Brenner C, Pace H C, Garrison P N, Robinson A K, Rosler A, Liu X H, Blackburn G M, Croce C M, Huebner K, Barnes L D
Kimmel Cancer Institute, Thomas Jefferson University, Philadelphia, PA 19107, USA.
Protein Eng. 1997 Dec;10(12):1461-3. doi: 10.1093/protein/10.12.1461.
Fragile histidine triad protein (Fhit) is a diadenosine triphosphate (ApppA) hydrolase encoded at the human chromosome 3 fragile site which is frequently disrupted in tumors. Reintroduction of FHIT coding sequences to cancer cell lines with FHIT deletions suppressed the ability of these cell lines to form tumors in nude mice even when the reintroduced FHIT gene had been mutated to allow ApppA binding but not hydrolysis. Because this suggested that the tumor suppressor activity of Fhit protein depends on substrate-dependent signaling rather than ApppA catabolism, we prepared two crystalline forms of Fhit protein that are expected to model its biologically active, substrate-bound state. Wild-type and the His96Asn forms of Fhit were overexpressed in Escherichia coli, purified to homogeneity and crystallized in the presence and absence of ApppA and an ApppA analog. Single crystals obtained by vapor diffusion against ammonium sulfate diffracted X-rays to beyond 2.75 A resolution. High quality native synchrotron X-ray data were collected for an orthorhombic and a hexagonal crystal form.
脆性组氨酸三联体蛋白(Fhit)是一种二磷酸腺苷三磷酸(ApppA)水解酶,由人类染色体3脆性位点编码,该位点在肿瘤中经常发生破坏。将FHIT编码序列重新导入缺失FHIT的癌细胞系中,即使重新导入的FHIT基因已发生突变以允许ApppA结合但不水解,这些细胞系在裸鼠中形成肿瘤的能力也会受到抑制。因为这表明Fhit蛋白的肿瘤抑制活性取决于底物依赖性信号传导而非ApppA分解代谢,所以我们制备了两种Fhit蛋白晶体形式,预期它们能模拟其生物活性的底物结合状态。野生型和His96Asn形式的Fhit在大肠杆菌中过表达,纯化至同质,并在有和没有ApppA及一种ApppA类似物的情况下结晶。通过气相扩散对抗硫酸铵获得的单晶将X射线衍射至超过2.75 Å分辨率。为正交晶系和六方晶系的晶体形式收集了高质量的天然同步辐射X射线数据。
