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1.
危险废物焚烧处置系统中烟气脱酸工艺主要有湿法、干法和半干法三种,不同工艺的适用范围和优缺点不同,并且脱酸效率受到温度、烟气流速、压力和脱酸剂用量的影响,因此需要根据各焚烧系统的具体情况进行综合考虑,方能确定最佳的工艺方案。  相似文献   

2.
目的建立一种无乙醇无苯酚的5型肺炎球菌荚膜多糖纯化工艺,并进行工艺验证。方法 5型肺炎球菌发酵培养液采用脱氧胆酸钠法去除蛋白质,再利用层析法去除核酸等杂质,并对去除蛋白质工艺、层析工艺分别进行优化。采用优化后的方法纯化3批5型肺炎球菌发酵培养液,并对新工艺进行验证。结果去除蛋白质工艺的最适参数为:脱氧胆酸钠体积分数为0.5%,pH 4.3;层析工艺的最佳条件为:氯化钠浓度200 mmol/L,pH 8.0,上样流速150 cm/h,多糖质量浓度0.50 mg/mL。在上述工艺条件下,纯化的荚膜多糖各项指标均符合《欧洲药典》9.0版标准。结论该工艺稳定、可靠,可用于大规模生产,相比于传统的乙醇苯酚纯化工艺具有先进性。  相似文献   

3.
赤霉素固态发酵溶剂提取工艺研究   总被引:1,自引:0,他引:1  
就赤霉素固发酵的溶剂提取工艺的设计原理,溶剂选择、工艺路线的确定以及工艺参数的选定进行了较系统的试验分析研究,确定了比较切合实际、符合生产要求的最佳工艺,为工业化大生产提供了依据。  相似文献   

4.
在CHO细胞培养过程中,氨基酸的变化和消耗,是伴随CHO细胞所表达的抗体不同而发生变化。这就要求在细胞培养工艺的后期添加不同成分和比例的氨基酸进行补充,本文研究了用相同的CHO细胞为载体,表达不同抗体的细胞培养工艺后期氨基酸变化情况。从而,为细胞培养工艺后期流加氨基酸提供依据。通过氨基酸的补充可以提高培养工艺中细胞的活率和维持的时间,从而提高单批产量。这在今后放大培养过程中,对工艺的优化有着重大的意义。  相似文献   

5.
刺梨活性冻干粉冷冻干燥工艺研究   总被引:1,自引:0,他引:1  
研究了刺梨汁的真空冷冻干燥工艺,得到其冻干曲线,测定了刺梨汁的共融点,确定经济合理的装料量和工艺参数.根据本研究工艺参数真空冷冻干燥刺梨汁,较好的保持了SOD的活性.  相似文献   

6.
实验以三氧化二铬(Cr2O3)为外源指示剂,采用“70%基础饲料+30%实验原料”的方法配制实验饲料,测定了初始体质量为(28.68±0.49) g的黄颡鱼(Peltobagrus fulvidraco)对国产鱼粉、进口鱼粉、进口鸡肉粉和脱脂黄粉虫粉在膨化制粒和非膨化制粒两种工艺下的干物质、粗蛋白、粗脂肪和氨基酸表观消化率。结果显示,在非膨化制粒工艺下,黄颡鱼对进口鸡肉粉的干物质表观消化率显著高于另外3种原料(P<0.05),黄颡鱼对黄粉虫粉蛋白消化率最低(P<0.05),黄颡鱼对进口鸡肉粉脂肪表观消化率显著高于国产鱼粉和进口鱼粉(P<0.05); 在膨化制粒工艺下,进口鸡肉粉的干物质表观消化率显著低于另外3种原料(P<0.05),国产鱼粉和进口鱼粉的粗蛋白质消化率达94%以上,显著高于另外两种原料(P<0.05),但进口鸡肉粉的脂肪表观消化率显著低于其他原料(P<0.05)。在非膨化制粒工艺和膨化制粒工艺下国产鱼粉、进口鱼粉和黄粉虫粉的干物质表观消化率无显著性差异,但在非膨化制粒工艺下进口鸡肉粉的干物质表观消化率显著高于膨化制粒工艺(P<0.05)。对于国产鱼粉、进口鱼粉和黄粉虫粉而言,非膨化制粒工艺的蛋白消化率显著低于膨化制粒工艺(P<0.05),而鸡肉粉则相反。膨化加工工艺进口鱼粉的脂肪表观消化率显著高于非膨化加工工艺(P<0.05),而膨化加工工艺的黄粉虫脂肪表观消化率显著低于非膨化加工工艺(P<0.05)。氨基酸的消化率结果与粗蛋白的表观消化率变化趋势基本一致。由此可知,对于黄颡鱼饲料,国产鱼粉和进口鱼粉是最佳的蛋白质来源,进口鸡肉粉和黄粉虫亦可以作为其优质的蛋白质来源。对于进口鱼粉、国产鱼粉和黄粉虫粉,膨化制粒工艺更有利于黄颡鱼对其干物质、蛋白、脂肪和氨基酸等营养元素的消化利用,而对于进口鸡肉粉,非膨化制粒工艺更有利于黄颡鱼对营养元素的消化利用。  相似文献   

7.
白桦茸凝集素提取工艺的优化   总被引:1,自引:0,他引:1  
对白桦茸凝集素最佳提取工艺进行了研究.以2%兔血细胞凝血效价为指标,确定了最佳提取缓冲液.通过正交试验对料液比、提取时间、提取液pH值、NaCl浓度等因素进行了优化分析并确定了提取工艺的最佳参数组合.结果表明,以TBS和PBS为提取缓冲液所得的白桦茸凝集素凝集效价分别为64、16;最佳提取工艺:液料比为50:1,提取时间为20h,NaCl浓度为0mol/L,缓冲液pH值为8.0,按该最佳工艺提取白桦茸凝集素凝血效价为256.所优化的提取工艺稳定、可行,为该凝集素进一步在免疫调节方面的开发应用提供一定基础.  相似文献   

8.
沉香叶提取工艺及其抗氧化活性实验研究   总被引:1,自引:0,他引:1  
采用单因素分析方法和正交试验法研究沉香叶提取工艺并评价沉香叶的体外抗氧化活性.沉香叶的最佳提取工艺为:以15倍量的60%乙醇为溶剂,超声提取40 min,提取1次.野生沉香叶和栽培沉香叶的氧化时间分别为(11.53±0.08)s和(9.98±0.16)s;超氧阴离子的清除率分别为(36.26±0.96)%和(35.67±1.25)%,总还原力的吸光度分别为0.188±0.008和0.129±0.011.该提取工艺简单、重复性好、提取液抗氧化活性强、工艺稳定、无污染;野生沉香叶和栽培沉香叶均具有较好的体外抗氧化活性.  相似文献   

9.
杜仲茶加工工艺与营养成分相关性研究   总被引:3,自引:0,他引:3  
本文利用高效液相色谱仪、氨基酸自动分析仪等对不同加工工艺所生产的杜仲茶中的绿原酸、氨基酸、水溶性糖及蛋白质的含量进行了测定。结果表明:采用炒青的加工工艺所得的杜仲茶质量最佳。  相似文献   

10.
壳聚糖制备及加工工艺的研究   总被引:13,自引:1,他引:12  
本文在实验研究和前人工作的基础上,系统地分析了从甲壳素制备壳聚糖中脱乙酰化反应随温度、时间和碱液浓度变化规律,从而得出了脱乙酰化反应中较佳的工艺条件,和较为简便的从虾、蟹壳制备壳聚糖的工艺路线,为天然资源的综合利用打下了基础。  相似文献   

11.
The present communication is an attempt to describe the mode of propagation of AIDS epidemic and its control programme using a branching process as well as a birth-death and immigration model. A comparison of the project of AIDS control programme on the basis of its propagation by a continuous branching process model with that of a linear birth and death process with immigration shows a remarkable contrast. Branching process model shows that it is possible to control the propagation of the disease by suitably increasing the detection rate and lowering the infection rate. However, the propagation of AIDS models by birth and death Process with or without immigration shows that it is increasingly difficult to control the invasion of AIDS merely by controlling the birth, death and immigration parameters.  相似文献   

12.
The French and Japanese Developmental Biology Societies, teaming up with Human Frontier Science Program, were eager to meet back in person in November 2022 in the lovely city of Strasbourg. Top scientists in the developmental biology field from France and Japan, but also from United States, United Kingdom, Switzerland or Germany shared their exciting science during the 4 days of this meeting. Core fields of developmental biology such as morphogenesis, patterning, cell identity, and cell state transition, notably at the single cell level, were well represented, and a diversity of experimental models, including plants, animals, and other exotic organisms, as well as some in vitro cellular models, were covered. This event also extended the scope of classic scientific gatherings for two reasons. First the involvement of artists during the preparation of the event and on site. Second, part of the meeting was open for the general public through a series of outreach events, including a music and video presentation through projection mapping at Rohan palace, as well as public lectures.  相似文献   

13.
厌氧氨氧化工艺是一项高效、低耗的生物脱氮工艺,但受限于底物类型、硝氮积累等问题,其在主流应用中仍然面临一些挑战。近些年来,针对上述问题,厌氧氨氧化组合工艺得到了广泛关注。通过对近年来所开发的厌氧氨氧化组合工艺,从工艺原理、优缺点、影响因素、工艺拓展性及其在推广应用中存在的关键瓶颈等角度进行探讨,并结合课题组相关工作,展望了厌氧氨氧化组合工艺在城市生活污水处理中的发展前景。  相似文献   

14.
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16.
In a single compartment quantal response model, besides the input and release processes, an inspection process, assumed to be independent of the input and release processes, is considered. Each time when a release occurs, we assume the amount of release is randomly proportional to the amount present and the proportional rates form a sequence of independent and identically distributed random variables with support on [0, 1]. The input policy we consider is a modification of (s, S) input policy in the inventory model. More precisely, let 0 ≦s2s1sS, if after a release, the amount of the drug in subject's body is less than a level s2 which is small enough, then there will be an input immediately with probability 1 — p and no more inputs thereafter with probability p, also there will be an input immediately if the dose level is in the interval [s2, s1). If the dose level is in the interval [s1, s) there will be no input unless the inspector arrives. On the other hand, if the dose level is greater than or equal to s, then there will be no input. We consider a stochastic model as described above, and obtain the expressions for some quantities of interest. A Monte Carlo study has also been carried out to demonstrate some behaviors of our quantal response process.  相似文献   

17.
Inference for gamma and stable processes   总被引:2,自引:0,他引:2  
BASAWA  I. V.; BROCKWELL  P. J. 《Biometrika》1978,65(1):129-133
  相似文献   

18.
The transfer of processes for biotherapeutic products into finalmanufacturing facilities was frequently problematic during the 1980's and early 1990's, resulting in costly delays to licensure(Pisano 1997). While plant startups for this class of products can become chaotic affairs, this is not an inherent or intrinsic feature. Major classes of process startup problems have been identified andmechanisms have been developed to reduce their likelihood of occurrence. These classes of process startup problems and resolution mechanisms are the major topic of this article. With proper planning and sufficient staffing, the probably of a smooth process startup for a biopharmaceutical product can be very high – i.e., successful process performance will often beachieved within the first two full-scale process lots in the plant. The primary focus of this article is the role of the Process Development Group in helping to assure this high probability of success.  相似文献   

19.
Spectra of some self-exciting and mutually exciting point processes   总被引:9,自引:0,他引:9  
HAWKES  ALAN G. 《Biometrika》1971,58(1):83-90
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20.
The growing interest in Bacillus lipopeptides for high-value applications has driven process design, development and optimization for enhanced lipopeptide production. Traditional optimization approaches have been directed towards improving the overall titres by modification of media components and environmental parameters, almost exclusively in submerged cultures. Carbon and nitrogen sources, trace elements and oxygen availability have all been demonstrated to exhibit significant influences on lipopeptide yield, productivity and selectivity. This insight into process-linked kinetics, especially selectivity, has led to the introduction of novel process intensification and integration strategies which further promote process efficiency, and which include foam fractionation, inverse fluidization, rotating disc contacting and microfiltration with recycle. These strategies have not only transformed the production capabilities, but have also successfully integrated upstream production with downstream purification through cell retention and in situ product removal. This review analyses and critically discusses the impact of process conditions and process optimization strategies for improving lipopeptide production kinetics, specifically highlighting the emerging trend of process intensification and integration strategies and further, proposes a heuristic route to enhance lipopeptide production.  相似文献   

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