A Structural Model of the Chloramphenicol Receptor Site

Hahn, Fred E.; Gund, Peter

doi:10.1007/978-3-7091-8405-9_17

Cited by 10 publications

(18 citation statements)

References 61 publications

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“…We tested the effect of CP, which inhibits protein synthesis by inhibiting the peptidyl-transferase activity of the 50s ribosomal subunit (24,25), on the MB-PDA and observed that it did not modify the glucose effect (data not shown). This result suggests that the glucose effect occurs independently of protein synthesis after photodynamic treatment.…”

Section: Discussionmentioning

confidence: 99%

Effect of Glucose on Photodynamic Action of Methylene Blue in Escherichia coli Cells

Capella¹,

Coelho

Menezes

1996

Photochem & Photobiology

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The results of this work show that the resistance of Escherichia coli cells to the photodynamic action of methylene blue is increased by the addition of glucose to the media in which they are grown. It is postulated that the increased resistance may be due to lowered retention of the dye by cells grown in the presence of glucose, leading to the diminution in DNA damage revealed in the alkaline sucrose gradients. The role of cyclic adenosine-monophosphate in the protective action of glucose is discussed.

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Section: Discussionmentioning

confidence: 99%

Effect of Glucose on Photodynamic Action of Methylene Blue in Escherichia coli Cells

Capella¹,

Coelho

Menezes

1996

Photochem & Photobiology

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“…1): 4-phenylpiperidines (PP); 3,3-diphenylpropylamines (DPA); diamines (DA); and several miscellaneous classes. The problem of deciding whether or not these drugs bind to a unique receptor site remains obscure for both pharmacologists and s P 2 P 3 Douglas et al, 1977Gund and Shen, 1977Gund et al, 1979aSmith et al, 1979Gund and Veber, 1979bLumma et al, 1978Veber et al, 1978Veber, 1980Freidinger and Veber, 1979Hahn and Gund, 1974Stuper et al, 1979Dyott et al, 1980Eaton and Pensak, 1978Nordby and Hodges, 1975 Nordby (to be published) Nordby and Hodges, 1975Cohen, 1979Rohrer et al, 1979Fullerton et al, 1979Fullerton et al. 1980Nichols et al, 1978Marshall et al, 1979Marshall, 1978Gorin and Marshall, 1977Cobb et al, 1978Sufrin et al, 1979Weaver et al, 1979Andrews, 1979bPauling, 1978Cody, 1979Humber et al, 1979Philipp et al, 1979 4 While several uniform receptor models [Feinberg et al, 1976;Galt, 19771 have been proposed, none of them can provide an explanation for the activity encountered in every structural class.…”

Section: A Opiate Receptor Modelingmentioning

confidence: 99%

Three‐dimensional computer modeling as an aid to drug design

Humblet¹,

Marshall²

1981

Drug Development Research

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Humblet, C., and G.R. Marshall: Three-dimensional computer modeling as an aid to drug design. Drug Dev. Res. 1:409-434, 1981. Three-dimensional computer graphic systems are an emerging tool in the design of therapeutic compounds. The molecular recognition process involved in drug receptor interaction implies a three-dimensional stereospecificity shared by a set of drugs of similar pharmacological action. In investigating the pharmacophore, it is therefore necessary to go beyond two-dimensional structures by including the description of the spatial properties of drugs. 410 Humblet and MarshallThis review describes both current and potential tools that a graphic computer can support to help the medicinal chemist in his structure-activity puzzle. An outline of the systems presently in use for this purpose and a summary of recent applications is given. Some current developments undertaken in our research group are presented in the field of opiates, GABA, clonidine, antipsychotics, and S-adenosyl-Lmethionine inhibitors.

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“…Chloramphenicol (CHL) is a broad-spectrum antibiotic, currently included in List of Essential Medicines (EML) published by the World Health Organization (WHO) [1]. Originally isolated from Streptomyces venezuelae in 1947 [2,3], its structure (shown in Fig. 1) was soon elucidated and became the first antibiotic to be synthesized by chemical means [2,3].…”

Section: Introductionmentioning

confidence: 99%

“…Originally isolated from Streptomyces venezuelae in 1947 [2,3], its structure (shown in Fig. 1) was soon elucidated and became the first antibiotic to be synthesized by chemical means [2,3]. CHL acts essentially as a bacteriostatic agent, inhibiting bacterial synthesis by binding to the 50S subunit of 70S ribosomes [2].…”

Section: Introductionmentioning

confidence: 99%