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1.
徜徉花海     
早春三月,花花草草从沉睡中醒来,带给我们无限惊喜,在我们的幻想世界中,人们都佩戴着美丽的首饰,其外表能够与毛莨,勿忘我,矢车菊和其它花朵相媲美,黎明,从花朵到露珠润湿的叶片,无不散发着隐藏的魔力。  相似文献   
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Connecting people across the “digital divide” is as much a social effort as a technological one. We are developing a community-centred approach to learn how interaction techniques can compensate for poor communication across the digital divide. We have incorporated the lessons learned regarding social intelligence design in an abstraction and in a device called the SoftBridge. The SoftBridge allows communication to flow from endpoints through adapters, getting converted if necessary, and out to destination endpoints. Field trials are underway with two communities in South Africa: disadvantaged Deaf users and an isolated rural community. Initial lessons learned show that we have to design user interfaces that allow users to understand and cope with delay. We also learned that social concerns are often more important than the technical issues in designing such systems.  相似文献   
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The gangliosides of melanoma and other tumours of neuroectodermal origin are suitable targets for immune intervention with tumour vaccines. The optimal vaccines in current use contain ganglioside plus bacillus Calmette-Guérin and induce considerable morbidity. We have screened a variety of new adjuvants in the mouse, and describe one antigen-delivery system, proteosomes, which is especially effective. Highly hydrophobic Neisserial outer membrane proteins (OMP) form multimolecular liposome-like vesicular structures termed proteosomes which can readily incorporate amphiphilic molecules such as GD3 ganglioside. The optimal GD3/proteosome vaccine formulation for induction of GD3 antibodies in the mouse is determined. Interestingly, the use of potent immunological adjuvants in addition to proteosomes augments the IgM and IgG antibody titres against OMP in these vaccines but GD3 antibody titres are unaffected. The application of proteosomes to enhance the immune response to GD3 extends the concept of the proteosome immunopotentiating system from lipopeptides to amphipathic carbohydrate epitopes such as cell-surface gangliosides. The demonstrated safety of meningococcal OMP in humans and the data in mice presented here suggest that proteosome vaccines have potential for augmenting the immunogenicity of amphipathic tumour antigens in humans.  相似文献   
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Luteinizing hormone releasing hormone (LHRH) stimulates the development of cellular FSH immunoreactivity in the perinatal hamster adenohypophysis. Because neuropeptide Y (NPY) can act directly on rat adenohypophysial cells to stimulate FSH and LH release and potentiate the stimulatory effect of LHRH on FSH and LH release, we investigated the effects of NPY alone and in combination with a low, ineffective dose of LHRH on inducing cellular FSH immunoreactivity in the neonatal hamster adenohypophysis. Neonatal female pituitary glands were grafted beneath the right renal capsules of hypophysectomized-ovariectomized adult hamster hosts with a catheter implanted in the external jugular vein. After treatment, hosts were decapitated and graft tissue was stained for FSH and LH immunoreactivity. The mean percentage of adenohypophysial cells that stained for FSH was low (2.8%) in grafts in hosts infused continuously with heparinized saline vehicle for 7 days. In other hosts, peptides were pulsed through the catheter every 12 h for 7 days. The mean percentage of FSH cells also was low after pulsing 6 ng LHRH or 2 micrograms NPY but increased substantially when the two peptides were pulsed simultaneously. No differences in the mean percentage of LH cells existed between any of the groups. The results demonstrate that NPY and LHRH can synergize to induce cellular FSH immunoreactivity in the neonatal female hamster.  相似文献   
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The subject of decoding Reed-Solomon codes is considered. By reformulating the Berlekamp and Welch key equation and introducing new versions of this key equation, two new decoding algorithms for Reed-Solomon codes will be presented. The two new decoding algorithms are significant for three reasons. Firstly the new equations and algorithms represent a novel approach to the extensively researched problem of decoding Reed-Solomon codes. Secondly the algorithms have algorithmic and implementation complexity comparable to existing decoding algorithms, and as such present a viable solution for decoding Reed-Solomon codes. Thirdly the new ideas presented suggest a direction for future research. The first algorithm uses the extended Euclidean algorithm and is very efficient for a systolic VLSI implementation. The second decoding algorithm presented is similar in nature to the original decoding algorithm of Peterson except that the syndromes do not need to be computed and the remainders are used directly. It has a regular structure and will be efficient for implementation only for correcting a small number of errors. A systolic design for computing the Lagrange interpolation of a polynomial, which is needed for the first decoding algorithm, is also presented.This research was supported by a grant from the Canadian Institute for Telecommunications Research under the NCE program of the Government of Canada  相似文献   
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We measured motion-detection and motion-discrimination performance for different directions of motion, using stochastic motion sequences. Random-dot cinematograms containing 200 dots in a circular aperture were used as stimuli in a two-interval forced-choice procedure. In the motion-detection experiment, observers judged which of two intervals contained weak coherent motion, the other internal containing random motion only. In the direction-discrimination experiment, observers viewed a standard direction of motion followed by comparison motion in a slightly different direction. Observers indicated whether the comparison was clockwise or counterclockwise, relative to the standard. Twelve directions of motion were tested in the detection task and five standard directions (three cardinal directions and two oblique directions) in the discrimination task. Detection thresholds were invariant with direction of motion, but direction-discrimination thresholds were significantly higher for motion in oblique directions, even at low-coherence levels. Results from control conditions ruled out monitor artifacts and indicate that the oblique effect is relative to retinal coordinates. These results have broad implications for computational and physiological models of motion perception.  相似文献   
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The problem of decoding cyclic error correcting codes is one of solving a constrained polynomial congruence, often achieved using the Berlekamp-Massey or the extended Euclidean algorithm on a key equation involving the syndrome polynomial. A module-theoretic approach to the solution of polynomial congruences is developed here using the notion of exact sequences. This technique is applied to the Welch-Berlekamp (1986) key equation for decoding Reed-Solomon codes for which the computation of syndromes is not required. It leads directly to new and efficient parallel decoding algorithms that can be realized with a systolic array. The architectural issues for one of these parallel decoding algorithms are examined in some detail  相似文献   
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