外来种入侵的不确定性动态模拟

外来种的入侵性和生境的可入侵性是研究生物入侵机制的两个关键因素。总结多数学者的研究成果,认为外来种的拓殖率(迁移率或繁殖率)、死亡率及在新生境中的竞争力是衡量外来种能否入侵成功的内在实质。从全新的角度出发,将引入的外来种看作是对原有生态系统的一种干扰,并在此基础上结合Tilman的多物种共存模型提出了外来种干扰模型。模拟发现外来种在入侵时具有明显的不确定性。拓殖率小的外来种在新的生态系统中由于不能适应环境无法成功定殖,被排斥在系统之外;相反,拓殖率足够大的话,外来种由于自身优势具有很强的入侵性,在几年或几十年的时间内就会成功地在新的环境中建立种群并拓殖入侵,影响了当地物种的生存及原有生态系统的稳定。研究还发现,物种入侵也存在一定的不确定性,入侵不一定会一直持续下去,或许在百年或几百年的时间内入侵种会突然灭绝,原生态系统又恢复到原来的水平。     

生境持续和瞬间部分毁坏下外来种入侵动态模拟

生境毁坏与生物入侵是造成生物多样性降低的两大重要原因, 二者结合研究是当前生物入侵研究的前沿和热点。通过外来种入侵干扰模型分析了外来种在生境完好、生境瞬间部分毁坏和生境持续部分毁坏下的入侵动态及其对土著种群的影响, 得出如下结论: 1)生境完好的情况下, 不同迁移能力的外来种会出现四种不同的入侵结果: 入侵失 败、归化、震荡共存和入侵成功; 2)无论生境瞬间部分毁坏或是生境持续部分毁坏, 当外来种的迁移率较弱时, 生境毁坏抑制入侵; 反之, 生境毁坏促进入侵成功; 3)生境毁坏从无-慢-快的变化过程中, 外来种的时滞时间表现出长-短-长的变化动态。当生境完好时, 外来种本身特征及种间竞争决定了时滞时间的长短, 当生境毁坏时, 干扰程度越强, 时滞时间越长, 外来种越需要较长的时间稳定种群。     

物种演化对人类活动作用下不同性质栖息地毁坏的响应

栖息地毁坏是物种多样性减少的首要因素之一, 因此研究物种演化对栖息地毁坏的响应是非常必要的。而栖息地的毁坏又有瞬间毁坏和持续毁坏两种, 以往对栖息地毁坏的研究集中在瞬间毁坏上, 而该文则是通过N_物种 竞争共存模型分析对比了物种演化对栖息地瞬间毁坏和持续毁坏的响应特征。研究发现 :不同性质的栖息地毁坏都会导致物种强弱关系的变化, 并非如通常所认为的强物种将免于遭受物种灭绝的威胁, 也不是强物种首先灭绝, 而是因集合种群结构的不同而异。在热带雨林群落, 瞬间毁坏下物种演化一般经历了强迫适应和恢复上升阶段, 而持续毁坏下物种得不到恢复, 只能持续衰退, 在较长一段时间内持续毁坏比瞬间毁坏更有利于物种的续存 ;而在温带森林群落, 瞬间毁坏下物种演化一般经历强迫适应, 恢复上升和准周期振荡, 最后平衡, 而持续毁坏下物种只能持续衰退, 出现了在栖息地持续毁坏率小于瞬间毁坏率时, 物种的栖息地占有率却小于瞬间毁坏时的占有率。     

物种多样性对栖息地毁坏时间异质性的响应

栖息地毁坏是物种多样性丧失最重要的因素之一.通过多物种竞争共存的非自治动力模型,利用香农多样性指数,研究并比较了不同结构集合种群群落的物种多样性对不同程度和不同速度的栖息地毁坏时间异质性的响应.结果表明:在栖息地瞬间毁坏下,物种多样性先快速下降,之后得到一定程度的恢复,最终在下降中走向平衡;在栖息地持续完全毁坏下,栖息地毁坏速度对物种多样性随累积栖息地毁坏率变化的影响,只有在最强物种多度 (q)较小时比较明显,而在q较大时较小;对于栖息地持续部分毁坏,栖息地毁坏速度只影响物种多样性振荡的幅度,而不影响其变化的最终结果,并且速度越快,物种多样性振荡幅度越大,越不利于群落的稳定.     

破碎栖息地中物种灭绝机制

栖息地毁坏既会直接降低物种多度,又会间接地降低物种迁移繁殖力,同时还会改变原有的种间平衡.尽管已有研究表明栖息地毁坏是物种灭绝的主要原因之一,但是尚未揭示破碎的栖息地中物种灭绝的驱动机制.通过元胞自动机模拟了物种灭绝对栖息地毁坏空间异质性响应的基础上,进一步研究了栖息地毁坏和种间竞争对物种灭绝的影响.结果发现:强物种的灭绝主要来自栖息地毁坏,而弱物种的灭绝,在随机毁坏下,主要由栖息地毁坏与种间竞争共同决定,而在边缘毁坏下则主要由种间竞争所引起的.栖息地毁坏与种间竞争共同引起的物种灭绝的时间非常短,而栖息地毁坏或种间竞争所引起的物种灭绝时间则较长.     

物种灭绝对不同时间尺度人类活动的响应机制研究

通过修改Tilman的多物种共存的经典模式中栖息地毁坏率（D）,使D随时间的推移呈线性增长情况下,本文模拟了百万年、万年和百年尺度人类活动对栖息地的破坏下,物种灭绝对栖息地毁坏的响应特征。结果表明,大时间尺度人类活动对栖息地毁坏导致物种的强弱关系发生变化,并且强物种先灭绝,而小时间尺度人类活动对栖息地破坏是弱物种先灭绝;在百万年和万年尺度上,物种对栖息地毁坏的响应是减幅振荡衰退直至灭绝,并且最强物种对栖息地的占有率（q）越大,振幅越大,而在百年尺度上,物种的演化几乎是直线衰退;在大时间尺度的栖息地毁坏情况下,q越大,则物种灭绝起始时间和所有物种灭绝的时间越长;而在较小的时间尺度的栖息地毁坏情况下,q越大,灭绝起始时间和所有物种最终灭绝的时间则越短。     

栖息地毁坏与动物物种灭绝关系的模拟研究

利用多个物种共存模式模拟了不同情况下的不同动物种群演化的动力学特性,研究结果表明：（1）由于栖息地的毁坏所导致的动手的种灭绝是依赖于对物种死亡率和有关平衡态的假设的,不同的假设下,既使栖息地的破坏率相同,灭绝的物种可能是竞争能力最强的若干物种,也可能是竞争能力相对较弱的若干物种,既不象传统的物种进化理论所认为的必是弱的物种先灭绝,也不象Tilman等人所认为的一定是最强的若干物种先灭绝;（2）如果弱的物种具有较高的平均死亡率,则当栖息地受到一定的毁坏时,将有较多强的物种灭绝,而且物种灭绝时间将大大缩短;（3）在物种死亡率不变的情形下,物种在未受毁坏栖息地上的平衡态和大占有率pl^0,将有利于物种的生存。     

迎接入侵种的挑战

入侵种是从原来生存的生境中被引入到一个新的生态环境的外来物种,它们勿需面对起源地的天敌和竞争,而且能很快适应新的生境,迅速繁衍,抢夺其他物种的养分和生存空间,造成其他本地物种的减少和灭绝,导致生态失衡,给社会带来经济上的负面冲击,甚至威胁人类的健康.入侵种属于外来种,但入侵种的范围却比外来种的范围小.并不是所有的外来种都会危害生态环境.其侵入过程错综复杂,并且会随着气候环境等因素的变化而变化,因而外来种引进的结果是不可预见的.       

物种灭绝对不同时间尺度栖息地毁坏响应的空间模拟

人类活动所引起的栖息地毁坏已成为当前物种多样性丧失的最主要的原因之一。空间显含模型相对于空间隐含模型来说,更加接近于现实,因此,通过元胞自动机,模拟了物种多样性对万年、千年、百年时间尺度人类活动所引起的栖息地毁坏的响应。研究结果表明：万年时间尺度上,物种是由强到弱的灭绝;而在千年时间尺度上,物种灭绝的序受集合种群结构的影响较大;在百年时间尺度上。物种由于栖息地毁坏过于剧烈和迅速,来不及作出响应。在栖息地完全毁坏时集体灭绝。因此,物种灭绝序不只是受竞争-侵占均衡机制的影响,还受不同时间尺度（不同速率）栖息地毁坏的影响。以及集合种群结构的影响。     

美国对入侵种的管理对策

外来种入侵是产生当前世界生物多样性危机的重要原因之一。目前外来种入侵问题已经引起人们的普遍关注。1999年2月美国联邦政府发布总统令,号召联邦政府机构执行人员防止外来入侵种所造成的严重环境威胁,指示有关职能部门行使职权阻止引入入侵种并且恢复本地种。总统令指示建立一个入侵物种理事会,并就理事会、联邦机构的职责做了相应界定。美国农业部等部门支持的入侵植物管理国家策略项目,提出了针对入侵种的三项国家目标一入侵种的预防、控制和本地种的恢复。国家管理策略的制定不同层次的人们提供了合作、教育和研究的机遇。美国政府部门以及有关社会团体已经就外来种入侵危害防范积极展开行动,包括制定标准防止入侵种进入,控制、根除入侵种,向民众进行有关外来种入侵的教育,增加财政年度预算等等。     

恒温脊椎动物最大持续能量代谢率及其研究进展

研究最大持续代谢率具有重要的理论和实践意义,本文概述了近年来国外对脊椎动物最大持续代谢率研究的成果,概括介绍了限制最大持续代谢率的四个假说：（1）食物限制假说（food limit hypothesis) ,(2)外周限制假说（peripheral limit hypotheisis),(3)中心限制假说（central limit hypothesis)和（4）对称性形态构成假说（symmorphosis hypothesis),分析了静止代谢率随持续代谢率的增加而增加的机理,讨论了最大持续代谢率对动物的生态进化意义,最后指出了最大持续代谢率研究中可能的发展前景。     

Fisheries bioeconomics: why is it so widely misunderstood?

Many fisheries management systems, even when based on apparently sound science, have failed to prevent severe overfishing. And even when successful in this sense, such systems have frequently resulted in a large degree of excess fishing capacity. The reason for these failures can often be found in a lack of consideration of the economic incentives affecting fishermen. Specifically, when forced to compete for a fixed total annual catch quota (TAC), fishermen are motivated to fish at high intensity, and to expand the fishing power of their vessels. Individual fishing quotas (IFQs) are being increasingly used as a method of altering economic incentives in a desirable way. IFQ systems, however, can also suffer severe shortcomings, unless substantial fees are extracted for the exclusive right to exploit a publicly owned resource. When combined with appropriate fees, or royalties, IFQs can indeed result in sustainable, profitable fisheries. There still remains the fundamental question of risk management, but this is also now beginning to be addressed. Thus there is now a strong hope for the future success of marine fisheries, at least within 200-mile coastal zones.     

绞股蓝的林下栽培

近年来由于绞股蓝的过度采收,野生资源面临枯竭危险,为了扩大绞股蓝植物的资源,人工栽培势在必行。１９９０－１９９３年在皖东琅琊山进行林下人工栽培试验,结果表明,在粗放管理的条件下,林下种植绞股蓝是可行的,选择适合的种源及林分郁闭度是关键因子,在刺槐林下栽培产量可到３３００ｋｇ／ｈｍ＾２。     

Polymer-Based Sustained-Release Dosage Forms for Protein Drugs, Challenges, and Recent Advances

While the concept of using polymer-based sustained-release delivery systems to maintain therapeutic concentration of protein drugs for extended periods of time has been well accepted for decades, there has not been a single product in this category successfully commercialized to date despite clinical and market demands. To achieve successful systems, technical difficulties ranging from protein denaturing during formulation process and the course of prolonged in vivo release, burst release, and incomplete release, to low encapsulation efficiency and formulation complexity have to be simultaneously resolved. Based on this updated understanding, formulation strategies attempting to address these aspects comprehensively were reported in recent years. This review article (with 134 citations) aims to summarize recent studies addressing the issues above, especially those targeting practical industrial solutions. Formulation strategies representative of three areas, microsphere technology using degradable hydrophobic polymers, microspheres made of water soluble polymers, and hydrophilic in vivo gelling systems will be selected and introduced. To better understand the observations and conclusions from different studies for different systems and proteins, physicochemical basis of the technical challenges and the pros and cons of the corresponding formulation methods will be discussed.     

Sustained release of acyclovir from nano-liposomes and nano-niosomes: an in vitro study

The present study was designed to develop and compare acyclovir containing nano-vesicular liposomes and niosomes based on cholesterol, soya L-alpha-lecithin and nonionic surfactant, span 20. The effort was made to study in vitro whether acyclovir-loaded nanovesicles could sustain the release of the drug by increasing residence time and thus, acyclovir could reduce its dose-related systemic toxicity. There were good vesicular distributions in both of the niosomes and the liposomes. The obtained vesicles were within 1 microm and about 35% of them were within a size of 100 nm. The percentage of drug loading varied and the niosomal vesicles contained more drug as compared with the liposomes. When the in vitro drug release was compared, it was found that the liposomes released about 90% drug in 150 min whereas the drug release was just 50% from the niosomal vesicles in 200 min. Again, the niosomes showed better stability compared with the liposomes. Thus, niosome could be a better choice for intravenous delivery of acyclovir.     

Development of egg PC/cholesterol/α-tocopherol liposomes with ionic gradients to deliver ropivacaine

Context: Ropivacaine (RVC) is an aminoamide local anesthetic widely used in surgical procedures. Studies with RVC encapsulated in liposomes and complexed in cyclodextrins have shown good results, but in order to use RVC for lengthy procedures and during the postoperative period, a still more prolonged anesthetic effect is required.

Objective: This study therefore aimed to provide extended RVC release and increased upload using modified liposomes.

Materials and methods: Three types of vesicles were studied: (i) large multilamellar vesicle (LMV), (ii) large multivesicular vesicle (LMVV) and (iii) large unilamellar vesicle (LUV), prepared with egg phosphatidylcholine/cholesterol/α-tocopherol (4:3:0.07?mol%) at pH 7.4. Ionic gradient liposomes (inside: pH 5.5, pH 5.5?+?(NH₄)₂SO₄ and pH 7.4?+?(NH₄)₂SO₄) were prepared and showed improved RVC loading, compared to conventional liposomes (inside: pH 7.4).

Results and discussion: An high-performance liquid chromatography analytical method was validated for RVC quantification. The liposomes were characterized in terms of their size, zeta potential, polydispersion, morphology, RVC encapsulation efficiency (EE(%)) and in vitro RVC release. LMVV liposomes provided better performance than LMV or LUV. The best formulations were prepared using pH 5.5 (LMVV 5.5_in) or pH 7.4 with 250?mM (NH₄)₂SO₄ in the inner aqueous core (LMVV 7.4_in?+?ammonium sulfate), enabling encapsulation of as much as 2% RVC, with high uptake (EE(%) ～70%) and sustained release (～25?h).

Conclusion: The encapsulation of RVC in ionic gradient liposomes significantly extended the duration of release of the anesthetic, showing that this strategy could be a viable means of promoting longer-term anesthesia during surgical procedures and during the postoperative period.     

Development and In Vivo Floating Behavior of Verapamil HCl Intragastric Floating Tablets

A novel gastro retentive controlled release drug delivery system of verapamil HCl was formulated in an effort to increase the gastric retention time of the dosage form and to control drug release. Hydroxypropylmethylcellulose (HPMC), carbopol, and xanthan gum were incorporated for gel-forming properties. Buoyancy was achieved by adding an effervescent mixture of sodium bicarbonate and anhydrous citric acid. In vitro drug release studies were performed, and drug release kinetics was evaluated using the linear regression method. The optimized intragastric floating tablet composed of 3:2 of HPMC K4M to xanthan gum exhibited 95.39% drug release in 24 h in vitro, while the buoyancy lag time was 36.2 s, and the intragastric floating tablet remained buoyant for >24 h. Zero-order and non-Fickian release transport was confirmed as the drug release mechanism from the optimized formulation (F7). X-ray studies showed that total buoyancy time was able to delay the gastric emptying of verapamil HCl intragastric floating tablet in mongrel dogs for more than 4 h. Optimized intragastric floating tablet showed no significant change in physical appearance, drug content, total buoyancy time, or in vitro dissolution pattern after storage at 40°C/75% relative humidity for 3 months.     

Oral delivery of allopurinol niosomes in treatment of gout in animal model

Context: Gout is a painful disorder which does not have an efficient delivery system for its treatment.

Objective: Development and in vitro, in vivo evaluation of allopurinol-loaded nonionic surfactant-based niosomes was envisaged.

Materials and methods: Niosomes were prepared with Span 20 and Tween 20 (1:1 molar ratio) using ether injection method. The formulations were screened for entrapment efficiency, particle size analysis, zeta potential, release kinetics, in vivo activity, and stability studies.

Result: Stable, spherical vesicles of average particle size 304?nm with zeta-potential and entrapment efficiency of 22.2?mV and 79.44?±?0.02%, respectively, were produced. In vitro release study revealed 82.16?±?0.04% release of allopurinol within 24?h. The niosomal formulation was further evaluated for its antigout potential in monosodium urate (MSU) crystal induced gout animal model. The formulation demonstrated significant uric acid level reduction and enhanced antigout activity when compared with the pure allopurinol.

Discussion: The better antigout activity displayed by niosomal formulation could be attributed to sustained release of drug, higher drug solubility within biological fluids, better membrane interaction, smaller size, and presence of cholesterol and surfactant.

Conclusions: This study reveals that niosomes can be an efficient delivery system for the treatment of gout.     

Differential metabolic adaptation to acute and long-term hypoxia in rat primary cortical astrocytes

Brain astrocytes provide structural and metabolic support to surrounding cells during ischemia. Glucose and oxygen are critical to brain function, and glucose uptake and metabolism by astrocytes are essential to their metabolic coupling to neurons. To examine astrocyte metabolic response to hypoxia, cell survival and metabolic parameters were assessed in rat primary cortical astrocytes cultured for 3 weeks in either normoxia or in either 1 day or 3 weeks sustained hypoxia (5% O2). Although cell survival and proliferation were not affected by the mildly hypoxic environment, substantial differences in glucose consumption and lactate release after either acute or prolonged hypoxia suggest that astrocyte metabolism may contribute to their adaptation. Hypoxia over a period of 1 day increased glucose uptake, lactate release, and glucose transporter 1 (GLUT1) and monocarboxylate transporter 1 (MCT1) expression, whereas hypoxia over a period of 3 weeks resulted in a decrease of all parameters. Furthermore, increased glucose uptake at 1 day of hypoxia was not inhibited by cytochalasin B suggesting the involvement of additional glucose transporters. We uncovered hypoxia-regulated expression of sodium-dependent glucose transporters (SGLT1) in astrocytes indicating a novel adaptive strategy involving both SGLT1 and GLUT1 to regulate glucose intake in response to hypoxia. Overall, these findings suggest that although increased metabolic response is required for the onset of astrocyte adaptation to hypoxia, prolonged hypoxia requires a shift to an energy conservation mode. These findings may contribute to the understanding of the relative tolerance of astrocytes to hypoxia compared with neurons and provide novel therapeutic strategies aimed at maintaining brain function in cerebral pathologies involving hypoxia.     

Rosin microparticles as drug carriers: Influence of various solvents on the formation of particles and sustained-release of indomethacin

The aim of this study was to formulate a sustained release system for indomethacin (IND) with rosin gum obtained from a pine tree. Rosin microparticles were prepared by a dispersion and dialysis method without the addition of surfactant. In order to investigate the influence of solvents on the formation of colloidal microparitcles, various solvents like ethanol, DMF, DMAc, and acetone were used. The rosin microparticles containing IND were characterized by X-ray diffractometry (XRD) and differential scanning calorimetry (DSC). The morphologies of rosin microparticles observed by scanning electron microscopy (SEM) were spherical. The solvents used to dissolve rosin significantly affected the drug content and drug release rate of IND. The release behaviors of IND from the rosin microparticles were dependent on the drug content and size of the particles. Rosin microparticles with a higher drug content and of a larger particle size had a slower drug release rate. Also, the IND release rate from the rosin microparticles could be regulated by the rosin content in the microparticles. From these results, rosin microparticles have the potential of being used as a sustained release system of IND.