Synthesis and anti-MRSA Activity of Novel Cephalosporin Derivatives

Stan V. D'Andrea,Daniel P. Bonner,Joanne J. Bronson,Junius M. Clark,Ken Denbleyker,Joan Fung-Tomc,Shelley E. Hoeft,Thomas W. Hudyma,John D. Matiskella,Raymond F. Miller,Peter F. Misco,Michael J. Pucci,Roman Z Sterzycki,Yuan Tsai,Yasutsuga Ueda,John A. Wichtowski,Janak Singh,Thomas P. Kissick,Jeffery T. North,Annie Pullockaran,Michael Humora,Brenda T Boyhan,Truc Chi Vu,Alan Fritz,J. Heikes,Rita Fox,Jollie D. Godfrey,Robert Kevin Perrone,Murray Arthur Kaplan,David R. Kronenthal,Richard H. Mueller

Synthesis and anti-MRSA Activity of Novel Cephalosporin Derivatives

2000

Abstract Cephalosporin derivatives containing a unique combination of lipophilic C -7 sidechains and polar C -3 thiopyridinium groups were synthesized and found to exhibit potent anti -MRSA activity in vitro and in vivo. The optimum C -7 sidechains utilized were 2,5-dichlorophenylthioacetamido and 2,6-dichloropyrid-4-ylthioacetamido. The C -3 thiopyridinium rings were substituted at nitrogen with amino acid and pyruvic acid groups that were designed to confer aqueous solubility as required for IV formulation. This paper describes the characteristics of these novel cephalosporins and highlights synthetic methods developed to allow their practical, large-scale syntheses.

Keywords:

Nitrogen
Solubility
Pyruvic acid
Amino acid
Organic chemistry
Cephalosporin
Aqueous solution
Biochemistry
Chemistry
anti mrsa
aqueous solubility
In vitro
In vivo
Stereochemistry

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