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Sir John R. Vane | Akateeminen Kirjakauppa

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Improved Non-Steroid Anti-Inflammatory Drugs: COX-2 Enzyme Inhibitors
Sir John R. Vane; Jack H. Botting; R.M. Botting
Springer (2011)
Pehmeäkantinen kirja
97,90
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ostoskoriin kpl
Siirry koriin
Selective COX-2 Inhibitors - Pharmacology, Clinical Effects and Therapeutic Potential
Sir John R. Vane; Jack H. Botting
Springer (2012)
Pehmeäkantinen kirja
97,90
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ostoskoriin kpl
Siirry koriin
Recent Advances in Prostaglandin, Thromboxane, and Leukotriene Research
Helmut Sinzinger; Bengt Samuelsson; Sir John R. Vane; Rodolfo Paoletti; Peter Ramwell; Patrick Y-K Wong
Springer Science+Business Media (1998)
Kovakantinen kirja
172,80
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ostoskoriin kpl
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New Targets in Inflammation - Inhibitors of COX-2 or Adhesion Molecules Proceedings of a conference held on April 15–16, 1996, i
N. Bazan; Jack H. Botting; Sir John R. Vane
Springer (2012)
Pehmeäkantinen kirja
97,90
Tuotetta lisätty
ostoskoriin kpl
Siirry koriin
Recent Advances in Prostaglandin, Thromboxane, and Leukotriene Research
Helmut Sinzinger; Bengt Samuelsson; Sir John R. Vane; Rodolfo Paoletti; Peter Ramwell; Patrick Y-K Wong
Springer-Verlag New York Inc. (2013)
Pehmeäkantinen kirja
172,80
Tuotetta lisätty
ostoskoriin kpl
Siirry koriin
Improved Non-Steroid Anti-Inflammatory Drugs: COX-2 Enzyme Inhibitors
97,90 €
Springer
Sivumäärä: 200 sivua
Asu: Pehmeäkantinen kirja
Painos: Softcover reprint of
Julkaisuvuosi: 2011, 25.12.2011 (lisätietoa)
Kieli: Englanti
In 1971, Vane proposed that the mechanism of action of the aspirin-like drugs was through their inhibition of prostaglandin biosynthesis. Since then, there has been intense interest in the interaction between this diverse group of inhibitors and the enzyme known as cyclooxygenase (COX). It exists in two isoforms, COX-l and COX-2 (discovered some 5 years ago). Over the last two decades several new drugs have reached the market based on COX-l enzyme screens. Elucidation of the three-dimensional structure of COX-l has provided a new understanding for the actions of COX inhibitors. The constitutive isoform of COX, COX-l has clear physiological functions. Its activation leads, for instance, to the production of prostacyclin which when released by the endothelium is anti-thrombogenic and anti-atherosclerotic, and in the gastric mucosa is cyto­ protective. COX-l also generates prostaglandins in the kidney, where they help to maintain blood flow and promote natriuresis. The inducible isoform, COX-2, was discovered through its activity being increased in a number of cells by pro­ inflammatory stimuli. A year or so later, COX-2 was identified as a distinct isoform encoded by a different gene from COX-I. COX-2 is induced by inflammatory stimuli and by cytokines in migratory and other cells. Thus the anti-inflammatory actions of non-steroid anti-inflammatory drugs (NSAIDs) may be due to the inhibition of COX-2, whereas the unwanted side-effects such as irritation of the stomach lining and toxic effects on the kidney are due to inhibition of the constitutive enzyme, COX-I.

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Myymäläsaatavuus
Helsinki
Tapiola
Turku
Tampere
Improved Non-Steroid Anti-Inflammatory Drugs: COX-2 Enzyme Inhibitors
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ISBN:
9789401090315
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