5-Methyl-2-[(2-nitrophenyl)amino]-3-thiophenecarbonitrile has been crystallized as six solvent-free
polymorphs, which differ in the mode of packing and in molecular conformation. The conformational difference
results principally from the thiophene torsion relative to the o-nitroaniline fragment, which leads to different
crystal colors (red, orange, and yellow). Thermodynamic stability relationships between polymorphs have been
determined from solid-state conversions and calorimetric data of melting and eutectic melting. Vibrational
spectroscopy and ab initio calculations showed that most conformers in solution feature perpendicularly arranged
thiophene and o-nitroaniline fragments, although a minor population of more planar conformers also exist.
Crystallization has a stabilizing effect for more planar and higher dipole conformers over perpendicular ones
by 3−6 kJ/mol. The only exception to this pattern is the one polymorph containing weak intermolecular hydrogen
bonds.
The rat meniscal transection model of OA reproducibly displays both osteochondral and synovial angiogenesis comparable to our previous observations in human knee OA. DH guinea pigs, by contrast, display low vascularity throughout their protracted course of OA development. Changes in vascularisation occur early during the development of OA in the rat, and may contribute to the pathogenesis of OA.
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