Bo Andersson scite author profile

A number of substituted imidazo[1,2-a]pyridines and related analogues were selected for biochemical characterization in vitro against both the purified gastric proton pump enzyme, H+/K(+)-ATPase, and the intact gastric gland. The inhibitory activity in these two in vitro models was then examined for correlation with the gastric antisecretory potency determined for these compounds in vivo by using the histamine-stimulated Heidenhain pouch dog. Analysis of the biological data suggested that the inhibitory activity of the analogues determined in two in vitro models is predictive of their in vivo gastric antisecretory activity following intravenous, but not oral, administration. Furthermore, the good correlation observed between the in vitro and in vivo models suggests that these compounds are gastric proton pump inhibitors in vivo. A molecular modeling study of these compounds using the active analogue approach has defined the molecular volume which is shared by the active analogues, as well as the molecular volume which is common to the inactive analogues. Graphical representation of the difference between these molecular volumes can be interpreted in terms of a hypothetical description of the pharmacophore by means of which 3-(cyanomethyl)-2-methyl-8-(phenylmethoxy)imidazo[1,2-a]pyridine, Sch 28080 (1) and its analogues interact with the gastric proton pump enzyme, H+/K(+)-ATPase.

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Towards LarKC: A Platform for Web-Scale Reasoning

Fensel

Harmelen

Andersson

et al. 2008

102

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Characterizing three-dimensional topography of engineering and biomaterial surfaces by confocal laser scanning and stylus techniques

Wennerberg

Ohlsson

Rosén

et al. 1996

Medical Engineering & Physics

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Comparison of ready‐to‐use EMDOGAIN^®‐gel and EMDOGAIN^® in patients with chronic adult periodontitis

Bratthall

Lindberg

Havemose-Poulsen

et al. 2001

J Clinic Periodontology

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Bo Andersson

An animal study of c.p. titanium screws with different surface topographies

Antiulcer agents. 5. Inhibition of gastric H+/K+-ATPase by substituted imidazo[1,2-a]pyridines and related analogs and its implication in modeling the high affinity potassium ion binding site of the gastric proton pump enzyme

Towards LarKC: A Platform for Web-Scale Reasoning

Characterizing three-dimensional topography of engineering and biomaterial surfaces by confocal laser scanning and stylus techniques

Comparison of ready‐to‐use EMDOGAIN^®‐gel and EMDOGAIN^® in patients with chronic adult periodontitis

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Bo Andersson

An animal study of c.p. titanium screws with different surface topographies

Antiulcer agents. 5. Inhibition of gastric H+/K+-ATPase by substituted imidazo[1,2-a]pyridines and related analogs and its implication in modeling the high affinity potassium ion binding site of the gastric proton pump enzyme

Towards LarKC: A Platform for Web-Scale Reasoning

Characterizing three-dimensional topography of engineering and biomaterial surfaces by confocal laser scanning and stylus techniques

Comparison of ready‐to‐use EMDOGAIN®‐gel and EMDOGAIN® in patients with chronic adult periodontitis

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Product

Resources

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Comparison of ready‐to‐use EMDOGAIN^®‐gel and EMDOGAIN^® in patients with chronic adult periodontitis