Study on the Synthesis and Bioactivity of Sulfanilamide and Thiazole analogues Abstract The sulfanilamides were the first effective antibacterial drug which is folic acid antagonist. The sulfanilamide lead molecule constituted the basis for the development of all these types of pharmacological agents which such a varied spectrum of biological actions, as exemplified below for antibacterial agent, carbonic anhydrase inhibitor, diuretic agent, hypoglycemic agent, HIV protease inhibitor, metalloprotease inhibitor. A host of structurally novel sulfonamide derivatives have recently been reported to show substantial antitumor activity in vitro and in vivo. Although they have a common chemical motif of aromatic/ heterocyclic sulfonamide, there are a variety of mechanisms of their antitumor action, such as carbonic anhydrase inhibition, cell cycle arrest in the G1 phase, disruption of microtuble assembly, functional suppression of the transcription activitor NF-Y, and angiogenesis ( matreix metalloproteinase) inhibition among others. Previously, we usedsulfanilamide analogues to attach cantharidin to synthesis a series of imide compounds and founded a part compounds had antihepatocellular carcinoma activity. In order to further structural study, we used various anhydrides replace the structure of cantharidin to synthesis a series of sulfanilamides analogues ( compounds 1- 34) by the following method: sulfanilamide or other analogues were dealed with various anhydrides by heated to 200℃ in a sealed tube for 2 hours. After cooling, the residuals were removed from the tube, and were further evaporated and purified by TLC plate. Another series of thiazole analogues (compounds 35-57) were synthesized by the same method. All of these sulfanilamide and thiazole imide analogues were measured by H-NMR, IR, mass spectrometry. Besides, the series synthetic compounds of the sulfa and thiazole were tested for their capability to suppress growth of human hepatocellular carcinoma cell line. The data indicated that almost compounds of sulfanilamide are non- cytotoxicity. Another series of thiazole analogues would be tested .