka


Archive | 2008

Original Article β-Arrestin 2: a Negative Regulator of Inflammatory Responses in Polymorphonuclear Leukocytes

Fahmin Basher; Hongkuan Fan; Basilia Zingarelli; Keith T. Borg; Lou M. Luttrell; P. V. Halushka; James A. Cook


Shock | 2006

??-ARRESTINS REGULATE LIPOPOLYSACCHARIDE (LPS)-INDUCED SIGNALING AND PROINFLAMMATORY GENE EXPRESSION

Hongkuan Fan; L.M. Luttrell; Basilia Zingarelli; J.J. Senn; George E. Tempel; P. V. Halushka; James A. Cook


Shock | 2004

THE ROLE OF PHOSPHATIDYLINOSITOL 3 KINASE IN THE INDUCTION OF LIPOPOLYSACCHARIDE TOLERANCE AND PRIMING TO STAPHYLOCOCCUS AUREUS.: 196

Octavia M. Peck; Hongkuan Fan; George E. Tempel; P. V. Halushka; Giuseppe Teti; James A. Cook


Shock | 2004

HETEROTRIMERIC GI PROTEINS MEDIATE TLR4 SIGNALING TO ERK1/2 AND TO LPS INDUCED CYTOKINE PRODUCTION: 118

Hongkuan Fan; Octavia M. Peck; George E. Tempel; P. V. Halushka; James A. Cook


Shock | 2004

GI PROTEINS COUPLE CONVERGENT SIGNALING PATHWAYS TO LIPOPOLYSACC-HARIDE AND GRAM-POSITIVE BACTERIAL STIMULI: 25

Hongkuan Fan; Octavia M. Peck; Giuseppe Teti; George E. Tempel; P. V. Halushka; James A. Cook


Shock | 1997

MACROPHAGE/MONOCYTE REGULATORY G PROTEINS; IN VIVO VERSUS IN VITRO ENDOTOXIN TOLERANCE INDUCTION: 63

James A. Cook; M. Durando; M. Makhlouf; Sarah Ashton; P. V. Halushka


Shock | 1997

EFFECT OF LPS TOLERANCE ON EXPRESSION OF SPECIFIC REGULATORY G PROTEINS IN RAT PERITONEAL MACROPHAGES (MØ).: 76

Lawrence P. Fernando; M. Makhlouf; P. V. Halushka; I. Cook


Shock | 1995

TUMOR NECROSIS FACTOR; CROSS-TOLERANCE TO ENDOTOXIN AND ALTERATIONS IN MACROPHAGE FUNCTION.: 71

Basilia Zingarelli; P. V. Halushka; Achille P. Caputi; James A. Cook

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James A. Cook

Medical University of South Carolina

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Hongkuan Fan

Medical University of South Carolina

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George E. Tempel

Medical University of South Carolina

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Basilia Zingarelli

Cincinnati Children's Hospital Medical Center

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M. Makhlouf

Medical University of South Carolina

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Octavia M. Peck

Medical University of South Carolina

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Wise Wc

Medical University of South Carolina

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Lawrence P. Fernando

Medical University of South Carolina

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