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111.
The Fifth World Parks Congress in Durban, South Africa, announced in September 2003 that the global network of protected areas now covers 11.5% of the planet's land surface. This surpasses the 10% target proposed a decade earlier, at the Caracas Congress, for 9 out of 14 major terrestrial biomes. Such uniform targets based on percentage of area have become deeply embedded into national and international conservation planning. Although politically expedient, the scientific basis and conservation value of these targets have been questioned. In practice, however, little is known of how to set appropriate targets, or of the extent to which the current global protected area network fulfils its goal of protecting biodiversity. Here, we combine five global data sets on the distribution of species and protected areas to provide the first global gap analysis assessing the effectiveness of protected areas in representing species diversity. We show that the global network is far from complete, and demonstrate the inadequacy of uniform--that is, 'one size fits all'--conservation targets.  相似文献   
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Pérez-Gussinyé M  Watts AB 《Nature》2005,436(7049):381-384
Field-based geological studies show that continental deformation preferentially occurs in young tectonic provinces rather than in old cratons. This partitioning of deformation suggests that the cratons are stronger than surrounding younger Phanerozoic provinces. However, although Archaean and Phanerozoic lithosphere differ in their thickness and composition, their relative strength is a matter of much debate. One proxy of strength is the effective elastic thickness of the lithosphere, Te. Unfortunately, spatial variations in Te are not well understood, as different methods yield different results. The differences are most apparent in cratons, where the 'Bouguer coherence' method yields large Te values (> 60 km) whereas the 'free-air admittance' method yields low values (< 25 km). Here we present estimates of the variability of Te in Europe using both methods. We show that when they are consistently formulated, both methods yield comparable Te values that correlate with geology, and that the strength of old lithosphere (> or = 1.5 Gyr old) is much larger (mean Te > 60 km) than that of younger lithosphere (mean Te < 30 km). We propose that this strength difference reflects changes in lithospheric plate structure (thickness, geothermal gradient and composition) that result from mantle temperature and volatile content decrease through Earth's history.  相似文献   
114.
The events of cell reproduction are governed by oscillations in the activities of cyclin-dependent kinases (Cdks). Cdks control the cell cycle by catalysing the transfer of phosphate from ATP to specific protein substrates. Despite their importance in cell-cycle control, few Cdk substrates have been identified. Here, we screened a budding yeast proteomic library for proteins that are directly phosphorylated by Cdk1 in whole-cell extracts. We identified about 200 Cdk1 substrates, several of which are phosphorylated in vivo in a Cdk1-dependent manner. The identities of these substrates reveal that Cdk1 employs a global regulatory strategy involving phosphorylation of other regulatory molecules as well as phosphorylation of the molecular machines that drive cell-cycle events. Detailed analysis of these substrates is likely to yield important insights into cell-cycle regulation.  相似文献   
115.
Small G proteins are GTP-dependent molecular switches that regulate numerous cellular functions. They can be classified into homologous subfamilies that are broadly associated with specific biological processes. Cross-talk between small G-protein families has an important role in signalling, but the mechanism by which it occurs is poorly understood. The coordinated action of Arf and Rho family GTPases is required to regulate many cellular processes including lipid signalling, cell motility and Golgi function. Arfaptin is a ubiquitously expressed protein implicated in mediating cross-talk between Rac (a member of the Rho family) and Arf small GTPases. Here we show that Arfaptin binds specifically to GTP-bound Arf1 and Arf6, but binds to Rac.GTP and Rac.GDP with similar affinities. The X-ray structure of Arfaptin reveals an elongated, crescent-shaped dimer of three-helix coiled-coils. Structures of Arfaptin with Rac bound to either GDP or the slowly hydrolysable analogue GMPPNP show that the switch regions adopt similar conformations in both complexes. Our data highlight fundamental differences between the molecular mechanisms of Rho and Ras family signalling, and suggest a model of Arfaptin-mediated synergy between the Arf and Rho family signalling pathways.  相似文献   
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