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H B Barlow 《Philosophical transactions of the Royal Society of London. Series B, Biological sciences》1980,290(1038):71-82
Our perceptions of the world around us are stable and reliable. Is this because the mechanisms that yield them are crude and insensitive and thus immune to false responses? Or is it because a statistical censor that blocks unreliable messages intervenes between the signals from our sense organs and our knowledge of them? This question can be answered by measuring the efficiency with which statistical information is utilized in perception. It is shown that mirror symmetry can be detected in displays of otherwise random dots with an efficiency of up to 50%; thus the statistical mechanisms are not crude and insensitive, and this aspect of sensory physiology and psychology may deserve more attention. 相似文献
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alpha-L-Fucosidase from serum of humans with either high or low enzyme activity was separately purified. the enzyme from either source had virtually the same heat stability and pH activity profile. It has been widely reported that alpha-L-fucosidase in crude sera from individuals with high and low enzyme activity differed with respect to heat stability and activity at pH 4 relative to activity at pH 5, the pH optimum of the enzyme. We investigated this discrepancy and found that both the heat stability and relative activity at pH 4 of alpha-L-fucosidase from sera with either high or low enzyme activity was dependent upon enzyme concentration. With decreasing enzyme concentration, the enzyme was more heat labile and had less relative activity at pH 4. Consequently, if the data obtained using high and low enzyme activity sera are compared on the basis of equivalent amounts of serum instead of equivalent amounts of enzyme activity, differences between the enzyme from high and low activity serum would be erroneously inferred. Apparently, this is what other investigators have done. Moreover, we found that alpha-L-fucosidase can exist in heat-stable or labile species with sedimentation coefficients of 9.8 S and 4.8 S, respectively. The interconversion and relative proportion of these species is dependent upon enzyme concentration and pH. 相似文献
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Interferon synthesis in the early post-implantation mouse embryo 总被引:6,自引:0,他引:6
Denise P. Barlow Beverley J. Randle Derek C. Burke 《Differentiation; research in biological diversity》1984,27(1-3):229-235
Abstract. A qualitative bioassay was adapted and used to determine the ability of the early post-implantation mouse embryo to synthesise interferon. Interferon production was not seen in any embryo tissue in the absence of an inducer and could only be detected in virus-induced tissue from the early 7th day of development. This induced interferon synthesis was initially confined to the trophoblast of the early 7th day embryo. It was then found in tissues of both trophoblast and inner cell mass origin in the early 8th day, and subsequently, in derivatives of the embryonic ectoderm in the 13th-day embryo. 相似文献
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Changes in chromatin structure during the mitotic cycle 总被引:3,自引:0,他引:3
P. W. Barlow 《Protoplasma》1977,91(2):207-211
Summary Optical density profiles of Feulgen-stained nuclei ofBryonia dioica at different stages of the mitotic cycle were determined. Nuclei in the G2 phase have a greater fraction of dense chromatin than nuclei in G1 phase. However, nuclei at the end of the S phase have dispersed chromatin of minimal density. Thus, chromatin density oscillates during the mitotic cycle of this species, consequently the progressive increase in density previously recorded throughout the intermitotic period of two other species (onion and mouse) cannot be a general rule. 相似文献
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Computer-aided molecular modelling of the endothelin (ET-A) receptor antagonists, BQ-123 and BE-18257B, shows that they have very similar 3D structures. Parts of their 3D structures are also shown to match closely with that reported for residues 6-8 in endothelin-1. On the basis of these similarities (and with supporting evidence from literature data on endothelin structure-activity relationships) a structural determinant is proposed for ET-A receptor binding, and novel designs of peptide are suggested for providing more potent and selective ET-A receptor antagonists. 相似文献