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多DSP系统的版本快速加载方法
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作者 符冬阳 《计算机系统应用》 2013年第8期169-172,共4页
研究了通信网络中多DSP系统的快速版本加载方法.核心是实现多个DSP的并行版本加载.各DSP在单板上有一个物理位置编号,对应于交换芯片上唯一的端口号,结合交换芯片驱动中的MAC地址学习表,找到DSP芯片MAC地址与交换芯片端口的对应关系,从... 研究了通信网络中多DSP系统的快速版本加载方法.核心是实现多个DSP的并行版本加载.各DSP在单板上有一个物理位置编号,对应于交换芯片上唯一的端口号,结合交换芯片驱动中的MAC地址学习表,找到DSP芯片MAC地址与交换芯片端口的对应关系,从而得到DSP芯片MAC地址与DSP物理位置编号的关系,进而得到版本类型与DSP芯片MAC地址的之间的对应关系.至此,HOST在同时复位所有DSP后,能够通过获取DSP版本请求报文中的源MAC地址,获知该DSP要下载的版本类型,达到支持多DSP并行加载版本的目的.通过实现多DSP的并行加载,能够将原来需要几十分钟的加载时间,缩短到几十秒钟的数量级,满足了通信系统快速启动的要求.此方法可以应用到具备以太网交换芯片、通过以太网方式加载版本的各种多DSP系统. 展开更多
关键词 数字信号处理器 版本加载 以太网交换 多DSP系统 MAC地址
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Enhanced release of the poorly soluble drug itraconazole loaded in ordered mesoporous silica 被引量:3
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作者 Xiao Liu Shunai Che 《Science China Chemistry》 SCIE EI CAS CSCD 2015年第3期400-410,共11页
It is known that the energy of the amorphous state of itraconazole loaded in ordered mesoporous materials is high relative to that of the crystalline state and is responsible for enhanced solubility and dissolution ra... It is known that the energy of the amorphous state of itraconazole loaded in ordered mesoporous materials is high relative to that of the crystalline state and is responsible for enhanced solubility and dissolution rate. We investigated the effects of particle size(0.7–5μm), mesostructure(2D p6 mm, cubic Ia-3d and cubic Fm-3m) and pore size(2.2–15.4 nm) of mesoporous silicas on the release performance of itraconazole. Results indicated that the release performance was not influenced by the particle sizes tested here, that the release performance increased with increasing pore diameter due to the lower probability of drug molecules colliding to recrystallize in large pores, and that the release performance was decreased in the cage-type pore structure(Fm-3m) compared to that in the cylindrical pore structures(p6mm and Ia-3d) because of the small entrance to the cagelike pores that retards the drug release. 展开更多
关键词 ITRACONAZOLE poorly soluble enhanced release mesoporous silica
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