PMCA1-4及其A端和C端剪接变异体在成年大鼠前庭组织中的表达

目的研究质膜钙ATP酶异构体1-4(plasma membrane Ca^(2+)-ATPase 1-4,PMCA1-4)在成年大鼠前庭组织的分布部位,及其A端和C端剪接变异体的表达类型。方法选择8周龄健康SD大鼠,解剖出内耳器官行前庭切片,同时取前庭椭圆囊斑和球囊斑提取总RNA。通过免疫荧光方法检测PMCA1-4在成年大鼠内耳前庭组织的表达部位,通过逆转录聚合酶链反应(RT-PCR)法检测PMCA1-4的A端和C端剪接变异体在成年大鼠前庭组织的表达类型。结果球囊和椭圆囊荧光染色切片中,于毛细胞和支持细胞的胞体外侧膜可见PMCA1表达,毛细胞纤毛中可见PMCA2强表达,毛细胞和支持细胞的胞体外侧膜可见PMCA3弱表达,PMCA4几乎不表达。4种PMCA亚型在球囊表达的剪接体分别为PMCA1x/b、PMCA2w/b、PMCA3z/(a,b)和PMCA4x/b,它们在椭圆囊的表达类型与球囊相同。结论PMCA1-4在成年大鼠前庭器官的表达部位存在差异,这4种PMCA亚型的剪接体类型也各不相同。这种差异性可能是为了满足前庭组织和亚细胞结构域对Ca2+调节的特殊需求。

Intracellular Transport of HIV-1 Matrix Protein Associated with Viral RNA

HIV-1 matrix protein (MA) is a multifunctional structural protein localized on N terminus of Gag precursor p55. MA participates in HIV-1 assembly as membranotropic part of Gag precursor as well as an individual protein spliced from Gag early in infection. MA is found in the nuclei of infected cells and in plasma membrane, the site of virus assembly, in association with viral genome RNA. MA mutated variant M4 which contains two changed amino acids in N-terminal regions is also associated with viral RNA, but it is localized in the nuclear and cytoskeleton fractions but not in the plasma membrane suggesting that the mutant is deprived of membranotropic signal and “sticks” in the nuclei an d cytoskeleton, its previous location sites. These data allow suggesting that MA involved into transmission of viral RNA is transported to plasma membrane by cytoskeleton.

浆细胞膜糖蛋白-1基因单核苷酸多态性与冠心病的相关性研究

目的探讨浆细胞膜糖蛋白-1(plasma cell membrane glycoprotein-1,PC-1)基因的单核苷酸多态性(singlenucleotide polymorphism,SNP)与冠心病(coronary artery disease,CAD)的相关性。方法提取192例CAD患者和189例健康对照者外周血有核细胞DNA,应用荧光标记单碱基延伸分型技术及寡核苷酸微阵列芯片杂交技术检测PC-1基因的5个标签SNP:rs12528076,rs858341,rs2021966,rs9398995和rs858345。结果 rs9398995基因型中CAD组的TT型频率显著高于对照组,CC型频率显著低于对照组,两组间T和C等位基因频率差异有统计学意义(P<0.05)。rs12528076基型型中CAD组的TC型频率显著高于对照组(P<0.05)。由rs12528076、rs9398995和rs2021966构建的单倍型中,CCC和CTC的单倍型频率在两组间具有统计学差异(P<0.05)。结论 PC-1基因的rs12528076、rs9398995和rs2021966多态性与CAD相关。

骨骼肌组织中浆细胞膜糖蛋白-1与妊娠期糖尿病发病关系的研究

目的:探讨妊娠期糖尿病(GDM)患者骨骼肌组织浆细胞膜糖蛋白-1(PC-1)表达与GDM发病的关系。方法:用Western blot及免疫沉淀法测定GDM20例患者(GDM组)、糖耐量正常孕妇20例(正常妊娠组)及糖耐量正常非孕妇女12例(对照组)骨骼肌组织PC-1、胰岛素受体的表达水平及其基础酪氨酸磷酸化水平和胰岛素刺激后胰岛素受体酪氨酸磷酸化程度。用葡萄糖氧化酶法及放射免疫法测定空腹血葡萄糖(FPG)及空腹血胰岛素(FINS)水平,计算胰岛素抵抗指数(HOMA-IR)。结果:(1)GDM组FPG、FINS、HOMA-IR均明显高于正常妊娠组(P<0.01);正常妊娠组FINS、HOMA-IR明显高于对照组(P<0.01);(2)GDM组PC-1表达水平为1.22±0.02,明显高于正常妊娠组的0.71±0.03及对照组的0.43±0.02(P<0.01);(3)各组胰岛素受体表达水平及基础酪氨酸磷酸化程度比较,差异均无显著性(P>0.05)。胰岛素刺激后酪氨酸磷酸化程度,GDM组为0.17±0.04明显低于正常妊娠组的0.24±0.02(P<0.01),正常妊娠组明显低于对照组的0.31±0.03(P<0.01);(4)正常妊娠组、GDM组PC-1表达水平与HOMA-IR呈明显正相关(r=0.611、0.734,P<0.01),与胰岛素刺激后胰岛素受体酪氨酸磷酸化呈负相关(r=-0.531、-0.522,P<0.05)。结论:骨骼肌组织PC-1高表达可能是妊娠期糖尿病患者胰岛素抵抗的分子机制之一,PC-1可能通过抑制胰岛素受体酪氨酸磷酸化发挥作用。

PC-1基因K121Q多态性与OSAHS相关性研究

目的:探讨浆细胞膜糖蛋白1(plasma cell membrane glycoprotein-1,PC-1)基因K121Q多态性与中国汉族人的阻塞性睡眠呼吸暂停低通气综合征(obstructive sleep apnea hypopnea syndrome,OSAHS)发病关系。方法:应用聚合酶链反应和限制性片段长度多态性方法,对入选上海地区420例汉族OSAHS患者和190例对照组进行PC-1基因K121Q多态性分型及研究;分析OSAHS患者K121Q多态性与其临床指标(血压、生化指标、人体测量学等)的关系和与高脂血症的危险因素之间的关系。结果:OSAHS患者和对照组PC-1基因K121Q多态性基因型及等位基因频率差异无统计学意义(P>0.05);不同性别和严重程度的OSAHS患者与对照组的基因型频率分布、等位基因频率分布差异无统计学意义(P>0.05);OSAHS患者不同基因型间ApoA-1的协方差分析显示差异有统计学意义(P=0.006)。不同基因型的OSAHS患者中伴高脂血症的患者差异无统计学意义(OR=0.935,P=0.786,95%CI为0.575～1.520)。结论:PC-1基因K121Q多态性与OSAHS发病无关,与不同性别OSAHS发病及OSAHS严重程度无关。121Q等位基因不是OSAHS患者发生高脂血症的风险因素,但121Q等位基因的OSAHS患者的ApoA-1水平显著增高。

ENPP1/PC-1 Gene K121Q Polymorphism Is Associated with Obesity in European Adult Populations: Evidence from A Meta-Analysis Involving 24 324 Subjects

Objective Findings from the previous studies have suggested a relationship between ectonucleotide pyrophosphatase /phosphodiesterase 1 （ENPP‐1） or plasma cell membrane glycoprotein 1 （PC‐1） gene single nucleotide polymorphism （K121Q, rs1044498） and genetic susceptibility to obesity. However, such relationship is not reproduced by some currently available studies. In this context, the present study is aimed to quantitatively analyze the association of K121Q variant with obesity in all published case‐control studies in European adult populations. Methods Published literature from PubMed, EMBASE, and ISI web of science databases were retrieved. The studies evaluating the association of ENPP1/PC1 gene K121Q polymorphism with obesity were included, in which sufficient data were presented to calculate the odds ratio （OR） with 95% confidence intervals （CIs）. Results Ten case‐control studies meeting the inclusion criteria identified a total of 24,324 subjects including 11,372 obese and 12,952 control subjects. The meta‐analysis results showed a statistically significant association of K121Q with obesity [OR （95%CI）： 1.25 （1.04‐1.52） P=0.021] under a recessive model of inheritance （QQ vs. KK＋KQ） without heterogeneity or publication bias. Conclusions The results from the present study have indicated that ENPP1/PC1 Q121 variant may increase the risk of obesity and that more well‐designed studies based on a larger population will be required to further evaluate the role of ENPP1/PC1 gene K121Q polymorphism in obesity and other related metabolic syndromes.

2型糖尿病伴肥胖患者解偶联蛋白3基因及浆细胞膜蛋白-1基因的表达研究

目的探讨解偶联蛋白3(UCP3)基因、浆细胞膜蛋白-1(PC-1)基因在2型糖尿病(T2DM)伴肥胖患者中的表达。方法收集本院2018年6—12月120例T2DM伴肥胖患者、120例T2DM非肥胖患者、120例肥胖患者、120例非T2DM非肥胖健康者的临床资料。采用聚合酶链反应和限制性内切酶片段长度多态性(PCR-RFLP)检测UCP3Tyr210Tyr(C-T)多态性基因型及PC-1基因第4外显子121位谷氨酰胺/赖氨酸多态性。记录腰臀比(WHR)、血压、血清总胆固醇(TC)、空腹血糖(FBG)、餐后2 h血糖(2 hPG)等指标,检测患者相关基因型。结果非T2DM非肥胖健康组与肥胖组(x^(2)=6.452,RR=5.290,P=0.016)、T2DM非肥胖组(x^(2)=4.658,RR=4.260,P=0.028)、T2DM伴肥胖组(x^(2)=10.982,RR=9.280,P=0.002)的差异均有统计学意义,其中T2DM伴肥胖群体具有PC-1 Q等位基因而肥胖的相对危险性是非糖尿病非肥胖群体的9.28倍。结论UCP3基因与T2DM伴肥胖无相关性,PC-1基因中Q等位基因是胰岛素抵抗的易感基因。应对T2DM伴肥胖家族史的人群进行早期诊断,指导其改变生活方式,改善患者预后。

PC-1与胰岛素抵抗和阻塞性睡眠呼吸暂停低通气综合征的关系

阻塞性睡眠呼吸暂停低通气综合征（obstructive sleep apnea hypopnea syndrome，OSAHS）是一种涉及多种基因、环境因素、生长因素的复杂疾病。本文通过探讨浆细胞膜糖蛋白-1（Plasma cell membrane glycoprotein-1，PC-1）与胰岛素抵抗（Insulin resistance，IR）、OSAHS与肥胖、OSAHS的遗传分子水平研究进展、OSAHS与IR、PC-1及其基因多态与OSAHS相互间的关系，得出在控制OSAHS中IR是关键因素，而PC-1及其基因多态性的研究为IR及与其相关的OSAHS危险因素的预测和防治提供了一种新思路。希望在不久的将来可以确定OSAHS的遗传模式，并找到具体遗传物质，为其基因水平的治疗奠定基础。