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81.
目的探讨乳凝集素(lactadherin)对新生仔兔在吮乳期及断奶期小肠粘膜发育以及小肠淋巴细胞发育的影响。方法新生仔兔共45只,随机分为母乳组(GB),配方奶组(GF)及配方奶加乳凝集素组(GL,100μg/ml),每组15只,在3w和5w应用图像分析技术检测新生仔兔小肠粘膜发育情况,分别在1、2、3、4和5w时,应用流式细胞技术测定小肠CD4+,CD8+,CD25+淋巴细胞发育情况。结果(1)GL组3w空肠绒毛周长、绒毛面积、绒毛高度及隐窝深度均超过GF组,GB组3w空肠绒毛周长及绒毛高度超过GF组;GL组5w空肠和回肠绒毛周长、绒毛面积、绒毛高度及隐窝深度均超过GF组和GB组。(2)5w各组小肠绒毛发生变化,绒毛表面由高密度的手指状变为平滑叶状或舌状,GL组绒毛面积和高度恢复较GB和GF组好。(3)GL组回肠CD4+淋巴细胞发育较GF组好,GB组较GL组好;GL组回肠CD25+淋巴细胞发育较GF组好(P<0.05)。结论乳凝集素对近端空肠粘膜形态发育和小肠CD4+和CD25+淋巴细胞发育有促进作用,并且可能帮助断奶期绒毛的恢复。  相似文献   
82.
Eight normal male volunteers received 80 mg doses of propranolol by the oral and rectal routes and 2.2 mg by intravenous administration in a crossover fashion. Plasma concentrations of propranolol were measured by a gas chromatographic method using an electron capture detector. Individual subject concentration-time data were analysed and results indicated that the data fit a two compartment model with first order absorption. An approximately two-fold higher plasma propranolol concentration was observed after rectal administration as compared with oral dosing. Statistical analysis of the difference in the total AUCs indicates a significantly higher bioavailability of propranolol administered by the rectal route. The reduced bioavailability after oral administration indicates a substantial first pass effect but that it is possible to bypass the liver, at least partially, by giving the drug rectally to man.  相似文献   
83.
目的 探讨马蹄莲不同部位微量元素的含量。方法 用发射光谱法、原子吸收法测定了马蹄莲根、茎、叶中20种微量元素的含量。结果 马蹄莲根、茎、叶中含有12种人体必需微量元素,其中Fe、Mn、Zn、Si、Li、Ca等七种元素含量较高。结论 马蹄莲富含多种人体必需的微量元素,预示马蹄莲具很高的药理保健价值。  相似文献   
84.
应用自显像技术对内镜活检胃肠化生和异型增生上皮进行~3H-TdR 标志,观察标记率及增殖带的变化。异型增生标记率(18.50~19.21)及大肠化生标记率(18.57)较高,与胃癌(19.32)相似,并且其增殖带向粘膜表面及深部移动。这种细胞动力学的变化可能是胃癌癌前病变的基础。  相似文献   
85.
本文报导用带蒂血管肠浆肌层环贴术防治各种复杂肠瘘,经过十一年的临床观察,疗效满意。本文还着重介绍了手术方法及操作过程中应注意的问题。  相似文献   
86.
采用2-甲基噻唑季胺盐与2-氯-1-甲酰基3-羟亚甲基环己烯,合成了五种题示染料。经IR及~1H-NMR谱确认了产物的结构,测定了电子吸收光谱、溶解度及稳定性,发现在染料苯环上引入甲氧基能改进染料溶解度,苯环上有氯取代的染料具有较高的光稳定性。  相似文献   
87.
This study has evaluated the possible role of serotonin, a potential morphogen, in the regulation of vasoactive intestinal polypeptide (VIP) gene expression in the target neurons of the suprachiasmatic nucleus (SCN) before and after the onset of the serotonin neurotransmitter function. VIP gene expression was quantified by in situ hybridization of the corresponding mRNA on cryostat sections with subsequent film autoradiography and densitometry. The content of VIP mRNA was measured in the SCN in fetuses at the 21st embryonic day (E21) and in postnatal rats at day 11 (P11) following chronic depletion of serotonin by p-chlorophenylalanine, an inhibitor of serotonin synthesis. This inhibitor was daily injected to pregnant rats for E13–20 or to postnatal animals for P2–10. Results of this study indicate that prenatal serotonin depletion caused a significant increase in VIP mRNA content in the SCN compared to control fetuses. On the contrary, the same treatment performed postnatally did not change VIP mRNA levels in the SCN. These data suggest that the VIP gene expression in differentiating target neurons of the SCN might be under serotonin inhibitory control during prenatal neurogenesis, prior to the onset of the serotoninergic neurotransmission.  相似文献   
88.
应用AB(pH1.0)KOH/PAS粘液组织化学和ABC法凝集素标记免疫组织化学方法对190例胃粘膜标本进行观察。结果表明,结肠不完全型肠上皮化生多见于肠型癌及其癌旁组织。在形态学和功能上,显示出一定程度的分化不成熟。两型肠化在弥漫型癌中无显著差异。5种凝集素受体含量和分布的差异与胃癌的组织学类型和分化程度有关,凝集素肠化分型和组织学类型的关系与粘液组化染色基本相符。我们认为不完全型肠化与肠型胃癌的发生关系密切,而完全型肠化可能与弥漫型胃癌有关。应用AB/KOH/PAS染色进行肠化分型和凝集素标记,对于癌前病变的检测和癌的早期诊断都具有一定价值。  相似文献   
89.
Summary Eight healthy volunteers participated in an open crossover study to assess the effect of a standardised meal on the systemic availability of a single oral dose of fenoldopam mesylate 100 mg. Subjects were studied on four separate occasions, twice fasting and twice fed in randomised, balanced order. Plasma and urine samples were obtained before and at regular intervals up to 25 h post dose. Measurement of fenoldopam (SK&F 82526) and its 8-sulphate metabolite (SK&F 87782) were by means of HPLC-EC analysis. Area under the plasma concentration time curve (AUC) and maximum detected plasma concentration (Cmax) for fenoldopam and SK&F 87782 were significantly reduced whereas time to maximum concentration was significantly increased with food. Using AUC's for fenoldopam and SK&F 87782, mean relative bioavailabilities were 35% and 81% respectively under fed compared with fasting conditions. Twenty-four hour excretion of fenoldopam was significantly reduced with food, but excretion of SK&F 87782 was apparently unchanged. Mean relative bioavailabilities calculated from these data were 83% and 86% respectively. Relatively large inter-subject variability in AUC and Cmax were seen, but intra-subject variability was not marked. Mild symptoms associated with vasodilation were reported on all study days.  相似文献   
90.
P-glycoprotein, a membrane-associated transport protein, has recently been recognised as an important element of the intestinal epithelium. This paper summarises thein vivodata on the pharmacological role of intestinal P-glycoprotein. These data show that P-glycoprotein contributes to the elimination of many drugs by mediating their direct secretion from the blood into the intestinal lumen. In addition, there is also evidence that this protein can limit oral drug absorption. Hence, inhibition of intestinal P-glycoprotein, e.g. by a reversal agent like cyclosporin A, may be a promising strategy for improving the oral bioavailability of P-glycoprotein substrate drugs. Indeed, several preclinical and clinical studies have shown that coadministration of drugs with a reversal agent can substantially increase oral drug absorption.  相似文献   
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