2‐Substituted tricyclic oxazolo[5,4‐ d ]pyrimidine library: Design, synthesis and cytotoxicity activity

Author(s):  
Yan Zeng ◽  
Lifei Nie ◽  
Khurshed Bozorov ◽  
Zukela Ruzi ◽  
Buer Song ◽  
...  
2006 ◽  
Vol 49 (2) ◽  
pp. 607-615 ◽  
Author(s):  
Tummala R. K. Reddy ◽  
Roger Mutter ◽  
William Heal ◽  
Kai Guo ◽  
Valerie J. Gillet ◽  
...  

2017 ◽  
Vol 22 (1) ◽  
pp. 43-56 ◽  
Author(s):  
Peter C. Ray ◽  
Michael Kiczun ◽  
Margaret Huggett ◽  
Andrew Lim ◽  
Federica Prati ◽  
...  

Author(s):  
Salum Kassim Ali ◽  
Alidmat Mohammad Murwih ◽  
Khairulddean Melati ◽  
Kamal Nik Nur Syazni Nik Mohammad ◽  
Muhammad Musthahimah

2002 ◽  
Vol 724 ◽  
Author(s):  
Elizabeth R. Wright ◽  
R. Andrew McMillan ◽  
Alan Cooper ◽  
Robert P. Apkarian ◽  
Vincent P. Conticello

AbstractTriblock copolymers have traditionally been synthesized with conventional organic components. However, triblock copolymers could be synthesized by the incorporation of two incompatible protein-based polymers. The polypeptides would differ in their hydrophobicity and confer unique physiochemical properties to the resultant materials. One protein-based polymer, based on a sequence of native elastin, that has been utilized in the synthesis of biomaterials is poly (Valine-Proline-Glycine-ValineGlycine) or poly(VPGVG) [1]. This polypeptide has been shown to have an inverse temperature transition that can be adjusted by non-conservative amino acid substitutions in the fourth position [2]. By combining polypeptide blocks with different inverse temperature transition values due to hydrophobicity differences, we expect to produce amphiphilic polypeptides capable of self-assembly into hydrogels. Our research examines the design, synthesis and characterization of elastin-mimetic block copolymers as functional biomaterials. The methods that are used for the characterization include variable temperature 1D and 2D High-Resolution-NMR, cryo-High Resolutions Scanning Electron Microscopy and Differential Scanning Calorimetry.


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