颅内动脉瘤夹闭术、血管内栓塞术治疗颅内动脉瘤的疗效及安全性研究

目的:探讨颅内动脉瘤夹闭术、血管内栓塞术治疗颅内动脉瘤的疗效及安全性。方法:回顾性分析2016年9月-2019年1月接受手术治疗的76例颅内动脉瘤患者的临床资料,根据手术方式的不同分为接受颅内动脉瘤夹闭术治疗的A组40例和接受血管内栓塞术治疗的B组36例。对比两组患者的动脉瘤完全闭合率、住院费用及血清炎性因子[C反应蛋白(CRP)、白介素-1β(IL-1β)、白介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)]、脑氧饱和度水平及日常生活能力量表(ADL)评分值,记录并发症发生情况。结果:两组患者的动脉瘤完全闭合率比较差异无统计学意义(x~2=0.515,P=0.473)。A组患者的住院费用低于B组患者(t=17.732,P=0.000);A组患者术后血清中CRP、IL-1β、IL-6、TNF-α的水平高于B组(t=10.580、12.904、9.355、19.176,P均=0.000);A组患者术后脑氧饱和度水平低于B组(t=2.113,P=0.019),两组ADL评分值的差异无统计学意义(t=1.211,P=0.115);A组术中再破裂、脑血管痉挛发生率高于B组患者(x~2=4.817、5.383,P=0.028、0.020)。结论:颅内动脉瘤夹闭术应用于颅内动脉瘤患者,动脉瘤完全闭合率与血管内栓塞术无明显差异,住院费用更低,但对目标血管的刺激较大,可能存在术中再破裂、脑血管痉挛等风险。     

Three proline rotamases involved in calcium homeostasis play differential roles in stress tolerance,virulence and calcineurin regulation of Beauveria bassiana

FK506‐sensitive proline rotamases (FPRs), also known as FK506‐binding proteins (FKBPs), can mediate immunosuppressive drug resistance in budding yeast but their physiological roles in filamentous fungi remain opaque. Here, we report that three FPRs (cytosolic/nuclear 12.15‐kD Fpr1, membrane‐associated 14.78‐kD Fpr2 and nuclear 50.43‐kD Fpr3) are all equally essential for cellular Ca²⁺ homeostasis and contribute significantly to calcineurin activity at different levels in the insect‐pathogenic fungus Beauveria bassiana although the deletion of fpr1 alone conferred resistance to FK506. Radial growth, conidiation, conidial viability and virulence were less compromised in the absence of fpr1 or fpr2 than in the absence of fpr3, which abolished almost all growth on scant media and reduced growth moderately on rich media. The Δfpr3 mutant was more sensitive to Na⁺, K⁺, Mn²⁺, Ca²⁺, Cu²⁺, metal chelate, heat shock and UVB irradiation than was Δfpr2 while both mutants were equally sensitive to Zn²⁺, Mg²⁺, Fe²⁺, H₂O₂ and cell wall‐perturbing agents. In contrast, the Δfpr1 mutant was less sensitive to fewer stress cues. Most of 32 examined genes involved in DNA damage repair, Na⁺/K⁺ detoxification or osmotolerance and Ca²⁺ homeostasis were downregulated sharply in Δfpr2 and Δfpr3 but rarely so affected in Δfpr1, coinciding well with their phenotypic changes. These findings uncover important, but differential, roles of three FPRs in the fungal adaptation to insect host and environment and provide novel insight into their essential roles in calcium signalling pathway.     

纳米δ-Bi2O3负载多孔沸石球填料对水体中Cr（Ⅵ）的吸附特征及其影响因素

在水热条件下合成纳米δ-Bi2O3负载多孔沸石球填料(Bi-PZSF),研究其对水体中Cr(Ⅵ)的吸附性能(包括等温吸附、吸附动力学和吸附稳定性)以及溶解氧、pH等因素对吸附过程的影响及其吸附机理。结果表明:朗格缪尔模型和准二级动力学模型对实验结果具有良好的拟合度,在中性条件下,水体中的溶解氧含量对吸附速率影响较小,Bi-PZSF的最大吸附量为955.69 mg·kg^-1,比天然沸石的吸附量提升了近120倍;Bi-PZSF在NO3^-和SO4^2-的溶液中呈现出较强的选择吸收Cr(Ⅵ)能力,Cr(Ⅵ)去除率均在97%以上;同时,Bi-PZSF在吸附Cr(Ⅵ)后表现出高稳定性。Cr(Ⅵ)的去除主要是通过与附着在Bi-PZSF上的纳米δ-Bi2O3的表面羟基交换完成的。     

喀斯特次生林幼树更新空间分布格局及种间关联性

本研究以贵州省喀斯特典型区域紫云苗族布依族自治县撂荒30余年后自然恢复形成的次生林为对象,设置140 m×120 m固定样地,系统调查样地内幼树更新,并采用空间点格局分析方法分析幼树更新优势种群在不同空间尺度下的分布格局和种间关联性。结果表明: 调查样地中幼树共计1291株,包括39个树种,其中光皮桦、化香、马尾松、枫香和山杨5个树种的幼树个体数量总和达83.7%,重要值总和达77.8%,为幼树更新的优势树种。光皮桦、化香和枫香3个幼树优势种群的空间分布格局在0～60 m空间尺度上均呈现较强的聚集分布;马尾松和山杨2个幼树优势种群在小尺度上呈现聚集分布,大尺度上则随机分布。幼树优势种群空间关联性多呈现正关联,仅马尾松与枫香和山杨在小尺度呈现正关联,大尺度呈现不相关。调查样地5个幼树优势种群空间分布格局及种间关联性差别较大,可能与树种的生物学特性、生境及空间资源的利用密切相关。目前,林分多以先锋树种为主,群落结构不稳定;以马尾松和光皮桦为优势种群的松-桦混交林可能成为下一阶段演替方向,建议通过森林经营措施加快植被恢复进程。     

叶面喷施亚精胺对高温胁迫下番茄叶绿素合成代谢的影响

以设施番茄栽培品种‘金棚朝冠’幼苗为试验材料,研究叶面喷施0.25 mmol·L~(-1)亚精胺(Spd)对高温胁迫下(38℃/28℃,昼/夜)番茄幼苗生长及叶绿素合成过程中前体物质含量、关键酶活性和叶绿素含量的影响,探讨Spd缓解番茄高温胁迫伤害的生理机制。结果表明:(1)高温胁迫显著抑制了番茄幼苗的生长,叶面喷施Spd可有效缓解高温胁迫对番茄幼苗地上部生长的抑制作用,但对于地下部的生长无显著缓解作用。(2)高温胁迫下番茄叶片叶绿素合成前体物质δ-氨基酮戊酸(ALA)和胆色素原(PBG)的含量显著提高,而尿卟啉原Ⅲ(UroⅢ)、原卟啉Ⅸ(ProtoⅨ)、镁-原卟啉Ⅸ(Mg-protoⅨ)和原叶绿素酸(Pchl)的含量显著降低,证明叶绿素前体由PBG向UroⅢ的转化受阻,导致叶绿素a(Chla)、总叶绿素(Chlt)含量和Chla/Chlb显著降低。(3)叶面喷施Spd能增强高温胁迫下胆色素原脱氨酶(PBGD)活性,有效缓解了高温胁迫对PBG到UroⅢ转化的阻碍作用,促进PBG之后叶绿素合成前体物质的合成,Chla含量和Chla/Chlb显著增加。研究发现,高温胁迫显著抑制番茄幼苗的生长,叶面喷施Spd可通过显著增强PBGD活性来缓解由PBG向UroⅢ的受阻程度,促进高温胁迫下番茄叶片的叶绿素前体合成,提高叶绿素含量和番茄植株的生长量,减轻高温胁迫对番茄幼苗生长的伤害。     

Land masses and oceanic currents drive population structure of Heritiera littoralis,a widespread mangrove in the Indo‐West Pacific

Phylogeographic forces driving evolution of sea‐dispersed plants are often influenced by regional and species characteristics, although not yet deciphered at a large spatial scale for many taxa like the mangrove species Heritiera littoralis. This study aimed to assess geographic distribution of genetic variation of this widespread mangrove in the Indo‐West Pacific region and identify the phylogeographic factors influencing its present‐day distribution. Analysis of five chloroplast DNA fragments’ sequences from 37 populations revealed low genetic diversity at the population level and strong genetic structure of H. littoralis in this region. The estimated divergence times between the major genetic lineages indicated that glacial level changes during the Pleistocene epoch induced strong genetic differentiation across the Indian and Pacific Oceans. In comparison to the strong genetic break imposed by the Sunda Shelf toward splitting the lineages of the Indian and Pacific Oceans, the genetic differentiation between Indo‐Malesia and Australasia was not so prominent. Long‐distance dispersal ability of H. littoralis propagules helped the species to attain transoceanic distribution not only across South East Asia and Australia, but also across the Indian Ocean to East Africa. However, oceanic circulation pattern in the South China Sea was found to act as a barrier creating further intraoceanic genetic differentiation. Overall, phylogeographic analysis in this study revealed that glacial vicariance had profound influence on population differentiation in H. littoralis and caused low genetic diversity except for the refugia populations near the equator which might have persisted through glacial maxima. With increasing loss of suitable habitats due to anthropogenic activities, these findings therefore emphasize the urgent need for conservation actions for all populations throughout the distribution range of H. littoralis.     

40种蕨类植物matK基因的系统分类及分子进化研究

采用“放松分子钟”模型、氨基酸位点正选择模型和分子内共进化网络估算方法,对蕨类植物Ⅱ型内含子成熟酶蛋白K(Maturase K,MATK)编码基因matK的进化趋势进行研究。结果显示:matK基因在蕨类植物系统学研究中具有一定的应用价值,与rbcL基因和psaA基因联合后能显著提升系统发育树的可信度;蕨类植物MATK蛋白中存在少数曾经历正选择的位点;MATK蛋白内部有多对氨基酸位点共同构成共进化网络。在被子植物兴起环境改变后,MATK蛋白部分位点发生适应性进化,通过位点间共进化网络协同作用方式提升蕨类植物对新光合环境的适应能力。     

Therapeutic management of Mycobacterium avium subspecies paratuberculosis infection with complete resolution of symptoms and disease in a patient with advanced inflammatory bowel syndrome

Molecular Biology Reports - A 26-year-old male had a history of frequent bowel movements, mushy stool with mucus and loss of 25 kg body weight in 6 months was diagnosed as a case...     

Epigenetic Modulation in Parkinson’s Disease and Potential Treatment Therapies

In the recent past, huge emphasis has been given to the epigenetic alterations of the genes responsible for the cause of neurological disorders. Earlier, the scientists believed somatic changes and modifications in the genetic makeup of DNA to be the main cause of the neurodegenerative diseases. With the increase in understanding of the neural network and associated diseases, it was observed that alterations in the gene expression were not always originated by the change in the genetic sequence. For this reason, extensive research has been conducted to understand the role of epigenetics in the pathophysiology of several neurological disorders including Alzheimer’s disease, Parkinson’s disease and, Huntington’s disease. In a healthy person, the epigenetic modifications play a crucial role in maintaining the homeostasis of a cell by either up-regulating or down-regulating the genes. Therefore, improved understanding of these modifications may provide better insight about the diseases and may serve as potential therapeutic targets for their treatment. The present review describes various epigenetic modifications involved in the pathology of Parkinson’s Disease (PD) backed by multiple researches carried out to study the gene expression regulation related to the epigenetic alterations. Additionally, we will briefly go through the current scenario about the various treatment therapies including small molecules and multiple phytochemicals potent enough to reverse these alterations and the future directions for a better management of PD.