Design of potent thiophene inhibitors of polo-like kinase 1 with improved solubility and reduced protein binding.

Kyle Allen Emmitte,George M. Adjebang,C. Webb Andrews,Jennifer G. Badiang-Alberti,Ramesh Bambal,Stanley D. Chamberlain,Ronda G. Davis-Ward,Hamilton D. Dickson,Daniel F. Hassler,Keith Hornberger,Jeffrey R. Jackson,Kevin Kuntz,Timothy J. Lansing,Robert A. Mook,Kristen E. Nailor,Mark Andrew Pobanz,Stephon C. Smith,Chiu-Mei Sung,Mui Cheung

Design of potent thiophene inhibitors of polo-like kinase 1 with improved solubility and reduced protein binding.

2009

Kyle Allen Emmitte
George M. Adjebang
C. Webb Andrews
Jennifer G. Badiang-Alberti
Ramesh Bambal
Stanley D. Chamberlain
Ronda G. Davis-Ward
Hamilton D. Dickson
Daniel F. Hassler
Keith Hornberger
Jeffrey R. Jackson
Kevin Kuntz
Timothy J. Lansing
Robert A. Mook
Kristen E. Nailor
Mark Andrew Pobanz
Stephon C. Smith
Chiu-Mei Sung
Mui Cheung

Abstract A series of thiophene PLK1 inhibitors was optimized for increased solubility and reduced protein binding through the appendage of basic amine functionality. Interesting selectivity between PLK1 and PLK3 was also obtained through these modifications.

Keywords:

Non-specific serine/threonine protein kinase
Solubility
PLK3
Enzyme
Organic chemistry
Thiophene
Polo-like kinase
Plasma protein binding
Biochemistry
Signal transduction
Chemistry
Selectivity
Stereochemistry
Chemical synthesis
Amine gas treating
PLK1

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations