湿性脚气病中的基因-环境相互作用:硫胺素缺乏对CD36缺陷大鼠的影响
Gene-environment interactions in wet beriberi: effects of thiamine depletion in CD36-defect rats.
作者信息
Tanaka Takao, Kono Tatsuji, Terasaki Fumio, Kintaka Taigo, Sohmiya Koichi, Mishima Takayuki, Kitaura Yasushi
机构信息
Third Division, Department of Internal Medicine, Osaka Medical College, Takatsuki, Osaka 569-8686, Japan.
出版信息
Am J Physiol Heart Circ Physiol. 2003 Oct;285(4):H1546-53. doi: 10.1152/ajpheart.00182.2003.
Selective vulnerability to thiamine deficiency is known to occur between individuals and within different tissues. However, no comprehensive explanation for this has been found, and there are no reports that reproduce the cardiovascular manifestations of human wet beriberi in animals. We hypothesized that the distinction of substrate reliance, namely, the primary dependency on glucose as substrate, could be an underlying factor in the selective vulnerability of thiamine deficiency. In the setting of impaired fatty acid entry, which occurs in CD36-defect rats, substrate reliance shifts from fatty acid to glucose, which would be expected to lead to a susceptibility to thiamine deficiency. Genomic DNA was analyzed for CD36 defects in three cognate strains of rats [spontaneously hypertensive rats (SHR)/NCrj, SHR/Izm, and Wistar-Kyoto (WKY)/NCrj], which identified the presence of a CD36 defect in SHR/NCrj rats but not in SHR/Izm and WKY/NCrj rats. Treatment with 2 wk of thiamine-depleted chow on 4-wk-old rats of each of these strains resulted in increased body and lung weight in the SHR/NCrj rats but not in the SHR/Izm and WKY/NCrj rats. The increased lung weight in the SHR/NCrj rats was accompanied with histological changes of congestive vasculopathy, which were not observed in either the SHR/Izm or the WKY/NCrj rats. Thiamine-deficient 12-wk-old SHR/NCrj rats demonstrated increased body weight (305.6 +/- 6.2 g in thiamine-deficient rats vs. 280.8 +/- 9.1 g in control; P < 0.0001), lactic acidemia (pH, 7.322 +/- 0.026 in thiamine-deficient rats vs. 7.443 +/- 0.016 in control; P < 0.0001; lactate, 2.42 +/- 0.28 mM in thiamine-deficient rats vs. 1.20 +/- 0.11 mM in control; P < 0.0001) and reduced systemic vascular resistance (4.61 +/- 0.42 x 104 dyn.s.cm-5 in thiamine-deficient rats vs. 6.55 +/- 1.36 x 104 dyn.s.cm-5 in control; P < 0.0001) with high cardiac output (186.0 +/- 24.7 ml in thiamine-deficient rats vs. 135.4 +/- 27.2 ml in control; P < 0.0019). In conclusion, SHR/NCrj rats harboring a genetic defect of long-chain fatty acid uptake present the relevant clinical cardiovascular signs of human wet beriberi, strongly indicating a close gene-environment interaction in wet beriberi.
已知个体之间以及不同组织内部对硫胺素缺乏存在选择性易感性。然而,尚未找到对此的全面解释,也没有在动物身上重现人类湿性脚气病心血管表现的相关报道。我们推测,底物依赖性的差异,即主要依赖葡萄糖作为底物,可能是硫胺素缺乏选择性易感性的一个潜在因素。在脂肪酸进入受损的情况下,如在CD36缺陷大鼠中发生的那样,底物依赖性从脂肪酸转变为葡萄糖,这预计会导致对硫胺素缺乏的易感性。对三种同源品系的大鼠[自发性高血压大鼠(SHR)/NCrj、SHR/Izm和Wistar-Kyoto(WKY)/NCrj]的基因组DNA进行了CD36缺陷分析,结果发现在SHR/NCrj大鼠中存在CD36缺陷,而在SHR/Izm和WKY/NCrj大鼠中不存在。对这些品系4周龄的大鼠用缺乏硫胺素的饲料喂养2周,结果SHR/NCrj大鼠的体重和肺重量增加,而SHR/Izm和WKY/NCrj大鼠则没有。SHR/NCrj大鼠肺重量增加伴有充血性血管病变的组织学变化,而在SHR/Izm或WKY/NCrj大鼠中均未观察到这种变化。缺乏硫胺素的12周龄SHR/NCrj大鼠体重增加(缺乏硫胺素的大鼠为305.6±6.2克,对照组为280.8±9.1克;P<0.0001),出现乳酸性酸中毒(缺乏硫胺素的大鼠pH值为7.322±0.026,对照组为7.443±0.016;P<0.0001;缺乏硫胺素的大鼠乳酸为2.42±0.28毫摩尔/升,对照组为1.20±0.11毫摩尔/升;P<0.0001),全身血管阻力降低(缺乏硫胺素的大鼠为4.61±0.42×104达因·秒·厘米-5,对照组为6.55±1.36×104达因·秒·厘米-5;P<0.0001),心输出量高(缺乏硫胺素的大鼠为186.0±24.7毫升,对照组为135.4±27.2毫升;P<0.0019)。总之,携带长链脂肪酸摄取遗传缺陷的SHR/NCrj大鼠呈现出人类湿性脚气病相关的临床心血管体征,有力地表明了湿性脚气病中基因与环境的密切相互作用。
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