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121.
对硫酸庆大霉素/α半水硫酸钙载药体系进行了模拟条件下体外释药研究,并对其晶体结构进行了分析。X-射线衍射分析结果表明,载药体系中一定含量的硫酸庆大霉素不会影响α半水硫酸钙的水化;模拟条件下体外释药研究表明,各种药物含量的载药体系均表现出了良好的缓释性能,持续释放时间超过了360h;随着试样中载药量的增加,其药物释放速率加快;另外,构制了均一分散和核壳结构两种载药体系,研究结果表明,均一分散型在前期释放速度要大于核壳结构型,而后期核壳结构型则比均一分散型要高。 相似文献
122.
研究了氮化铝薄膜对LED灯散热情况的影响,并与导热硅脂(Ks609)涂层的散热效果进行了比较,结果表明:导热涂层能加强LED的散热,氮化铝薄膜散热效果优于导热硅脂;对红、白、绿3种颜色LED,相同条件下,散热材料对红色LED的散热效果最好。研究结果为氮化铝薄膜应用于LED散热系统提供了参考数据。 相似文献
123.
合成了一种新颖的乙炔衍生物,2-甲基-8-(9,9-二丁基芴)-3,5,7-三炔-2-辛醇(6a),并利用红外光谱(IR),紫外光谱(Uv),核磁(NMR),质谱(MS)等对其结构进行了表征。利用红外光谱(IR)和紫外光谱(Uv)对其拓扑固相聚合性质进行了研究。实验结果表明,这些化合物在加热和紫外光照射条件下都能够发生固相聚合,但得到的是结构复杂的聚合物。 相似文献
124.
We have used the yeast two-hybrid system to localize the ligand-dependent dimerization domain of the estrogen receptor-alpha (ER) to region E in vivo. In this system, the cDNAs corresponding to the A-D, E, E/F, A-E (deltaF), and full-length (wtER) domains of the human ER were each cloned into the yeast two-hybrid vectors GAL4 DB and GAL4 TA and expressed in different combinations in yeast harboring a GAL1-lacZ reporter. The reporter was used as a relative measure of the interaction between the ER domains, through reconstitution of GAL4 activity. We found that the interaction of E or E/F domains of the ER with full-length ER is estradiol dependent and estrogen responsive element independent, as measured by the reconstitution of GAL4 activity from GAL4-E domain-containing fusion protein interactions. In the presence of F domain, this activity is reduced 10-fold. The results suggest that sequences in the F domain are inhibitory to the dimerization signal that is present in the E region. We propose that the full-length ER contains intrinsic dimerization restraints contributed by regions outside domain E that are released upon binding hormone agonist. In addition, we have demonstrated that coactivator RIP140 is able to interact with the ER in vivo at the E domain of the receptor in the presence of estrogen. Yeast two-hybrid analysis shows that RIP140 does not homodimerize in the presence or absence of estrogens. We present evidence showing that the ER has the inherent ability to interact with RIP140 in the presence of antiestrogens, but sequences inherent in the ER itself that are present outside of the E domain compromise this ability. 相似文献
125.
OBJECTIVE: To describe the steps pharmacists must complete when seeking compensation from third party payers for pharmaceutical care services. DATA SOURCES: Government publications; professional publications, including manuals and newsletters; authors' personal experience. DATA SYNTHESIS: Pharmacists in increasing numbers are meeting with success in getting reimbursed by third party payers for patient care activities. However, many pharmacists remain reluctant to seek compensation because they do not understand the steps involved. Preparatory steps include obtaining a provider/supplier number, procuring appropriate claim forms, developing data collection and documentation systems, establishing professional fees, creating a marketing plan, and developing an accounting system. To bill for specific patient care services, pharmacists need to collect the patient's insurance information, obtain a statement of medical necessity from the patient's physician, complete the appropriate claim form accurately, and submit the claim with supporting documentation to the insurer. Although many claims from pharmacists are rejected initially, pharmacists who work with third party payers to understand the reasons for denial of payment often receive compensation when claims are resubmitted. CONCLUSION: Pharmacists who follow these guidelines for billing third party payers for pharmaceutical care services should notice an increase in the number of paid claims. 相似文献
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The binding of 3,6-hydroxy and keto disubstituted bile salts to human serum albumin was studied using differential scanning calorimetry, fluorescence spectroscopy and circular dichroism. The bile salts assayed did not produce any modification in the shape of the albumin thermogram, its thermal unfolding process in their presence being reversible; however, an increase in the enthalpy of unfolding and in the Tm was observed in the presence of 3,6-diketo and 3-hydroxy-6-keto bile salts. These two derivatives induced a negative circular dichroism spectrum of the protein around 280-290 nm, quenched the native fluorescence of the buried tryptophan of albumin and induced energy transfer between 1 aniline-8-naphthalene sulfonate and the buried tryptophan 214 of albumin. The presence of a keto group at C6 in the steroid ring of the bile salts plays an important role in producing slight movement of the albumin domains, increasing the distance between domains I and II. 相似文献
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