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331.
逃逸函数算法及其在光学设计中的应用   总被引:1,自引:0,他引:1  
用阻尼最小二乘法进行光学系统的优化 ,得到的结果往往是评价函数在结构变量空间的一个局部极小值。日本东京工艺大学的一色教授提出了能够跳出此局部极小值继续寻找其它结果的逃逸函数全局优化算法 ,该算法的运行由多个不加或加入逃逸函数的阻尼最小二乘法局部优化组成。描述了逃逸函数的基本原理 ,给出了北京理工大学研制的GOLD软件在加入了这种算法后对光学系统进行全局优化的设计实例。实验证明了逃逸函数算法是提高光学设计效率和质量的一种有效工具。  相似文献   
332.
The THz-radiation power from InAs reaches sub-mW level in a 1.7-T magnetic field irradiated with femtosecond laser pulses of 1.5-W average power. The THz-radiation power is related almost quadratically both to the magnetic field and to the excitation laser power. Furthermore, the THz-radiation spectrum is found to be controlled by the excitation pulsewidth, chirp direction of the excitation pulse, and the magnetic field.  相似文献   
333.
The ZnSe : N epitaxial layers were grown on (1 1 0) ZnSe substrates in a low-pressure metalorganic chemical vapor deposition (MOCVD) system using hydrogen as a carrier gas, and using ammonia as a dopant source. In order to obtain highly doped ZnSe : N epitaxial layers, the optimum growth and doping conditions were determined by studying the photoluminescence (PL) spectra from the ZnSe epitaxial layers grown at different ammonia flux and VI/II flux ratio. Furthermore, in order to enhance the concentration of active nitrogen in ZnSe epitaxial layer, a rapid thermal anneal technique was used for post-heat-treating. The results show that the annealing temperature of over 1023 K is necessary. Beside, a novel treatment method to obtain a smooth substrate surface for growing high quality ZnSe epitaxial layers is also described.  相似文献   
334.
335.
Without elongational treatments, the fiber period of chondroitin-4-sulfate (0.87 nm) is shorter than in the elongated case (0.96 nm). The fiber period may change corresponding to its mechanical history. © 1996 John Wiley & Sons, Inc.  相似文献   
336.
Cancer cells recognize physical cues transmitted from the surrounding microenvironment, and accordingly alter the migration and chemosensitivity. Cell adhesive biomaterials with tunable physical properties can contribute to the understanding of cancer cell responses, and development of new cancer therapies. Previously, it was reported that polyrotaxane-based surfaces with molecular mobility effectively modulate cellular functions via the yes-associated protein (YAP)-related signaling pathway. In the present study, the impact of molecular mobility of polyrotaxane surfaces on the migration and chemosensitivity of lung (A549), pancreatic (BxPC-3), and breast cancer (MDA-MB-231) cell lines is investigated, and it is found that the cellular spreading of adherent A549 and BxPC-3 cells and nuclear YAP translocation are promoted on low-mobility surfaces, suggesting that cancer cells alter their subcellular YAP localization in response to molecular mobility. Furthermore, low-mobility surfaces suppress cellular migration more than high-mobility surfaces. Additionally, low-mobility surfaces promote the cisplatin chemosensitivity of each cancer cell line to a greater extent than high-mobility surfaces. These results suggest that the molecular mobility of polyrotaxane surfaces suppresses cellular migration and enhances chemosensitivity via the subcellular translocation of YAP in cancer cells. Biointerfaces based on polyrotaxanes can thus be a new platform for elucidating cancer cell migration and chemoresistance mechanisms.  相似文献   
337.
A polyrotaxane consisting of many β-cyclodextrins (β-CDs) and a triblock copolymer of poly(ethylene glycol) (PEG) and poly(propylene glycol) (PPG) capped with bulky end-groups was synthesized as a model of stimuli-responsive supramolecules for nanoscale devices. The polyrotaxane was reversibly soluble-insoluble in water in response to temperature. This was achieved through the assembled and dispersed states of β-CDs along the block copolymer. It is considered that intermolecular hydrogen bondings of β-CDs, as well as the PEG segment length of the copoloymer, are predominant factors for regulating such thermally switchable behavior of the polyrotaxane.  相似文献   
338.
The supramolecular network formation through inclusion complexation between α‐cyclodextrin‐based molecular tube (MT) and poly(ethylene oxide) monocetylether‐graft‐dextran (5C16PEO‐g‐Dex40) was demonstrated. From isothermal titration calorimetric (ITC) measurement, it was confirmed that MT formed an inclusion complex with two C16PEO side chains in 5C16PEO‐g‐Dex40. From viscosity measurements, the specific viscosity of the solution containing MT and 5C16PEO‐g‐Dex40 was much larger than that containing 5C16PEO‐g‐Dex40. It is considered that MT participates in the supramolecular network formation of 5C16PEO‐g‐Dex40 through inclusion complexation with two C16PEOs grafted to independent Dex40s.  相似文献   
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