The BNIP-2 and Cdc42GAP Homology (BCH) Domain of p50RhoGAP/Cdc42GAP Sequesters RhoA from Inactivation by the Adjacent GTPase-activating Protein Domain

The BNIP-2 and Cdc42GAP homology (BCH) domain is a novel regulator for Rho GTPases, but its impact on p50-Rho GTPase-activating protein (p50RhoGAP or Cdc42GAP) in cells remains elusive. Here we show that deletion of the BCH domain from p50RhoGAP enhanced its GAP activity and caused drastic cell rounding. Introducing constitutively active RhoA or inactivating GAP domain blocked such effect, whereas replacing the BCH domain with endosome-targeting SNX3 excluded requirement of endosomal localization in regulating the GAP activity. Substitution with homologous BCH domain from Schizosaccharomyces pombe, which does not bind mammalian RhoA, also led to complete loss of suppression. Interestingly, the p50RhoGAP BCH domain only targeted RhoA, but not Cdc42 or Rac1, and it was unable to distinguish between GDP and the GTP-bound form of RhoA. Further mutagenesis revealed a RhoA-binding motif (residues 85-120), which when deleted, significantly reduced BCH inhibition on GAP-mediated cell rounding, whereas its full suppression also required an intramolecular interaction motif (residues 169-197). Therefore, BCH domain serves as a local modulator in cis to sequester RhoA from inactivation by the adjacent GAP domain, adding to a new paradigm for regulating p50RhoGAP signaling.     

人酸性成纤维细胞生长因子神经营养作用的初步研究

本实验研究了人酸性成纤维细胞生长因子(haFGF)的体外神经营养作用。结果表明,haFGF在体外能明显促进鸡胚(E-8)脊髓组织神经突起的生长,并能明显改变新生大鼠脑星形胶质细胞的形态,使扁平、多角形紧密联接的细胞转化为具有纤维样突起的胶质细胞,同时对胶质细胞DNA合成也有一定促进作用。实验还证明,haFGF可增加体外培养新生大鼠海马神经元的存活,且大大增加神经元胞体体积及突起长度。     

中华眼镜蛇蛇毒因子(CVF)对补体系统的作用及与人补作C_3和其他蛇毒抗原性关系

中华眼镜蛇蛇毒经DEAE-Sepharose CL-6B。HPLC等多次柱层析分离出有抗补体及溶血活性的眼镜蛇蛇毒因子(Cobra venom factor,CVF),纯化后的CVF在聚丙烯酰胺凝胶电泳图谱上呈单一区带,分子量为225000—230000,等电点为6.20。用二硫苏糖醇还原经SDS-聚丙烯酰胺凝胶电泳得三类亚基,其分子量总和为237,000。 体外抗补体及溶血试验表明,CVF的作用是通过补体旁路途经使总补体活力下降。双向免疫电泳鉴定,发现CVF与人血清作用后,其中补体成分C_3分子的抗原性发生改变,则表明CVF的作用是通过激活补体成分C_3而发挥的。给豚鼠腹腔注射CVF(0.15ug/g体重)后,其血清总补体水平下降到正常值的3％以下,7天后回升,13天后恢复到正常水平。 单相免疫电泳表明,CVF与人补体C_3抗血清间无任何交叉免疫反应,但人血清与CVF抗血清间有微弱的免疫沉淀反应。另外,CVF的氨基酸组成与人补体C_3也较为相似。鉴定还表明眼镜蛇科中四种蛇毒与CVF抗血清有强烈的免疫沉淀反应,蝰蛇毒及海蛇毒也有免疫沉淀反应,但只有眼镜蛇毒具有抗补体活性。     

pCMBS对完整红细胞膜阴离子通透性的影响

根据等渗ＮＨ４Ｃｌ溶血动力学,探讨了ｐＣＭＢＳ（对氯汞苯磺酸）对完整红细胞膜阴离子通透性的影响．０．０５ｍｍｏｌ／ＬｐＣＭＢＳ使阴离子通透系数Ｐｃｌ下降为对照的８６．５％;１．０ｍｍｏｌ／Ｌ以上浓度时Ｐｃｌ值反而变大。ｐＣＭＢＳ浓度高于０．３ｍｍｏｌ／Ｌ时,细胞悬浮液在１０ｓ之前光密度下降过快,偏离理论拟合方程且不受ＤＩＤＳ抑制．半胱氨酸对ｐＣＭＢＳ引起的效应有恢复作用。结果表明ｐＣＭＢＳ和股骨架蛋白上特殊－ＳＨ基相互作用,导致ｂａｎｄ３构象改变,致使改变膜时阴离子的通透性。     

毛乌素沙地油蒿叶性状对光能利用效率动态的影响

目前对于荒漠灌木光能利用效率（LUE）的季节变异及其调控因素,尤其是其生物调控因素的认识非常有限,导致了荒漠生态系统生产力模型的不确定性。拟验证假设：长期干旱环境下,典型荒漠灌木油蒿光能利用效率日均值（LUE_day）的动态变化与叶片性状的季节性调整有关。试验采用Li-6400便携式光合仪定期测量了油蒿生长季叶片LUE_day的季节动态及相关叶性状指标,探究叶性状对LUE_day的影响。结果表明：LUE_day的季节波动范围为0.003-0.017 mol/mol,整体变异系数（CV）为38.75%。完全展叶期LUE_day均值相比生长季平均值降低17.37%,相比展叶期和落叶期时降低30%;8个叶性状的季节变异幅度差异较大,其中总叶绿素含量（Chl）、类胡萝卜素含量（Car）和叶氮含量（LNC）均表现出较大的季节变异性（CV ≥ 20%）,叶碳含量（LCC）和叶片相对含水量（LRWC）的变异程度最低（CV<7%）。LRWC与所有叶片化学性状（Chl、Chl a/b、Car、LNC和LCC）均存在显著相关,表明其变化与叶片的养分吸收、光合色素合成以及碳同化的运输过程密切相关;油蒿LUE_day的相对变化与LRWC、Chl a/b和LNC显著正相关,而LRWC和LNC的季节动态受空气温度（T_a）和土壤含水量（VWC）的共同调节,Chl a/b的季节波动主要由浅层土壤含水量（10 cm VWC）控制。以上研究结果强调,在未来预计极端的气候事件（如极端干旱和持续热浪事件）发生更频繁的旱地场景中,时间尺度植物叶性状对于土壤干旱和高温的适应性调整应当被充分考虑到旱地生态系统的通量建模方案中。该结果将为构建叶片尺度的光合生理模型与厘清LUE的生物调控机制提供理论依据。     

生长抑素受体2的小鼠时空组织表达谱

生长抑素(somatostatin, SST)作为一种抑制性多肽激素,在多种生物过程中发挥重要的功能。生长抑素受体2 (somatostatin receptor 2, SSTR2)作为生长抑素表达最广泛的受体在多种组织中表达,但其表达的具体细胞类型尚不清楚。本研究在小鼠不同发育阶段的多种组织中鉴定了SSTR2蛋白表达的细胞类型。通过多色免疫荧光在小鼠胚胎期15.5 d、出生后1 d、7 d、15 d、3个月和6个月的脑、骨、肺、肠道、皮肤、胃、脾和肾等组织中检测了Sstr2基因的表达。结果发现Sstr2在不同发育阶段的多种组织的特定细胞类型中表达,包括脑神经元和星形胶质细胞,骨的间充质基质细胞、造血细胞和B细胞,肺的巨噬细胞、Ⅱ型肺泡上皮细胞和气道纤毛细胞,肠道的上皮细胞和神经元,皮肤的毛囊细胞,胃体的上皮细胞,脾的造血干细胞、造血祖细胞和神经纤维,肾的肾小管上皮细胞等。本研究确定了小鼠多组织不同发育阶段Sstr2表达的细胞类型,为生长抑素与生长抑素受体2的生理功能研究提供了新的线索。     

植物根际促生菌促生特性研究进展

根际微生物组是决定农作物健康状况的关键因素之一,也是调节农作物与生物和非生物环境相互作用的重要因素。植物根际促生菌(plant growth-promoting rhizobacteria, PGPR)为农作物宿主提供了多种有益作用,通过化学交流以复杂的方式与农作物、土壤相互作用,进而促进农作物生长。本文综述了PGPR对农作物的促生机制、PGPR与农作物的互作及其在农业实践中的应用,并展望了PGPR在农业实践中应用的发展趋势,以期为今后PGPR的应用和研究提供新的思路和理论支撑。     

The dependency of fetal left ventricular biomechanics function on myocardium helix angle configuration

The helix angle configuration of the myocardium is understood to contribute to the heart function, as finite element (FE) modeling of postnatal hearts showed that altered configurations affected cardiac function and biomechanics. However, similar investigations have not been done on the fetal heart. To address this, we performed image-based FE simulations of fetal left ventricles (LV) over a range of helix angle configurations, assuming a linear variation of helix angles from epicardium to endocardium. Results showed that helix angles have substantial influence on peak myofiber stress, cardiac stroke work, myocardial deformational burden, and spatial variability of myocardial strain. A good match between LV myocardial strains from FE simulations to those measured from 4D fetal echo images could only be obtained if the transmural variation of helix angle was generally between 110 and 130°, suggesting that this was the physiological range. Experimentally discovered helix angle configurations from the literature were found to produce high peak myofiber stress, high cardiac stroke work, and a low myocardial deformational burden, but did not coincide with configurations that would optimize these characteristics. This may suggest that the fetal development of myocyte orientations depends concurrently on several factors rather than a single factor. We further found that the shape, rather than the size of the LV, determined the manner at which helix angles influenced these characteristics, as this influence changed significantly when the LV shape was varied, but not when a heart was scaled from fetal to adult size while retaining the same shape. This may suggest that biomechanical optimality would be affected during diseases that altered the geometric shape of the LV.