The molecular sociology of the cell

Proteomic studies have yielded detailed lists of the proteins present in a cell. Comparatively little is known, however, about how these proteins interact and are spatially arranged within the 'functional modules' of the cell: that is, the 'molecular sociology' of the cell. This gap is now being bridged by using emerging experimental techniques, such as mass spectrometry of complexes and single-particle cryo-electron microscopy, to complement traditional biochemical and biophysical methods. With the development of integrative computational methods to exploit the data obtained, such hybrid approaches will uncover the molecular architectures, and perhaps even atomic models, of many protein complexes. With these structures in hand, researchers will be poised to use cryo-electron tomography to view protein complexes in action within cells, providing unprecedented insights into protein-interaction networks.     

Terrestrial isopods and myriapods in a forested scree slope: subterranean biodiversity,depth gradient and annual dynamics

Diversity, depth distribution and seasonal activity of isopods and myriapods were studied using subterranean traps buried in a forested limestone scree slope in the ?ierna Hora Mts, Western Carpathians, Slovakia, throughout the depth gradient from 5 to 95 cm. A total of five isopod, 13 diplopod and 11 chilopod species were identified. Most edaphic species strongly preferred the uppermost organic soil layers. Among the species captured, some represented rare stenoecous Carpathian endemics, namely the isopod Trichoniscus carpaticus, and diplopods Julus curvicornis and Leptoiulus mariae. Others were subterranean forms, partly adapted to hypogean conditions: the isopod Mesoniscus graniger, and diplopods Mecogonopodium carpathicum and Trachysphaera costata. The annual activity in the vast majority of the species ceased completely in winter, and was gradually relaunched in spring. In evaluating the age structure of two predominant diplopods Polydesmus denticulatus and Mecogonopodium carpathicum, both widespread across the depth gradient, a vertical segregation of early post-embryonic stages was found. While P. denticulatus tended to undergo the early stages of development in the soil-filled topmost levels, the early juvenile stage of M. carpathicum was distributed deep in the scree slope profile.     

Discharge properties of Mg–Sn–Y alloys as anodes for Mg-air batteries

Mg–Sn–Y alloys with different Sn contents (wt%) were assessed as anode candidates for Mg-air batteries. The relationship between microstructure (including the second phase, grain size, and texture) and discharge properties of the Mg–Sn–Y alloys was examined using mi-crostructure observation, electrochemical measurements, and galvanostatic discharge tests. The Mg–0.7Sn–1.4Y alloy had a high steady dis-charge voltage of 1.5225 V and a high anodic efficiency of 46.6% at 2.5 mA·cm?2. These good properties were related to its microstructure:small grain size of 3.8 μm, uniform distribution of small second phase particles of 0.6 μm, and a high content (vol%) of (11(2)0)/(10(1)0) orient-ated grains. The scanning Kelvin probe force microscopy (SKPFM) indicated that the Sn3Y5 and MgSnY phases were effective cathodes caus-ing micro-galvanic corrosion which promoted the dissolution of Mg matrix during the discharge process.     

Stabilization of protein structure by interaction of alpha-helix dipole with a charged side chain

The alpha-helix in proteins has a dipole moment resulting from the alignment of dipoles of the peptide bond which can perturb the pKas of ionizing groups. One of the two histidine residues (His18) in barnase, the small ribonuclease from Bacillus amyloliquefaciens, is located at the negatively charged end (C-terminal) of an alpha-helix. From NMR titrations of wild-type and engineered mutants we find that the pKa of His18 is 7.9 in wild-type enzyme, 1.6 units above the value in the urea-denatured enzyme and in model peptides. This implies that there is a favourable interaction between the protonated form of His18 and the alpha-helix that should stabilize the native structure at neutral pH by 2.1 kcal mol-1. Denaturation at various values of pH of wild-type and muant enzymes engineered at position 18 shows that this is so. The increase in stability of the enzyme as the pH changes from 8.5 to 6.3 is attributable to this interaction, and the pH-stability curve fits pKa values for His18 in native and urea-denatured enzymes that are consistent with the NMR data.     

Contribution of hydrophobic interactions to protein stability

A major factor in the folding of proteins is the burying of hydrophobic side chains. A specific example is the packing of alpha-helices on beta-sheets by interdigitation of nonpolar side chains. The contributions of these interactions to the energetics of protein stability may be measured by simple protein engineering experiments. We have used site-directed mutagenesis to truncate hydrophobic side chains at an alpha-helix/beta-sheet interface in the small ribonuclease from Bacillus amyloliquefaciens (barnase). The decreases in stability of the mutant proteins were measured by their susceptibility to urea denaturation. Creation of a cavity the size of a -CH2-group destabilizes the enzyme by 1.1 kcal mol-1, and a cavity the size of three such groups by 4.0 kcal mol-1.     

Structural genomics: beyond the human genome project.

With access to whole genome sequences for various organisms and imminent completion of the Human Genome Project, the entire process of discovery in molecular and cellular biology is poised to change. Massively parallel measurement strategies promise to revolutionize how we study and ultimately understand the complex biochemical circuitry responsible for controlling normal development, physiologic homeostasis and disease processes. This information explosion is also providing the foundation for an important new initiative in structural biology. We are about to embark on a program of high-throughput X-ray crystallography aimed at developing a comprehensive mechanistic understanding of normal and abnormal human and microbial physiology at the molecular level. We present the rationale for creation of a structural genomics initiative, recount the efforts of ongoing structural genomics pilot studies, and detail the lofty goals, technical challenges and pitfalls facing structural biologists.     

Transiting circumbinary planets Kepler-34 b and Kepler-35 b

Most Sun-like stars in the Galaxy reside in gravitationally bound pairs of stars (binaries). Although long anticipated, the existence of a 'circumbinary planet' orbiting such a pair of normal stars was not definitively established until the discovery of the planet transiting (that is, passing in front of) Kepler-16. Questions remained, however, about the prevalence of circumbinary planets and their range of orbital and physical properties. Here we report two additional transiting circumbinary planets: Kepler-34 (AB)b and Kepler-35 (AB)b, referred to here as Kepler-34 b and Kepler-35 b, respectively. Each is a low-density gas-giant planet on an orbit closely aligned with that of its parent stars. Kepler-34 b orbits two Sun-like stars every 289?days, whereas Kepler-35 b orbits a pair of smaller stars (89% and 81% of the Sun's mass) every 131?days. The planets experience large multi-periodic variations in incident stellar radiation arising from the orbital motion of the stars. The observed rate of circumbinary planets in our sample implies that more than ～1% of close binary stars have giant planets in nearly coplanar orbits, yielding a Galactic population of at least several million.