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首页> 美国卫生研究院文献>Cancer Science >Glutathione S‐Transferases in Small Intestinal Mucosa of Patients with Coeliac Disease
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Glutathione S‐Transferases in Small Intestinal Mucosa of Patients with Coeliac Disease

机译:腹腔疾病患者小肠粘膜中的谷胱甘肽S-转移酶

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Patients with villous atrophy due to coeliac disease have an increased risk of developing small intestinal malignancies. Intestinal glutathione (GSH) and glutathione S‐transferases (GST) are involved in the protection against carcinogenesis. The aim of this study was to evaluate GSH content and GST enzyme activity in small intestinal mucosa of untreated coeliacs compared to controls. We evaluated GSH content and GST enzyme activity, including the levels of GST classes α, μ, π, θ in small intestinal biopsies of untreated coeliacs (flat mucosa, Marsh IHC, n=12) compared to normal subjects (n=23). Next, we evaluated GSH and GST's in coeliacs in remission (Marsh 0‐1, n=11), coeliacs with persisting villous atrophy while on a gluten‐free diet (partial villous atrophy, Marsh IIIA (n=5); subtotal villous atrophy, Marsh IIIB (n=6) and patients with infiltrative/crypt‐hyperplastic Marsh II lesions (n=4). Total GST enzyme activity and content of GSTa are markedly suppressed in Marsh IIIC lesions compared to controls (resp. 220±79 vs. 4641189 nmol/mg protein‐min (P<0.001) and 2.79±2.46 vs. 6.47±2.29 μg/mg protein (P<0.001). In coeliacs in remission these levels normalized. Total GST enzyme activity and GSTα levels are proportionately lowered according to the degree of mucosal pathology in Marsh II, IIIA and IIIB. (Spearman's σ correlation coefficient for total GST, ‐0.596, P<0.001; GSTα, ‐0.620, P<0.001). GSTμ, π and θ and GSH levels are not significantly different in the selected study groups of mucosal pathology compared to controls. Total GST enzyme activity and content of GSTα in small intestinal mucosa are significantly lower in untreated coeliac disease compared to controls. In Marsh II, IIIA and IIIB, GST enzyme activity and GSTα content are proportionally lower according to the degree of mucosal pathology. Normal values are seen in coeliacs in remission. This correlation between coeliac disease and a suppressed GSH/GST detoxification system may explain in part the carcinogenic risk in untreated coeliac disease.
机译:因腹腔疾病导致绒毛萎缩的患者罹患小肠恶性肿瘤的风险增加。肠谷胱甘肽(GSH)和谷胱甘肽S-转移酶(GST)参与了抗癌发生的保护作用。这项研究的目的是评估未处理的乳糜泻小肠粘膜中的GSH含量和GST酶活性。我们评估了未经处理的乳糜泻(扁平粘膜,沼泽IHC,n = 12)与正常受试者(n = 23)的小肠活检中的GSH含量和GST酶活性,包括GST类α,μ,π,θ的水平。接下来,我们评估了在无麸质饮食下持续缓解的乳糜泻(Marsh 0-1,n = 11),持续存在绒毛萎缩的乳糜泻(部分绒毛萎缩,Marsh IIIA(n = 5);次要的绒毛萎缩,Marsh IIIB(n = 6)和浸润性/隐匿增生性Marsh II病变的患者(n = 4)。与对照组相比,在Marsh IIIC病变中总GST酶活性和GSTa含量显着受到抑制(分别为220±79 vs 。4641189 nmol / mg蛋白-分钟(P <0.001)和2.79±2.46 vs. 6.47±2.29μg/ mg蛋白(P <0.001)。在缓解的乳糜中,这些水平正常化,总GST酶活性和GSTα水平成比例降低根据Marsh II,IIIA和IIIB中黏膜病理的程度(总GST的Spearmanσ相关系数,-0.596,P <0.001;GSTα,-0.620,P <0.001);GSTμ,π和θ和GSH水平为与对照组相比,在选定的黏膜病理学研究组中没有显着差异。与对照组相比,未经治疗的腹腔疾病的所有肠粘膜均显着降低。在沼泽II,IIIA和IIIB中,GST酶活性和GSTα含量根据粘膜病理的程度成比例地降低。在缓解的腹腔中可见正常值。腹腔疾病与GSH / GST排毒系统抑制之间的这种相关性可能部分解释了未经治疗的腹腔疾病的致癌风险。

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