Description
Methoxy PEG Succinimidyl Succinate with superior quality specification of ≥95% Substitution.
JenKem Technology’s Methoxy PEG Succinimidyl Succinate (Methoxy PEG SS) is a high quality amine reactive NHS PEG product with degradable cleavable ester linker between the PEG polymeric chain and the NHS ester. Linear NHS PEGs with Cleavable Linker (degradable PEGs) are especially employed in controlled release drug development applications. Methoxy PEG Succinimidyl Succinate reacts with the amine group of lysine(s), or amines such as on the active ingredients of Adagen®, Peg-ademase, or PEG-adenosine deaminase, PEG aspargase, PEG-L-asparaginase, or related biosimilars, at pH 7-8, while the ester linkage is cleaved under regular ester cleaving reaction conditions. JenKem Technology offers Methoxy PEG SS with MW 5000 Da (M-SS-5000) and MW 20000 Da (M-SS-20K), in 1g and 10g packing sizes.
Different MW of Methoxy PEG Succinimidyl Succinate products may be available by custom synthesis, please email us at tech@jenkemusa.com for details on custom PEGs. Other linear NHS esters are available – please select other cleavable linker NHS PEGs; or stable linker NHS PEGs. JenKem Technology provides repackaging services for an additional fee, please contact us if you require a different package size than our catalog selection.
Bulk PEGs and GMP grade PEGs are made-to-order. Please contact us for bulk pricing.
Click here to download the MSDS
References:
1. Xiong, Q., et al., Facile fabrication of reduction-responsive supramolecular nanoassemblies for co-delivery of doxorubicin and sorafenib towards hepatoma cells, Frontiers in pharmacology, 2018, 9, p.61.
2. Mastorakos, P., et al., Biodegradable brain-penetrating DNA nanocomplexes and their use to treat malignant brain tumors, Journal of Controlled Release, 2017, 262, P. 37-46.
3. Mastorakos, P., et al., Biodegradable DNA Nanoparticles that Provide Widespread Gene Delivery in the Brain, Small, 2015.
4. Jain, S., et al., Combinatorial bio-conjugation of gemcitabine and curcumin enables dual drug delivery with synergistic anticancer efficacy and reduced toxicity, RSC Adv., 2014, 4, 29193-29201.
5. Tesfay, M.Z., et al., PEGylation of vesicular stomatitis virus extends virus persistence in blood circulation of passively immunized mice. J Virol, 2013, 87(7): p. 3752-9.
6. Helgeson, L.A., et al, Mechanism of synergistic activation of Arp2/3 complex by cortactin and N-WASP, eLife, 2013, 2:e00884.
7. Depp, V., et al., Native protein-initiated ATRP: A viable and potentially superior alternative to PEGylation for stabilizing biologics, Acta Biomaterialia, 5(2), 2009, p: 560-569.
Founded in 2001 by experts in PEG synthesis and PEGylation, JenKem Technology specializes exclusively in the development and manufacturing of high quality polyethylene glycol (PEG) products and derivatives, and related custom synthesis and PEGylation services. JenKem Technology is ISO 9001 and ISO 13485 certified, and adheres to ICH Q7A guidelines for GMP manufacture. The production of JenKem® PEGs is back-integrated to in-house polymerization from ethylene oxide, enabling facile traceability for regulated customers. JenKem Technology caters to the PEGylation needs of the pharmaceutical, biotechnology, medical device and diagnostics, and emerging chemical specialty markets, from laboratory scale through large commercial scale.
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我想提取中药中的有效成分,好像目前醇提取的比较多,中药有比如黄柏,桑白皮这些。有谁知道醇提取步骤吗?能不能帮帮忙,万分感激
求助战友们:
有做过中药醇提取,但是在收醇的时候,当浓缩至醇浓度约20%的时候,有析出现象,析出的还是我的有效成分,怎么才能解决这个问题呢?如果在未析出时停止浓缩,药液太稀,无法干燥呢?
问题1:我该如何浓缩定参数?
问题2:如果在未析出时放液,由于药液太稀,我该如何选择干燥方式?
求助站里的大侠们,谢谢!
补充:
一般使用浓硫酸作催化剂,使醇类脱去羟基生成含双键的有机物。应注意的是醇发生消去反应时的温度控制,温度较低(140℃)时会生成副产物醚类,温度达到一定范围(170℃)时才会发生消去反应。消去反应的本质是羟基与β位上的一个H原子共同脱去生成H2O的反应,因而能发生消去反应的醇类必须要有β-H原子。
如果羟基相连接的碳的邻位碳有多个,且都有氢原子,则消去有氢原子较少的邻位碳上的氢原子。 示例:
乙醇发生消去反应的方程式
CH3CH2OH→CH2=CH2+H2O (条件为浓硫酸 170摄氏度)
用蛋黄卵磷脂制备的“脂质体”粒径50-60nm,而文献中一般都是100多纳米,现在担心形成的不是脂质体,而是胶束,两者有什么方法可以鉴别吗?
甲磺酸与低级醇形成的甲磺酸烷基酯,具有潜在基因毒性。那么,几个碳的低级醇形成的甲磺酸烷基酯按照基因毒性杂质控制?(C<5?)上述结构化合物是否也需按照基因毒性杂质进行研究?
若是,按照此类杂质总和小于TTC(1.5ug/天)来控制,是否合适?
PS:一起始原料中引入此中间体,采用甲磺酰氯与对应醇反应所得,合成路线其他步骤也同时用到甲醇,会引入甲磺酸甲酯。
(二)连接回流冷凝管时,冷凝管连接水不会对浸出物造成影响吗?
请求大神指点,不胜感激!
本人目前在做一个中药提取方法的研究,水提醇沉,醇沉浓度分别为50%、60%和70%,检验结果,得率分别为21.99%、23.85%和25.55%,但含量分别是33.48mg/g、16.60mg/g和19.42mg/g。理论上是醇沉浓度越高,去除的杂质越多,得率越低吗?含量是不是也应该是醇沉浓度越高含量越高?我的试验有什么问题,求各位大虾指点!
各位老师好,有做环黄芪醇的吗?其对心血管效果怎么样?使用剂量范围是不是很窄,我看文献,有报道,黄芪提取物对血管的作有是双向的,会不会在低剂量时对身体是有害的
在本例中,溴处在间位,因此不参与反应。
而氯恰好处于对位,因而能发生反应,被甲氧基取代。
因此产物是4-硝基-2-溴苯甲醚。
完全醇水溶液如长期存放,会出现粘度增加甚至凝胶化的现象,聚合度和粘度越高,储存温度越低,越容易出现这种想象。可以采取以下措施:
(1)将聚乙烯醇水溶液重新加热搅拌即可恢复原来的流动性。
(2)添加硫氰盐酸盐(如钙、钠、铵等盐类)、苯酚、丁醇、山梨酸等可以有效防止凝胶化,添加量为5~10%。部分醇解型PVA长期存放不易产生粘度增加的情况。同时要注意长期存放容易发生发霉、腐化现象,需添加防霉、防腐剂。建议配置好水溶液后即时使用。
小弟有一中药处方,需要水煮醇沉处理,问下具体该怎么做,给我方子的老师去世了
告诉我中药先水煮,在用水煮醇沉法外敷治疗
给电话我直接问液可以