Greene D M, Azcona-Olivera J I, Murtha J M, Pestka J J
Department of Food Science and Human Nutrition, Michigan State University, East Lansing 48824-1224, USA.
Fundam Appl Toxicol. 1995 Jun;26(1):107-16. doi: 10.1006/faat.1995.1080.
Ingestion of the trichothecene vomitoxin (VT) by mice induces effects that mimic the common human glomerulonephritis, IgA nephropathy (IgAN). These include elevation of serum IgA, IgA immune complexes, and mesangial IgA deposition. Based on previous observations that male mice are more prone to VT-induced IgAN, the effects of castration of male and female B6C3F1 mice and sex hormone supplementation on several immunopathologic indicators of the disease were compared. In the first study, castrated and intact male and female mice were fed control AIN-76A diet or the same diet containing 10 ppm VT for 12 weeks. At Week 12, all but the intact female group fed VT exhibited increased serum IgA, with castrated female mice having greater levels than intact females. When microscopic hematuria was used as an indicator of disease severity in intact VT-fed mice, erythrocyte counts for males exceeded those for females at weeks 4 and 12. VT-fed, castrated females exhibited greater hematuria than intact counterparts, whereas VT-fed, castrated males had lower urinary erythrocyte counts than intact counterparts. In a second study, castrated male and female mice were implanted with controlled release pellets of placebo, 5 alpha-dihydrotestosterone (DHT), or 17 beta-estradiol (E2) and then were fed either control diet or a 10 ppm VT diet for 8 weeks. Castrated male and female mice treated with VT and DHT pellet exhibited more severe hematuria, higher IgA levels, and greater mesangial IgA deposition than mice exposed to the same diet with placebo or E2 pellet at Week 8. While VT-fed animals with an E2 pellet exhibited greater hematuria and mesangial IgA deposition at Week 8 than the placebo groups, their IgA levels were not significantly elevated over those for VT-fed mice with a placebo pellet. Relative to two other pathologic markers for IgAN, the aforementioned effects in both studies were generally consistent with mesangial deposition of complement component C3 but not IgG. The results suggest that (1) enhanced male susceptibility to VT-induced IgAN may be related to modulation by the biologically active androgen DHT and (2) while castration of females increased severity of VT-induced IgAN, supplementation of castrated male or female mice with E2 did not reverse this effect but rather increased disease severity.
小鼠摄入单端孢霉烯族呕吐毒素(VT)会引发一些效应,这些效应类似于常见的人类肾小球肾炎——IgA肾病(IgAN)。这些效应包括血清IgA、IgA免疫复合物升高以及系膜IgA沉积。基于之前观察到雄性小鼠更易发生VT诱导的IgAN,比较了对雄性和雌性B6C3F1小鼠去势以及补充性激素对该疾病若干免疫病理指标的影响。在第一项研究中,给去势和未去势的雄性及雌性小鼠喂食对照AIN - 76A饮食或含10 ppm VT的相同饮食,持续12周。在第12周时,除了喂食VT的未去势雌性组外,所有喂食VT的组血清IgA均升高,去势雌性小鼠的血清IgA水平高于未去势雌性小鼠。当将显微镜下血尿用作喂食VT的未去势小鼠疾病严重程度的指标时,在第4周和第12周,雄性小鼠的红细胞计数超过雌性小鼠。喂食VT的去势雌性小鼠比未去势的雌性小鼠血尿更严重,而喂食VT的去势雄性小鼠的尿红细胞计数低于未去势的雄性小鼠。在第二项研究中,给去势的雄性和雌性小鼠植入安慰剂、5α - 二氢睾酮(DHT)或17β - 雌二醇(E2)的控释微丸,然后喂食对照饮食或含10 ppm VT的饮食8周。在第8周时,与接受相同饮食但植入安慰剂或E2微丸的小鼠相比,植入DHT微丸且喂食VT的去势雄性和雌性小鼠血尿更严重、IgA水平更高且系膜IgA沉积更多。虽然在第8周时,植入E2微丸且喂食VT的动物比安慰剂组血尿更严重且系膜IgA沉积更多,但其IgA水平相对于植入安慰剂微丸且喂食VT的小鼠并未显著升高。相对于IgAN的其他两个病理标志物,上述两项研究中的效应总体上与补体成分C3的系膜沉积一致,但与IgG的系膜沉积不一致。结果表明:(1)雄性对VT诱导的IgAN易感性增强可能与生物活性雄激素DHT的调节有关;(2)虽然雌性去势会增加VT诱导的IgAN的严重程度,但给去势的雄性或雌性小鼠补充E2并不能逆转这种效应,反而会增加疾病严重程度。
