水位下降对若尔盖泥炭地垂直剖面土壤甲烷产生及厌氧氧化潜势的影响

泥炭地是主要的甲烷（CH₄）排放源,甲烷循环过程对水位变化响应敏感。研究选取两块具有水位差异的泥炭地土壤,通过厌氧培养实验探究水位变化对泥炭地甲烷产生和甲烷厌氧氧化（Methane Anaerobic Oxidation,AOM）潜势的影响,并分析影响其潜势大小的生物地球化学因子。结果显示,高水位泥炭地（0 cm） CH₄产生累积量为（0.89±0.01）μg/g,要显著高于低水位（-30 cm：（0.70±0.03）μg/g）泥炭地甲烷产生量,但低水位AOM累积量要显著高于高水位泥炭地（0 cm：（2829.93±35.99）μg/g）,低水位泥炭地AOM量为（3588.06±24.78）μg/g。通过相关性分析发现甲烷产生潜势与含水量和DOC具有显著相关性,AOM潜势与含水量、pH、DOC具有显著相关性,含水量和DOC是影响若尔盖泥炭地甲烷产生及AOM潜势大小的重要因子。此外,发现高水位泥炭地甲烷产生潜势对温度升高的响应较为明显,特别是表层土壤（0-20 cm）。本研究明确了水位变化对若尔盖泥炭地甲烷产生及AOM潜势的影响特征,估算了全国泥炭地甲烷产生及AOM潜势的大小,以期为减缓全球气候变暖提供一定的理论支撑。     

The impacts of climate change and human activities on biogeochemical cycles on the Qinghai‐Tibetan Plateau

With a pace of about twice the observed rate of global warming, the temperature on the Qinghai‐Tibetan Plateau (Earth's ‘third pole’) has increased by 0.2 °C per decade over the past 50 years, which results in significant permafrost thawing and glacier retreat. Our review suggested that warming enhanced net primary production and soil respiration, decreased methane (CH₄) emissions from wetlands and increased CH₄ consumption of meadows, but might increase CH₄ emissions from lakes. Warming‐induced permafrost thawing and glaciers melting would also result in substantial emission of old carbon dioxide (CO₂) and CH₄. Nitrous oxide (N₂O) emission was not stimulated by warming itself, but might be slightly enhanced by wetting. However, there are many uncertainties in such biogeochemical cycles under climate change. Human activities (e.g. grazing, land cover changes) further modified the biogeochemical cycles and amplified such uncertainties on the plateau. If the projected warming and wetting continues, the future biogeochemical cycles will be more complicated. So facing research in this field is an ongoing challenge of integrating field observations with process‐based ecosystem models to predict the impacts of future climate change and human activities at various temporal and spatial scales. To reduce the uncertainties and to improve the precision of the predictions of the impacts of climate change and human activities on biogeochemical cycles, efforts should focus on conducting more field observation studies, integrating data within improved models, and developing new knowledge about coupling among carbon, nitrogen, and phosphorus biogeochemical cycles as well as about the role of microbes in these cycles.     

铜尾矿废弃地土壤动物多样性特征

土壤动物的恢复、群落演替及其多样性对于铜尾矿废弃地的生态重建具有重要意义.为了解铜尾矿废弃地土壤动物群落多样性特征,在铜陵市铜尾矿区设置4个样地23采样点,共捕获土壤动物4622只个体,隶属5门10纲18目29类.结果表明,铜尾矿自然废弃地与其对照组土壤动物多样性差异明显,自然废弃地土壤动物丰富度指数d、大型土壤动物密度、中小型土壤动物密度、多样性指数H'和D·G指数均小于其对照组且存在显著差异.而复垦废弃地中小型土壤动物密度和D·G指数小于其对照组且存在显著差异,多样性指数H'大于其对照组且差异极显著,其他土壤动物群落指标与其对照组均无显著差异.相似系数q表明,外围林地间土壤动物群落相似性最大,其次是复垦废弃地与外围林地间,自然废弃地与其它3个样地间相似性最小.从垂直分层来看,复垦废弃地土壤动物表聚性强于自然废弃地,尾矿废弃地表聚性强于外围林地.灰色关联分析表明,铜尾矿区土壤理化性质与土壤动物群落结构指标关系密切,其中最重要的因素是土壤含水量和总钾含量,重金属全镉含量也不容忽视,植被因素和土壤全铜含量对土壤动物的影响相对较小.由此可见,土壤含水量、土壤基质的优劣、土壤有机质与营养元素的含量等因素限制了铜尾矿废弃地土壤动物的恢复与重建,而这些因素的改善主要归功于尾矿废弃地的土地复垦和作物种植.所以,尾矿废弃地的复垦与利用有利于土壤动物的恢复与重建.     

Post-translational modifications of protein in response to ionizing radiation

Based on central dogma of genetics, protein is the embodiment and executor of genetic function, post-translational modifications (PTMs) of protein are particularly important and involved in almost all aspects of cell biology and pathogenesis. Studies have shown that ionizing radiation (IR) alters gene expression much more profoundly and a broad variety of cell-process pathways, lots of proteins are modified and activated. Our understanding of the protein in response to ionizing radiation is steadily increasing. Among the various biological processes known to induce radioresistance, PTMs have attracted marked attention in recent years. The present review summarizes the latest knowledge about how PTMs response to ionizing radiation and pathway analysis were conducted. The data provided insights into biological effects of IR and contributing to the development of novel IR-based strategies.     

TGF-β1对话Hedgehog-Gli1信号调控肾小管上皮细胞表型转化和胶原累积

该研究旨在探讨Hedgehog-Gli1(HH)信号在肾小管上皮细胞表型转化(epithelial-mesenchymal transition,EMT)和胶原累积中的作用及与TGF-β1信号的对话机制。该实验通过体外培养大鼠肾小管上皮细胞NRK-52E,以溶剂作为对照组,以1~50 ng/m L重组蛋白sonic hedgehog(Shh)或5 ng/m L TGF-β1作为诱导组,以加入或不加入HH信号特异性阻断剂环靶明(cyclopamine,Cyp)5μmol/L为干预组。细胞培养24 h,采用ELISA、q RT-PCR、免疫细胞荧光染色和Western blot等方法检测HH信号相关分子(Ptch1、Smo和Gli1)、TGF-β1、EMT相关分子(Rac1蛋白、肌成纤维细胞标志物α-SMA和上皮细胞标志物E-cadherin)、III型胶原m RNA或蛋白的表达。结果发现,外源性Shh上调Smo和Gli1表达,抑制Ptch1表达,继而激活HH信号;HH信号活化抑制肾小管上皮细胞E-cadherin的表达,上调α-SMA、III型胶原和TGF-β1的表达。环靶明干预后,Smo表达下调,进而抑制HH信号、EMT和胶原累积,并下调TGF-β1的表达。应用TGF-β1诱导小管上皮细胞EMT,同时也上调HH信号分子Smo和Gli1的表达,下调Ptch1的表达,提示TGF-β1可诱导HH信号活化。综上所述,HH信号和TGF-β1均参与了肾小管上皮细胞EMT和胶原累积过程。HH信号活化可促进TGF-β1的表达,同时TGF-β1能激活HH信号,推测TGF-β1与HH信号可能存在交叉对话以调控EMT和胶原累积。     

Two new scorpionates vanadium haloperoxidases model complexes: synthesis and structure of VO(O2)(pzH)(HB(pz)3) and VO(O2)(pzH)(B(pz)4) (pzH = pyrazole(C3H4N2))

Using vanadate, poly(1H-pyrazol-1-yl)borate and pyrazole as starting materials, two new neutral peroxovanadium(V) complexes with poly(1H-pyrazol-1-yl)borate, VO(O(2))(pzH)(HB(pz)(3))(1) and VO(O(2))(pzH)(B(pz)(4))(2), were synthesized successfully. Both complexes were characterized by elemental analysis, IR, UV-vis and NMR spectra. And the structure of complex 1 was determined by X-ray diffraction, which is somewhat relevant for haloperoxidase enzymes. Cytotoxic effects also are discussed on 3T3 cell proliferation. In the concentration range (0.1-100mumol), both complexes have an inhibiting cellular proliferation effect. When the cells cultivated with the complexes at high dose, the toxicity effect of both complexes is more and more predominant.     

Novel Function and Intracellular Localization of Methionine Adenosyltransferase 2β Splicing Variants

Human methionine adenosyltransferase 2β (MAT2β) encodes for two major splicing variants, V1 and V2, which are differentially expressed in normal tissues. Both variants are induced in human liver cancer and positively regulate growth. The aim of this work was to identify interacting proteins of V1 and V2. His-tagged V1 and V2 were overexpressed in Rosetta pLysS cells, purified, and used in a pulldown assay to identify interacting proteins from human colon cancer cell line RKO cell lysates. The eluted lysates were subjected to Western blot and in solution proteomic analyses. HuR, an mRNA-binding protein known to stabilize the mRNA of several cyclins, was identified to interact with V1 and V2. Immunoprecipitation and Western blotting confirmed their interaction in both liver and colon cancer cells. These variant proteins are located in both nucleus and cytoplasm in liver and colon cancer cells and, when overexpressed, increased the cytoplasmic HuR content. This led to increased expression of cyclin D1 and cyclin A, known targets of HuR. When endogenous expression of V1 or V2 is reduced by small interference RNA, cytoplasmic HuR content fell and the expression of these HuR target genes also decreased. Knockdown of cyclin D1 or cyclin A blunted, whereas knockdown of HuR largely prevented, the ability of V1 or V2 overexpression to induce growth. In conclusion, MAT2β variants reside mostly in the nucleus and regulate HuR subcellular content to affect cell proliferation.     

Dual roles of Atg8-PE deconjugation by Atg4 in autophagy

Modification of target molecules by ubiquitin or ubiquitin-like (Ubl) proteins is generally reversible. Little is known, however, about the physiological function of the reverse reaction, deconjugation. Atg8 is a unique Ubl protein whose conjugation target is the lipid phosphatidylethanolamine (PE). Atg8 functions in the formation of double-membrane autophagosomes, a central step in the well-conserved intracellular degradation pathway of macroautophagy (hereafter autophagy). Here we show that the deconjugation of Atg8-PE by the cysteine protease Atg4 plays dual roles in the formation of autophagosomes. During the early stage of autophagosome formation, deconjugation releases Atg8 from non-autophagosomal membranes to maintain a proper supply of Atg8. At a later stage, the release of Atg8 from intermediate autophagosomal membranes facilitates the maturation of these structures into fusion-capable autophagosomes. These results provide new insights into the functions of Atg8-PE and its deconjugation.     

我国土壤动物群落生态学研究综述

总结了我国土壤动物群落生态学研究的特点,即区域分布集中于中国东部、研究的生态系统类型广泛、研究角度多种多样与应用研究发展迅速。并从土壤动物群落与环境关系、土壤动物群落的组成和多样性、土壤动物群落结构、土壤动物群落功能、土壤动物群落演替与受干扰生态系统的土壤动物群落6个方面综述其最新研究成果。在此基础上指出我国土壤动物群落生态学中有待开拓的研究领域是基础研究、特色区域和生态系统的研究、土地覆盖/土地利用对土壤动物的影响研究、土壤动物多样性及其保护研究、土壤动物在土壤生态系统和陆地生态系统物质循环和能量流动中的作用研究、全球变化响应研究与土壤动物应用研究。