Aquaporin 1在中国人肺鳞癌细胞的表达

目的研究Aquaporin 1(AQP1)对中国人肺鳞癌细胞分化过程的影响。方法采用HE染色和AQP1免疫组织化学法对高、中、低分化的人肺癌细胞进行染色,光学显微镜观察并显微摄影。结果AQP1在高、中分化的肺鳞癌细胞呈阳性表达,在低分化的肺鳞癌细胞呈阴性表达;在高分化鳞癌中,角化珠旁的癌细胞呈较强阳性表达,癌巢周围的癌细胞呈阴性表达。结论AQP1参与人肺麟癌细胞的分化,其表达可能同分化程度相关。

GST Fusion Protein Based Specific Polyclonal Antibody Preparation of Mouse Aquaporin 1

Aquaporins（AQPs） are specific membrane channels for water and other small nonionic molecules.In order to overcome the difficulties to generate the effictive antibody of membrane protein,we selected the cytoplasmic C-terminus of Aquaporin 1（AQP1） as an unique antigen.The long C-terminus of mouse AQP1 was overexpressed in the Glutathione S-tansferase Gene Fusion System.On the basis of the resonable amounts of soluable membrane protein peptides,we prepared the specific antibody.To pursure this object,we constructed pGEX-4T-1/mAQP1（DNA sequence from 700 to 801 bp） recombinant plasmid and transformed it into Escherichia coli BL21 cells.The GST-AQP1 C-terminal hydrophilic peptide fusion protein was induced by IPTG and further purified by Glutathione Sepharose 4B to obtain the right size fusion protein.Then we immunized the New Zealand rabbits to prepare the antiserum.The purified AQP1 antibody showed high sensitivity by ELISA assay and high specificity by Western blot with AQP1 null mice served as negative control.Finally,we also checked the AQP1 localization in the mouse renal tissues in wild type of mice and AQP1 null mice served as negative control.We demonstrated that AQP1 was highly expressed at the descending limb of Henle tube using our purified AQP1 antibody,which was consistent with previous report.The successful design and preparation of AQP1 antibody through GST technique is an example as making antibodies against a specific membrane protein.

Aquaporin 1 Facilitated Hepatocellular Carcinoma SMMC7221 Cell Migration Associated with Water Permeability

The authors investigated the regulation of human aquaporin I（hAQP1） and the involvement of aquaporin 1 （AQP 1） in the migration of human hepatocellular carcinoma SMMC-7221 cells using RNA intereference technology Firstly, two short hairpin RNA（shRNA） constructs in PBSU6 vector were reconstructed and their knockdown effects were identified in SMMC-7221 cells. Next, the involvement of endogenous hAQP1 in regulating the migration of SMMC-7221 cells was investigated via siRNA technology. HAQPI-shRNA can specifically inhibit AQP1 dependent osmotic water permeability. Meanwhile the migration of SMMC-7221 cells was inhibited remarkably after silencing AQP1 by performing transwell cell migration assay and in vitro wound healing assay. Furthermore, in the presence of an inhibitor HgCl2, the water permeability of the cell membrane was remarkably decreased, the expression of AQP1 was upregulated after HgCla treatment and the cell movement was decreased at the moment. Increased AQP1 cannot attenuate cell migration ability when cell membrane loses its water permeability function. This demonstrates that the cell migration was remarkably related to the transporting water function of cell membrane.

Correlation between the Expression of Aquaporin 1 and Hypoxia-inducible Factor 1 in Breast Cancer Tissues

The correlation between aquaporin 1 （AQP1） and hypoxia-inducible factor 1 （HIF 1） in breast cancer tissues was preliminarily studied. In 155 cases of breast cancer, the expression levels of AQP1 were detected by immunohistochemisty in HIFl-positive group or HIFl-negative group, and the correlation between AQP1 and HIF1 was analyzed. The overexpression of AQP1 and HIF1 were observed in 155 cases of breast cancer tissues. The expression level of AQP1 in HIFl-positive group was significantly higher than that in HIFl-negative group. The positive expression rate of AQP1 was 296.55±24.67 and 168.37±37.53 in HIFl-positive group and HIFl-negative group respectively with the difference being very significant between them （P〈0.001）. It was concluded that AQP1 was overexpressed in the HIFl-positive group and there were some correlations between AQP1 and HIF1, suggesting they interact each other and regulate the oncogenesis of breast cancer.

Comment on: Cloning and characterization of porcine aquaporin 1 water channel expressed extensively in the gastrointestinal system

TO THE EDITOR Sir,I read with great interest the recently pubiished article in rhe World Journal of Gastroenterology by JIn and co-workers on the cloning and characterization of Porcine aquaporin 1 water channel from the pig liver and studies on its expression in

Aquaporin 1 overexpression may enhance glioma tumorigenesis by interacting with the transcriptional regulation networks of Foxo4,Maz,and E2F families

Background The glioblastoma has served as a valuable experimental model system for investigating the growth and invasive properties of glioblastoma.Aquaporin-1(AQP1)in facilitating cell migration and potentially contributing to tumor progression.In this study,we analyzed the role of AQP1 overexpression in glioblastoma and elucidated the main mechanisms involved.Methods AQP1 overexpression recombinant vector was introduced into C6 rat glioma cells to construct an AQP1 overexpression C6 cell line,and its effect on cell viability and migration ability was detected by MTT and Transwell.RNA was extracted by Trizol method for gene sequencing and transcriptomics analysis,and the differentially expressed genes(DEGs)were enriched for up-and downregulated genes by Principal component analysis(PCA),and the molecular mechanism of AQP1 overexpression was analyzed in comparison with the control group using the NCBI GEO database.Statistical analysis was performed using Mann-Whitney paired two tailed t test.Results The cell viability of AQP1-transfected cell lines increased by 23%and the mean distance traveled increased by 67%compared with the control group.Quantitative analysis of gene expression showed that there were 12,121 genes with an average transcripts per million(TPM)value greater than 1.DEGs accounted for 13%of the genes expressed,with the highest correlation with upregulated genes being FOXO4 and MAZ,and the highest with down-regulated genes being E2F TFs.Conclusions AQP1 may be implicated in glioma formation by interacting with the transcriptional regulation networks involving the FOXO4,MAZ,and E2F1/2.These findings shed light on the potential significance of AQP1 in glioma pathogenesis and warrant further investigations to unravel the underlying molecular mechanisms.

血清Omentin-1、AQP4、VILIP-1预测急性前循环大血管闭塞性脑梗死的价值分析

目的:探讨急性前循环大血管闭塞性脑梗死(ALVS)患者在急诊血管内治疗术后血管再通后血清视椎蛋白样蛋白1(VILIP-1)、水通道蛋白-4(AQP4)、网膜素-1(Omentin-1)的表达和临床意义。方法:选取154例我院2019年9月-2022年9月就诊的ALVS患者,入院后均行血管内治疗术,根据术后90d改良Rankin(mRS)评分分为预后良好组116(75.32%)、预后不良组38例(24.68%),比较两组临床资料及术前、术后1个月Omentin-1、AQP4、VILIP-1的表达水平,Pearson分析术后1个月上述指标与mRS评分相关性,Logistic回归方程分析预后影响因素,并分析其预测价值。结果:与预后良好组比较,预后不良组术前血清VILIP-1、AQP4水平较低(P<0.05),Omentin-1水平较高(P<0.05),术后1个月血清VILIP-1、AQP4水平较低(P<0.05),Omentin-1水平较高(P<0.05),且术后1个月更为显著(P<0.05);术后1个月血清VILIP-1、AQP4水平与mRS评分呈正相关,Omentin-1水平与mRS评分呈负相关(P<0.05);VILIP-1、AQP4为术后90d预后不良危险因素,Omentin-1为预后不良保护因素(P<0.05);与低危组比较,高危组术后90d不良预后发生率高于低危组(P<0.05)。结论:血清VILIP-1、AQP4、Omentin-1水平为ALVS患者血管内治疗术后血管再通预后的重要影响因素,为临床早期评估和预测预后提供可靠依据。

老年急性脑梗死患者血清Lp-PLA2、CaM、AQP1变化及其与预后的关系

目的检测老年急性脑梗死患者血清脂蛋白相关磷脂酶A2(Lp-PLA2)、钙调蛋白(CaM)、水通道蛋白1(AQP1)水平,并探讨其与预后的关系。方法回顾性分析2021年2月至2022年2月于北京中医药大学孙思邈医院就诊的104例老年急性脑梗死患者的临床资料,依据入院后美国国立卫生研究院卒中(NHISS)量表评分进行分组,其中重度组23例,中度组43例,轻度组38例;采用改良Rankin(mRS)量表评估所有患者3个月后预后情况,并依据评分分组,其中预后不佳组37例,预后良好组67例,比较不同神经功能缺损程度患者血清Lp-PLA2、CaM、AQP1水平,应用Spearman相关性分析老年急性脑梗死患者血清Lp-PLA2、CaM、AQP1水平与神经功能缺损程度的相关性,采用多因素Logistic回归分析探究老年急性脑梗死患者预后不佳的影响因素。结果重度组患者的Lp-PLA2、CaM、AQP1水平分别为(328.24±84.26)U/L、(227.59±61.34)ng/mL、(44.51±8.26)μg/L,明显高于中度组的(264.56±61.44)U/L、(150.17±44.38)ng/mL、(35.19±5.98)μg/L和轻度组的(201.83±55.12)U/L、(83.24±20.14)ng/mL、(24.32±3.48)μg/L,且中度组患者的Lp-PLA2、CaM、AQP1水平明显高于轻度组,差异均有统计学意义(P<0.05);经Spearman相关性分析显示,老年急性脑梗死患者Lp-PLA2、CaM、AQP1水平与神经功能缺损程度均呈正相关性(P<0.05);预后不佳组与预后良好组患者的性别、年龄、身体质量指数(BMI)、基础疾病等资料比较差异均无统计学意义(P>0.05),但预后不佳组患者的NIHSS评分为(16.58±3.51)分,明显高于预后良好组的(14.24±2.35)分,血清Lp-PLA2、CaM、AQP1水平分别为(273.84±53.26)U/L、(174.69±48.65)ng/mL、(41.32±6.88)μg/L,明显高于预后良好组的(211.56±51.89)U/L、(130.43±38.55)ng/mL、(32.64±3.72)μg/L,差异均具有统计学意义(P<0.05);经多因素Logistic回归分析显示,血清Lp-PLA2、CaM、AQP1水平为老年急性脑梗死患者预后不佳的危险因素(P<0.05)。结论伴随老年急性脑梗死神经功能缺损程度加重,患者血清Lp-PLA2、CaM、AQP1水平均会出现升高现象;且血清Lp-PLA2、CaM、AQP1为老年急性脑梗死患者预后不佳的危险因素,值得临床重视。

急性大血管闭塞性卒中患者中omentin-1、AQP4、VILIP-1与急诊血管内治疗后血管再通的关系

目的探讨急性大血管闭塞性卒中(ALVOS)患者中网膜素-1(omentin-1)、水通道蛋白4(AQP4)、视锥蛋白样蛋白-1(VILIP-1)与急诊血管内治疗后血管再通的关系及联合预测效能。方法选取110例行急诊血管内治疗的ALVOS患者,根据术后血管是否再通分为未再通组(23例)和再通组(87例),比较2组的临床资料和omentin-1、AQP4、VILIP-1水平。采用LASSO回归初筛术后血管再通的特征变量,寻找可使模型性能优良且影响因素最少的变量。采用logistic回归分析术后血管再通的影响因素。应用R语言绘制列线图预测术后血管再通,应用受试者操作特征(ROC)曲线和校准曲线评价、验证列线图的预测效能和校准度。结果未再通组高血压患者占比、术前美国国立卫生研究院卒中量表(NIHSS)评分、急诊血糖、AQP4和VILIP-1水平高于再通组,发病至血管内治疗时间长于再通组,术前Alberta卒中项目早期CT评分(ASPECTS)、静脉溶栓患者占比、血小板、omentin-1水平低于再通组(P<0.05)。术前ASPECTS、omentin-1水平是术后血管再通的相关独立保护因素,发病至血管内治疗时间、术前NIHSS评分、AQP4和VILIP-1水平是术后血管再通的相关独立危险因素(P<0.05)。运用R语言对logistic回归进行列线图可视化分析,该列线图预测术后血管再通的一致性指数为0.994,呈现出良好的区分度;列线图的ROC曲线显示,列线图预测术后血管再通的AUC为0.994,预测灵敏度为98.90%,特异度为95.70%,校准度为0.975,与实际观测结果曲线贴合度良好。结论omentin-1、AQP4、VILIP-1水平为ALVOS患者急诊血管内治疗后血管再通的重要影响因素,临床可通过监测其水平进行早期预测,采取针对性治疗,改善血管再通情况。

水通道蛋白1作为急性呼吸窘迫综合征肺部炎症水平的新生物标志物探索研究

目的探讨急性呼吸窘迫综合征(ARDS)肺组织水通道蛋白1(AQP1)表达水平的时效规律以及与肺损伤程度、经典炎症指标的相关性,旨在为ARDS寻找新的生物标志物及干预靶点。方法脂多糖(LPS)滴鼻制备ARDS小鼠模型,每日称量小鼠体质量,取6 h、1 d、3 d和7 d四个时间点肺组织和肺泡灌洗液,HE分析肺组织病理变化,ELISA和qPCR检测炎症因子IL-1β、IL-6和TNF-α的表达水平,流式细胞术分析中性粒细胞、肺泡巨噬细胞、嗜酸性粒细胞、单核细胞等天然免疫细胞数量及比例,qPCR和Western blotting检测AQP1 mRNA和蛋白表达水平,Pearson法分析AQP1与炎性细胞相关性。结果LPS刺激6 h后小鼠肺组织有炎性细胞浸润,至第3日出现严重肺损伤,第7日有所恢复;炎症因子IL-1β、IL-6和TNF-αmRNA和蛋白水平持续升高至第3日,第7日降低(P<0.05);中性粒细胞比例显著升高,第7日降低,肺泡巨噬细胞和嗜酸性粒细胞、单核细胞比例持续降低至第3日,第7日升高(P<0.05);AQP1 mRNA和蛋白表达水平持续降低(P<0.05);AQP1表达水平与四种炎性细胞显著相关(P<0.01)。结论ARDS肺组织AQP1表达水平与肺损伤程度及炎症指标呈显著负相关,可作为肺损伤的新生物标志物,进一步揭示AQP1可能扮演的保护性角色具有潜在临床价值。

高频重复经颅磁刺激联合高压氧对颅脑损伤后昏迷患者预后、意识障碍程度及血清AQP-1水平的影响

目的探究高频重复经颅磁刺激联合高压氧对颅脑损伤后昏迷患者预后、意识障碍程度及血清水通道蛋白1(AQP-1)水平的影响。方法前瞻性将2021年3月至2023年5月在沧州市人民医院就诊的88例颅脑损伤后昏迷患者纳入研究。按照随机数字表法将其分为对照组(n=44)和研究组(n=44)。对照组采用高压氧治疗,研究组在对照组的基础上联合高频重复经颅磁刺激治疗。检测并比较两组患者治疗前、治疗4周后血清AQP-1、超氧化物歧化酶(SOD)、乳酸脱氢酶(LDH)、C反应蛋白(CRP)、胶质纤维酸性蛋白(GFAP)、脑源性神经营养因子(BDNF)、神经元特异性烯醇化酶(NSE)水平;用格拉斯哥昏迷评分量表(GCS)、昏迷恢复修订量表(CRS-R)评估患者治疗前后的意识状态,并统计两组患者清醒率及清醒时间、昏迷期间并发症情况以及不良反应。结果研究组治疗4周后血清AQP-1、LDH、CRP水平分别为(21.24±6.61)μg/L、(246.61±32.88)U/L、(24.70±4.37)mg/L,均显著低于对照组[(26.33±7.86)μg/L、(295.73±50.09)U/L、(30.88±5.92)mg/L],SOD水平为(27.56±7.62)U/mL,显著高于对照组[(20.19±4.68)U/mL],差异均有统计学意义(P<0.05)。研究组患者治疗4周后GFAP、NSE水平分别为(2.07±0.68)、(3.81±1.16)ng/mL,均显著低于对照组[(4.49±1.13)、(7.20±1.44)ng/mL],BDNF水平为(2.64±0.89)ng/mL,高于对照组[(1.87±0.51)ng/mL],差异均有统计学意义(P<0.05)。研究组患者治疗4周后GCS评分与CRS-R评分分别为(12.39±3.05)、(19.66±4.89)分,均显著高于对照组[(9.17±2.46)、(14.94±3.55)分],差异均有统计学意义(P<0.05)。研究组意识清醒时间为(22.36±5.74)d,显著短于对照组[(28.18±8.25)d],清醒率为93.18%,显著高于对照组(77.27%),并发症发生率为13.64%,显著少于对照组(38.63%),差异均有统计学意义(P<0.05)。两组不良反应发生率比较,差异无统计学意义(P>0.05)。结论联合高频重复经颅磁刺激与高压氧治疗可以有效改善颅脑损伤后昏迷患者意识状态,降低血清AQP-1水平,缩短患者意识清醒时间。

鸦胆子油乳联合调强放疗对喉癌治疗效果、放疗副作用及血Treg/Th17细胞因子水平的影响

目的:研究鸦胆子油乳联合调强放疗对喉癌治疗效果、放疗副作用、血调节性T细胞/辅助性T细胞17(Treg/Th17)细胞因子水平的影响,为临床提供参考。方法:选择2021年1月—2022年7月商丘市第一人民医院收治的126例喉癌患者作为研究对象,采用随机数表法分为对照组和观察组,每组各63例。对照组采用调强放疗治疗,观察组采用鸦胆子油乳联合调强放疗治疗。比较两组患者临床疗效、治疗前及治疗21 d后血清Treg/Th17相关细胞因子[白细胞介素(IL-6)、IL-17、IL-23、转化生长因子-β (TGF-β)]水平、血清细胞角蛋白19片段抗原21-1 (CYFRA21-1)、鳞状细胞癌相关抗原(SCC)、水通道蛋白-1 (AQP-1)、斯钙素-1 (STC-1)水平,卡氏评分(KPS)及放疗副作用。结果:观察组临床总有效率高于对照组,差异有统计学意义(χ^(2)=5.420,P<0.05);治疗21 d后,观察组血清IL-6、IL-17、IL-23、TGF-β水平低于对照组,差异有统计学意义(t=5.211、17.611、7.748、9.482,P<0.05);治疗21 d后,观察组血清CYFRA21-1、SCC、AQP-1、STC-1水平低于对照组,差异有统计学意义(t=10.299、5.663、9.091、7.389,P<0.05);治疗21 d后观察组KPS评分高于对照组(t=13.674,P<0.05);观察组放疗副作用低于对照组,差异有统计学意义(χ^(2)=4.203、4.881、4.308、5.143,P<0.05)。结论:采用鸦胆子油乳与调强放疗联合治疗喉癌患者可获得更好的临床疗效,能进一步下调血清Treg/Th17细胞因子水平,提高患者体能状态,有效缓解毒副反应。

Aquaporin-1蛋白在缺血心肌中表达变化及其与心肌水肿的关系

目的在动物心肌梗塞模型中探讨心肌缺血状态下心肌细胞膜水通道蛋白Aquaporin-1的变化趋势及其与心肌水肿的联系。方法采用抗AQP1特异性免疫组化考查AQP1在心肌组织中的分布特点;以Real-timePCR及Westernblotting了解在缺血状态下心肌组织AQP1基因转录及蛋白表达的动态变化趋势;采用Evan’blue定量测定法了解缺血心肌组织中毛细血管通透性的变化及用心肌水含量测定法了解缺血心肌的水肿程度。结果AQP1在心肌中存在着广泛分布,并主要分布于心肌的血管及心肌细胞膜。缺血造成AQP1在心肌的转录及蛋白表达呈现先减后增的趋势;缺血后心肌水肿程度存在着双峰样变化趋势而且AQP1蛋白的表达增加的时间特征上与缺血后的第二个水肿高峰的变化趋势相一致。结论AQP1蛋白在心肌缺血后存在着先减后增的动态变化,AQP1蛋白的表达增加可能与部分地联系到缺血后的心肌水肿的形成。

Aquaporin-1在大鼠睾丸输出小管的免疫组织化学定位研究

目的 研究正常大鼠睾丸输出小管上皮细胞上Aquaporin 1(AQP 1)的定位分布以期了解其在水重吸收上的作用机制。方法 对正常Wistar大鼠睾丸输出小管进行常规免疫组织化学方法染色观察。结果 在睾丸输出小管非纤毛上皮细胞的刷状缘及基侧部AQP 1阳性表达强烈 ,核上区的胞内体的质膜上也有阳性表达 ;纤毛上皮细胞的纤毛亦呈阳性反应。结论 Aquaporin 1可能与睾丸输出小管非纤毛上皮细胞水重吸收功能有密切关系。

缺血预适应后心肌水肿与水通道Aquaporin-1蛋白表达变化的关系

目的通过对缺血预适应动物模型与单纯心肌缺血动物模型之间的对照研究,探讨预适应对心肌细胞膜水通道蛋白Aquaporin-1表达的影响及与心肌水肿的关系。方法以Real-time PCR及Western blotting了解在心肌组织AQP1基因转录及蛋白表达的动态变化趋势;采用Evan blue定量测定法了解心肌组织中微血管通透性的变化及用心肌水含量测定法了解缺血心肌的水肿程度。结果与缺血对照组相似,缺血预适应后心肌AQP1基因及其蛋白的表达呈现先减后增的趋势,但增加的程度较对照组为高。预适应后组织血管通透性增高明显受到抑制,但仅伴随着缺血后早期阶段心肌水肿的减轻。与微血管通透性的持续降低形成对比的同时,心肌水肿状态在之后一段时期内保持较高水平与AQP1蛋白表达增高在时间关系上相对应。结论预适应早期心肌水肿的减轻与血管通透性的抑制有关,而AQP1蛋白表达的增加可能是心肌水肿状态维持的因素。

Effects of shenmai injection on pulmonary aquaporin 1 in rats following traumatic brain injury

Background Aquaporin-1 （AQP1） has involved in fluid transport in diverse pulmonary edema diseases. Our study aimed to explore the dynamic changes of AQP1 in pulmonary water metabolism in rats following traumatic brain injury （TBI） and the protective effect provided by shenmai injection.Methods Sixty male Sprague Dawley rats weighting 280-300 g were randomly divided into three groups： the normal control group, the model group and the shenrnai injection （SMI） group. One piece skull was taken away without injuring cerebral tissue in normal control group, while rats in model group and SMI group were subject to free fall injury in the cerebral hemisphere. Rats in model group received intraperitoneal normal sodium （15 mi/kg） at one hour post-injury and the same dose of shenmai injection instead in SMI group, respectively. The expression of AQP1 was detected by immunohistochemical analysis and semi-quantitative RT-PCR at 0 hour, 10 hours, 72 hours and 120 hours after TBI.Arterial blood gas analysis and lung wet to dry were also measured.Results AQP1 was mainly presented in the capillary endothelium and slightly alveolar epithelial cells in three groups, but the expression of AQP1 in the normal control group was positive and tenuous, weakly positive in the model and SMI groups,respectively. Compared with normal control group, AQP1 mRNA levels were down regulated in the model and SMI groups at 10 hours, 72 hours and 120 hours （P ￡1/40.05）. While AQP1 mRNA levels in the SMI group was up-regulated than that in the model group （P￡1/40.05）. Lung wet to dry weight ratio （W/D） in the model and SMI groups at 10 hours were higher than that in normal control group （P ￡1/40.05）. Compared with normal control group, PaO2 was markedly lower in the model and SMI groups （P ￡1/40.05）, but there were no statistically significant differences between model and SMI groups （P ￡3/40.05）.Conclusions The decreased AQP1 expression may be involved in the increased lung water content and dysfunction of pulmonary water metabolism following TBI. The treatment with SMI could improve water metabolism by promoting AQP1 expression.

Aquaporin-1 mRNA在人非小细胞肺癌组织中的表达和意义

目的:探讨Aquaporin-1(AQP1)mRNA在人非小细胞肺癌组织中的表达和意义。方法:以相应患者手术切除的正常肺组织为对照,采用半定量RT-PCR技术检测人非小细胞肺癌(17例鳞癌和18例腺癌)组织中AQP1 mRNA的表达水平。结果:人肺腺癌组织中AQP1 mRNA表达水平为0.419±0.135,高于正常肺组织中的表达水平(0.250±0.124),二者之间差异有统计学意义(P<0.05);人肺鳞癌组织中AQP1 mRNA表达水平为0.341±0.099,与正常肺组织中AQP1 mRNA表达水平(0.264±0.114)之间无统计学差异(P>0.05)。结论:AQP1mRNA在人肺腺癌组织中表达增加,提示AQP1可能与人肺腺癌的发生和发展有关系。

Aquaporin1～9 mRNA在成人大肠黏膜中的表达

明确Aquaporin基因各亚型(aqps)mRNA在成人大肠黏膜的表达,探讨aqps在正常大肠生理中的作用.以RT-PCR方法分别检测左半结肠、右半结肠黏膜各10例标本中1～9共9个亚型mRNA的表达情况.结果示aqp6在左、右半结肠均未见有表达,1、2、3、4、5、7、8、9 mRNA在左右半结肠黏膜均有表达,aqp9在左半结肠表达更丰富.结论:成人大肠黏膜中多种水通道蛋白的表达提示aqps尤其aqp9与大肠的水分吸收、黏液分泌等有密切关系.

血清AQP-1联合脑电双频指数对颅脑损伤患者病情严重程度和预后的评估

目的探讨血清水通道蛋白-1(AQP-1)联合脑电双频指数(BIS)对颅脑损伤(TBI)患者病情严重程度和预后的评估价值。方法选取2018-01—2021-12赤峰市医院收治的125例TBI患者为TBI组,根据格拉斯哥昏迷量表(GCS)分为轻度组51例,中度组42例,重度组32例,根据90 d格拉斯哥预后量表分为预后不良组和预后良好组,选取同期60名健康体检者为对照组。收集TBI患者临床资料,检测血清AQP-1水平和监测BIS。分析TBI患者血清AQP-1水平和BIS与GCS评分的相关性及AQP-1水平和BIS与TBI患者预后的不良关系和评估价值。结果TBI组血清AQP-1水平高于对照组(P<0.05)。轻度组、中度组、重度组血清AQP-1水平依次升高,BIS依次降低(P均<0.05)。Spearman相关性分析显示,TBI患者GCS评分与血清AQP-1水平呈负相关,与BIS呈正相关(rs=-0.829、0.855,P均<0.001)。随访90 d,125例TBI患者预后不良发生率为26.40%(33/125)。多因素Logistic回归分析显示,GCS评分(OR=0.697,95%CI:0.569~0.854)、BIS(OR=0.705,95%CI:0.590~0.843)增加为TBI患者预后不良的独立保护因素,中线移位≥5 mm(OR=4.568,95%CI:1.200~17.387)、基底池异常(OR=3.620,95%CI:1.092~12.002)和AQP-1(OR=1.115,95%CI:1.023~1.215)升高为其独立危险因素(P均<0.05)。ROC曲线分析显示,血清AQP-1联合BIS(AUC=0.837,95%CI:0.760~0.897)评估TBI患者预后不良的曲线下面积(AUC)大于AQP-1(AUC=0.759,95%CI:0.674~0.831)、BIS(AUC=0.769,95%CI:0.685~0.840)单独评估(P均<0.05)。结论血清AQP-1水平升高和BIS降低与TBI患者病情加重和预后不良有关,血清AQP-1联合BIS评估TBI患者预后不良的价值较高。

孕中期水通道蛋白1、白细胞介素37对高风险孕妇发生子痫前期的预测

目的探讨孕中期水通道蛋白1(AQP1)、白细胞介素37(IL-37)对高风险孕妇发生子痫前期的预测价值。方法选取2020年1月—2020年12月连云港市第一人民医院收治的70例孕早期预测有子痫前期的高风险孕中期孕妇作为研究对象,将其中22例发生子痫前期的孕妇分为子痫前期组,48例未发生子痫前期且血压维持正常的孕妇分为非子痫前期组,另选取同期在连云港市第一人民医院体检的30名健康非高风险孕妇作为对照组。对比三组孕妇孕中期AQP1、IL-37表达水平,应用受试者操作特征(ROC)曲线分析AQP1、IL-37对高风险孕妇发生子痫前期的预测价值。对所有产妇进行随访,记录70例有子痫前期高风险孕妇产后新生儿情况,将20例羊水污染程度为Ⅲ度、胎儿胎心率超过180次/min、新生儿Apgar评分<7分的产妇分为妊娠结局不良组,将其余的50例产妇分为妊娠结局良好组,对比两组产妇一般临床特征和孕中期相关临床指标,应用Logistic回归分析分析AQP1、IL-37对子痫前期不良妊娠结局的预测价值。结果三组孕妇孕中期AQP1、IL-37表达水平对比,子痫前期组明显高于非子痫前期组与对照组,差异有统计学意义(P<0.05);AQP1、IL-37两者联合对子痫前期的预测灵敏度和特异度明显高于AQP1、IL-37单一预测,差异有统计学意义(P<0.05),通过预测最高阈值和最低阈值计算出预测平均阈值,AQP1的预测阈值为14.58μg/L,IL-37为234.62 pg/mL;不良妊娠结局组与良好妊娠结局组孕妇年龄、身体质量指数、妊娠次数、产次、高血压家族史、妊娠前高血压史对比,差异无统计学意义(P>0.05),孕中期DBP、SBP、尿蛋白、AQP1、IL-37水平对比,差异有统计学意义(P<0.05);Logistic回归分析结果表明:尿蛋白、AQP1、IL-37是子痫前期高风险孕妇不良妊娠结局的独立影响因素(P<0.05)。结论孕中期AQP1、IL-37水平对高风险孕妇子痫前期具有重要预测价值,且其预测阀值分别为14.58μg/L、234.62 pg/mL,且两者联合的预测效能更高。同时,孕中期AQP1、IL-37也能够预测子痫前期高风险孕妇不良妊娠结局的发生,因此临床需要针对孕中期AQP1、IL-37水平升高的产妇进行相关干预,预防不良结局发生。