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  • GEOMAR Catalogue / E-Books  (2)
  • Articles  (18)
  • Wiley-Blackwell  (16)
  • Berlin, Heidelberg :Springer Berlin / Heidelberg,  (2)
  • The American Society for Biochemistry and Molecular Biology (ASBMB)  (2)
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  • GEOMAR Catalogue / E-Books  (2)
  • Articles  (18)
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  • 1
    Keywords: Machine learning -- Congresses. ; Cybernetics -- Congresses. ; Electronic books.
    Type of Medium: Online Resource
    Pages: 1 online resource (1128 pages)
    Edition: 1st ed.
    ISBN: 9783540335856
    Series Statement: Lecture Notes in Computer Science Series ; v.3930
    DDC: 006.31
    Language: English
    Note: Intro -- Preface -- Organization -- Table of Contents -- Author Index.
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  • 2
    Online Resource
    Online Resource
    Berlin, Heidelberg :Springer Berlin / Heidelberg,
    Keywords: Engineering. ; Electronic books.
    Type of Medium: Online Resource
    Pages: 1 online resource (286 pages)
    Edition: 1st ed.
    ISBN: 9783662484470
    DDC: 681.111
    Language: English
    Note: Intro -- Preface -- Contents -- 1 A Sketch of Ancient Western Astronomy -- 1.1 Historical Development of Western Astronomy -- 1.1.1 Egyptian Civilization -- 1.1.2 Mesopotamian Civilization -- 1.1.3 Aegean Civilization -- 1.1.3.1 Minoan and Mycenaean Civilization -- 1.1.3.2 Dark Age -- 1.1.3.3 Classical Age -- 1.1.3.4 Ionia School -- 1.1.3.5 Pythagoras School -- 1.1.3.6 Plato School -- 1.1.3.7 Hellenistic Age -- 1.2 Astronomical Cycles and Calendars -- 1.2.1 Egyptian Calendar -- 1.2.2 Metonic Cycle -- 1.2.3 Callippic Cycle -- 1.2.4 Saros Cycle -- 1.2.5 Exeligmos Cycle -- 1.3 Ancient Astronomical Theories -- 1.3.1 Solar Theory -- 1.3.2 Lunar Theory -- 1.3.3 Planetary Theory -- 1.4 Remarks -- References -- 2 Ancient Astronomical Instruments -- 2.1 Classifications Based on Functions -- 2.1.1 Observation Application -- 2.1.2 Measuring Position and Distance Application -- 2.1.3 Measuring Time Application -- 2.1.4 Computing Application -- 2.1.5 Demonstration Application -- 2.2 Jacob's Staff -- 2.3 Astrolabe -- 2.4 Sundial -- 2.5 Calendrical Device -- 2.5.1 Astrolabe with Calendrical Gearing -- 2.5.2 Sundial with Calendrical Gearing -- 2.6 Planetarium, Astrarium, and Astronomical Clock -- 2.7 Orrery -- 2.8 Comparisons of Astronomical Instruments -- 2.9 Remarks -- References -- 3 Amazing Discovery of Archaeology -- 3.1 Origination and Process of the Discovery -- 3.1.1 Historical Background of Salvage -- 3.1.2 Story of the Antikythera Finding -- 3.2 Introduction of the Excavations -- 3.3 Known Antikythera Astronomical Device -- 3.3.1 Front Plate -- 3.3.2 Back Plate -- 3.3.3 Display Pointers -- 3.3.3.1 Axial Rotation -- 3.3.3.2 Radial Rotation -- 3.3.3.3 Axial Rotation and Radial Sliding -- 3.3.4 Interior Structure of Mechanisms -- 3.4 Relative Historical Background and Records -- 3.5 Remarks -- References -- 4 Modern Reconstruction Research. , 4.1 Early Mentions -- 4.2 Reconstruction Work by Price -- 4.3 Reconstruction Work by Edmund and Morgan -- 4.4 Reconstruction Work by Wright -- 4.5 Reconstruction Work by Freeth et al. -- 4.6 Others' Research After AD 2000 -- References -- 5 Reconstruction Design Methodology -- 5.1 Reconstruction Research -- 5.2 Reconstruction Design Methodology -- 5.2.1 Design Specifications -- 5.2.2 Generalized Chains -- 5.2.3 Specialized Chains -- 5.2.4 Reconstruction Designs -- 5.3 Historical Archives of Antikythera Device -- 5.3.1 Detected Evidence -- 5.3.2 Decoded Information -- 5.3.3 Ancient Astronomy -- 5.3.4 Ancient Astronomical Instruments -- 5.3.5 Modern Kinematic and Mechanism Analyses -- 5.4 Reconstruction Research by Yan and Lin -- 5.4.1 Concepts of Mechanical Designs -- 5.4.1.1 Mechanical Members -- Link or Kinematic Link (KL) -- Gear (KG) -- 5.4.1.2 Joints -- Revolute Joint (JR) -- Pin-in-Slot Joint (JA) -- Gear Joint () -- 5.4.1.3 Degrees of Freedom -- 5.4.1.4 Topological Structure -- 5.4.2 Date Subsystem -- 5.4.3 Eclipse Prediction Subsystem -- 5.4.4 Calendrical Subsystem -- 5.4.5 Lunar Subsystem -- 5.4.6 Solar Subsystem -- 5.4.7 Planetary Subsystem -- 5.4.8 Summary -- 5.5 Comparisons Among Different Reconstruction Researches -- 5.5.1 Comparison with Price's Design -- 5.5.2 Comparison with Edmund and Morgan's Design -- 5.5.3 Comparison with Wright's Design -- 5.5.4 Comparison with the Design of Freeth et al. -- 5.6 Remarks -- References -- 6 Reconstruction Designs of the Calendrical Subsystem -- 6.1 Historical Archives of the Calendrical Subsystem -- 6.2 Design Process of the Calendrical Subsystem -- 6.2.1 Design Specifications -- 6.2.2 Generalized Chains -- 6.2.3 Specialized Chains -- 6.2.3.1 Ground Link (Member 1) -- 6.2.3.2 Callippic Cycle Link (Member 5) -- 6.2.3.3 Olympiad Cycle Link (Member 4) -- 6.2.3.4 Input Link (Member 2). , 6.2.3.5 Metonic Cycle Link (Member 3) -- 6.2.3.6 Transmission Link (Link 6) -- 6.2.4 Reconstruction Designs -- 6.2.4.1 Tooth Calculation of the Feasible Designs -- Feasible Reconstruction Design of Fig. a -- Feasible Reconstruction Design of Fig. b -- 6.3 Remarks -- References -- 7 Reconstruction Designs of the Lunar Subsystem -- 7.1 Historical Archives of the Lunar Subsystem -- 7.1.1 Kinematic Analysis of the Lunar Theory -- 7.1.2 Kinematic Analysis of Epicyclic Gear Trains -- 7.2 Design Process of the Lunar Subsystem -- 7.2.1 Design Specifications -- 7.2.2 Generalized Chains -- 7.2.3 Specialized Chains -- 7.2.3.1 Pin-in-Slot Device (Members 3, 5, and 6, and Joint JA) -- 7.2.3.2 Anomalistic Link (Member 4) -- 7.2.3.3 Ground Link (Member 1) -- 7.2.3.4 Sidereal Link and Output Link (Members 2 and 7) -- 7.2.3.5 Revolute Joints (Joints JR) -- 7.2.3.6 Gear Joints (JG) -- 7.2.4 Reconstruction Designs -- 7.3 Remarks -- References -- 8 Reconstruction Designs of the Solar Subsystem -- 8.1 Historical Archives of the Solar Subsystem -- 8.1.1 Possible Arrangements of the Driving Power -- 8.1.2 Kinematic Analysis of the Solar Theory -- 8.1.3 Eccentric System of the Solar Motion -- 8.1.4 Epicyclic System of the Solar Motion -- 8.1.4.1 Four-Bar Mechanism with 5 Joints -- 8.1.4.2 Five-Bar Mechanism with 7 Joints -- 8.2 Design Process of the Solar Subsystem -- 8.2.1 Type 1 Design of the Solar Subsystem -- 8.2.2 Type 2 Design of the Solar Subsystem -- 8.2.3 Type 3 Design of the Solar Subsystem -- 8.2.3.1 Ground Link (Member 1) -- 8.2.3.2 Input Link (Member 2) -- 8.2.3.3 Output Link (Member 3) -- 8.2.3.4 Transmission Links (Members 4 and 5) -- 8.2.3.5 Pin-in-Slot Joint (Joint JA) -- 8.2.3.6 Revolute Joints (Joint JR) -- 8.2.3.7 Gear Joints (Joint JG) -- 8.3 Remarks -- References -- 9 Reconstruction Designs of the Planetary Subsystem. , 9.1 Historical Archives of the Planetary Subsystem -- 9.1.1 Type 1 Design: Mechanism with One Gear Joint -- 9.1.2 Type 2 Design: Mechanism with Two Gear Joints -- 9.1.2.1 All Planet Gears Are Adjacent to Each Other by a Gear Joint -- 9.1.2.2 Two Planet Gears Are Adjacent to Each Other by a Pin-in-Slot Joint -- 9.2 Design Process of the Planetary Subsystem -- 9.2.1 Type 1 Design of the Planetary Subsystem -- 9.2.2 Type 2 Design of the Planetary Subsystem -- 9.2.2.1 Ground Link (Member 1) -- 9.2.2.2 Output Link (Member 3) -- 9.2.2.3 Input Link (Member 2) -- 9.2.2.4 Transmission Links (Members 4 and 5) -- 9.2.2.5 Pin-in-Slot Joint (Joint JA) -- 9.2.2.6 Gear Joints (Joint JG) -- 9.2.2.7 Revolute Joints (Joint JR) -- 9.3 Remarks -- References -- 10 Reconstruction Designs of the Moon Phase Display Device -- 10.1 Historical Archives of the Moon Phase Display Device -- 10.1.1 Related Evidence and Available Designs -- 10.1.2 Possible Driving Power Arrangements -- 10.1.3 Possible Design Types -- 10.2 Design Process of the Moon Phase Display Device -- 10.2.1 Example 1: Ordinary Gear Trains -- 10.2.2 Example 2: Epicyclic Gear Trains with 1-DOF -- 10.2.3 Example 3: Epicyclic Gear Trains with 2-DOF -- References -- 11 Assembly Work and Models -- 11.1 Complete Interior Mechanisms -- 11.1.1 Assembly Constraints of the Lost Mechanisms -- 11.1.1.1 Driving Power of Lost Mechanisms -- 11.1.1.2 Gear Sizes -- 11.1.1.3 Types of Planets -- 11.1.1.4 Epicyclic System of Superior Planets -- 11.1.2 Assembly Work -- 11.2 3D Reconstruction Model -- 11.2.1 Tooth Calculation -- 11.2.1.1 Calendrical Subsystem -- 11.2.1.2 Solar Subsystem -- 11.2.1.3 Planetary Subsystem -- 11.2.2 Detail Designs of Gears -- 11.2.3 Space Arrangement -- 11.2.4 Simulation Model -- References -- Appendix A All 48 Feasible Designs of CompleteInterior Mechanisms -- Appendix B Detailed Design of Model 9. , Index.
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  • 3
    ISSN: 1434-1948
    Keywords: Iridium ; Selenium ; Diselenolenes ; Carboranes ; X-ray crystal structure analysis ; NMR spectroscopy ; Chemistry ; General Chemistry
    Source: Wiley InterScience Backfile Collection 1832-2000
    Topics: Chemistry and Pharmacology
    Notes: The reaction of [Cp*IrCl2]2 with dilithium 1,2-ortho-carborane-1,2-diselenolate 3 leads to the green 16-electron diselenolene complex [Cp*Ir{Se2C2(B10H10)}] (4) which takes up two-electron ligands such as trimethylphosphane to give the 18-electron diselenolate derivative [Cp*Ir(PMe3){Se2C2(B10H10)}] (5). The molecular structures of 4 and 5 were determined by X-ray crystal structure analysis. The 77Se-nuclear shielding in 4 is lower by almost 500 ppm relative to that in 5.
    Additional Material: 2 Ill.
    Type of Medium: Electronic Resource
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  • 4
    Publication Date: 2017-07-29
    Description: Activation of hepatic stellate cells (HSCs) is a critical step in the development of liver fibrosis. During activation, HSCs lose their lipid droplets (LDs) containing triacylglycerols (TAGs), cholesteryl esters, and retinyl esters (REs). We previously provided evidence for the presence of two distinct LD pools, a preexisting and a dynamic LD pool. Here we investigate the mechanisms of neutral lipid metabolism in the preexisting LD pool. To investigate the involvement of lysosomal degradation of neutral lipids, we studied the effect of lalistat, a specific lysosomal acid lipase (LAL/Lipa) inhibitor on LD degradation in HSCs during activation in vitro. The LAL inhibitor increased the levels of TAG, cholesteryl ester, and RE in both rat and mouse HSCs. Lalistat was less potent in inhibiting the degradation of newly synthesized TAG species as compared with a more general lipase inhibitor orlistat. Lalistat also induced the presence of RE-containing LDs in an acidic compartment. However, targeted deletion of the Lipa gene in mice decreased the liver levels of RE, most likely as the result of a gradual disappearance of HSCs in livers of Lipa−/− mice. Lalistat partially inhibited the induction of activation marker α-smooth muscle actin (α-SMA) in rat and mouse HSCs. Our data suggest that LAL/Lipa is involved in the degradation of a specific preexisting pool of LDs and that inhibition of this pathway attenuates HSC activation.
    Print ISSN: 0021-9258
    Electronic ISSN: 1083-351X
    Topics: Biology , Chemistry and Pharmacology
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  • 5
    Publication Date: 2017-06-01
    Description: The deep sea is one of the most extensive ecosystems on earth. Organisms living there survive in an extremely harsh environment, and their mitochondrial energy metabolism might be a result of evolution. As one of the most important organelles, mitochondria generate energy through energy metabolism and play an important role in almost all biological activities. In this study, the mitogenome of a deep-sea sea anemone ( Bolocera sp.) was sequenced and characterized. Like other metazoans, it contained 13 energy pathway protein-coding genes and two ribosomal RNAs. However, it also exhibited some unique features: just two transfer RNA genes, two group I introns, two transposon-like noncanonical open reading frames (ORFs), and a control region-like (CR-like) element. All of the mitochondrial genes were coded by the same strand (the H-strand). The genetic order and orientation were identical to those of most sequenced actiniarians. Phylogenetic analyses showed that this species was closely related to Bolocera tuediae . Positive selection analysis showed that three residues (31 L and 42 N in ATP6 , 570 S in ND5 ) of Bolocera sp. were positively selected sites. By comparing these features with those of shallow sea anemone species, we deduced that these novel gene features may influence the activity of mitochondrial genes. This study may provide some clues regarding the adaptation of Bolocera sp. to the deep-sea environment. The deep sea is regarded as the most extensive ecosystem on earth, and the organisms living there survive in an extremely harsh environment. The mitochondrial energy metabolism of some organisms may be different from that of shallow sea species. We uncovered a number of mitochondrial genome features that may provide some clues for Bolocera sp. on the adaptation of the seamount Bolocera sp. to the deep-sea environment.
    Electronic ISSN: 2045-7758
    Topics: Biology
    Published by Wiley-Blackwell
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  • 6
    Publication Date: 2017-12-27
    Description: Ericerus pela Chavannes (Hemiptera: Coccoidae) is an economically important scale insect because the second instar males secrete a harvestable wax-like substance. In this study, we report the molecular cloning of a fatty acyl-CoA reductase gene ( EpFAR ) of E. pela . We predicted a 520-aa protein with the FAR family features from the deduced amino acid sequence. The EpFAR mRNA was expressed in five tested tissues, testis, alimentary canal, fat body, Malpighian tubules, and mostly in cuticle. The EpFAR protein was localized by immunofluorescence only in the wax glands and testis. EpFAR expression in High Five insect cells documented the recombinant EpFAR reduced 26-0:(S) CoA and to its corresponding alcohol. The data illuminate the molecular mechanism for fatty alcohol biosynthesis in a beneficial insect, E. pela .
    Print ISSN: 0739-4462
    Electronic ISSN: 1520-6327
    Topics: Biology
    Published by Wiley-Blackwell
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  • 7
    Publication Date: 2017-11-25
    Description: Tumors depend on their microenvironment for sustained growth, invasion, and metastasis. In this environment, endothelial cells (ECs) are an important stromal cell type interacting with malignant cells to facilitate tumor angiogenesis and cancer cell extravasation. Of note, lysosomal acid lipase (LAL) deficiency facilitates melanoma growth and metastasis. ECs from LAL-deficient (lal−/−) mice possess enhanced proliferation, migration, and permeability of inflammatory cells by activating the mammalian target of rapamycin (mTOR) pathway. Here we report that lal−/− ECs facilitated in vivo tumor angiogenesis, growth, and metastasis, largely by stimulating tumor cell proliferation, migration, adhesion, and transendothelial migration via increased expression of IL-6 and monocyte chemoattractant protein 1 (MCP-1). This prompted us to look for lysosomal proteins that are involved in lal−/− EC dysfunctions. We found that lal−/− ECs displayed increased expression of Rab7, a late endosome/lysosome-associated small GTPase. Moreover, Rab7 and mTOR were co-increased and co-localized to lysosomes and physically interacted in lal−/− ECs. Rab7 inhibition reversed lal−/− EC dysfunctions, including decreasing their enhanced migration and permeability of tumor-stimulatory myeloid cells, and suppressed EC-mediated stimulation of in vitro tumor cell transmigration, proliferation, and migration and in vivo tumor growth and metastasis. Finally, Rab7 inhibition reduced overproduction of reactive oxygen species and increased IL-6 and MCP-1 secretion in lal−/− ECs. Our results indicate that metabolic reprogramming resulting from LAL deficiency enhances the ability of ECs to stimulate tumor cell proliferation and metastasis through stimulation of lysosome-anchored Rab7 activity.
    Print ISSN: 0021-9258
    Electronic ISSN: 1083-351X
    Topics: Biology , Chemistry and Pharmacology
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  • 8
    Publication Date: 2012-08-25
    Description: Abstract. Sodium ethene-bis-nitrobenzenesulfonate, [Na 2 (ENS) · 6H 2 O] n ( 1 ) was synthesized through coupling reaction of o -nitrotoluenesulfonic acid in NaOH solution and characterized by single crystal X-ray diffraction, elemental analysis, IR and 1 H NMR spectroscopy, XRPD, DSC and TGA (where ENS 2– = ethene-bis-nitrobenzenesulfonate). The asymmetrical unit of ( 1 ) consists of two octahedral Na I ions, and the neighboring metal centers are bridged by μ 2 water molecules resulting in the formation of an inorganic tetranuclear unit. The tetranuclear units were connected through the ENS 2– ligands into a 2D topology net. The weak π–π stacking and H-bonding interactions further stabilized the structure. The crystals of (C 7 H 6 NO 5 S) – · (H 5 O 2 ) + ( 2 ) were obtained by post-processing the unreacted raw material to recycle. Furthermore, the rigidity and the conjugation effect of the aromatic system in compound 1 were increased through the coordination interactions of metal atoms to ligands, resulting in the emission coming from ligand enhanced with red-shifting about 9 nm of the maximal wavelength. The conjugation effects and the steric arrangement of the substituent groups play the main role to the luminescence intensity and red-shift effect.
    Print ISSN: 0044-2313
    Electronic ISSN: 1521-3749
    Topics: Chemistry and Pharmacology
    Published by Wiley-Blackwell
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  • 9
    Publication Date: 2014-09-13
    Description: ABSTRACT This study was the first to investigate the genetic abnormalities and structural dysplasia of anorectal malformations (ARMs) in male rats induced by di( n -butyl) phthalate (DBP). DBP was administered to timed-pregnant rats to establish the ARM rat model. The incidence of ARMs in male offspring was 39.5%. In neonatal period, decreased body weight and anogenital distance were observed. The general image and histological analysis of male offspring confirmed the presence of ARMs. Anatomical examination of the ARM male rats revealed the dysplasia in solid organs (heart-lung, liver, spleen, and kidney). The decreases of serum testosterone concentration and androgen receptor expression in terminal rectum were indicative of the antiandrogenic effects of DBP. Moreover, significant decreased mRNA expressions of these androgen-related genes such as sonic hedgehog, Gli2, Gli3, bone morphogenetic protein 4, Wnt5a, Hoxa13, Hoxd13, fibroblast growth factor 10, and fibroblast growth factor receptor 2 were found in terminal rectum of the ARM male pubs. These results demonstrated that development of ARM rats was impaired by maternal exposure to DBP. The antiandrogenic effects of DBP disturbing the androgen-related signaling networks might play an important role in the occurrence of ARMs. © 2014 Wiley Periodicals, Inc. Environ Toxicol, 2014.
    Print ISSN: 1520-4081
    Electronic ISSN: 1522-7278
    Topics: Energy, Environment Protection, Nuclear Power Engineering
    Published by Wiley-Blackwell
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  • 10
    Publication Date: 2015-12-24
    Description: Solid tumors often suffer from suboptimal oxygen and nutrient supplies. This stress underlies the requirement for metabolic adaptation. Aberrantly activated de novo lipogenesis is critical for development and progression of human hepatocellular carcinoma (HCC). However, whether de novo lipogenesis influences biologic behaviors of HCCs under conditions of metabolic stress are still poorly understood. Here we show that HCCs display distinct levels of glucose-derived de novo lipogenesis, which are positively correlated with their survival responses to glucose limitation. The enhanced lipogenesis in HCCs is characterized by an increased expression of rate-limiting enzyme acetyl-CoA carboxylase (ACCα). ACCα-mediated fatty acid synthesis determines the intracellular lipid content that is required to maintain energy hemostasis and inhibit cell death by means of fatty acid oxidation (FAO) during metabolic stress. In accordance, overexpression of ACCα facilitates tumor growth. ACCα forms a complex with carnitine palmitoyltransferase 1 (CPT1A) and prevents its mitochondria distribution under nutrient-sufficient condition. During metabolic stress, phosphorylation of ACCα leads to dissociation of the complex and mitochondria localization of CPT1A, thus promoting FAO-mediated cell survival. Therefore, ACCα could provide both the substrate and enzyme storage for FAO during glucose deficiency. Upregulation of ACCα is also significantly correlated with poorer overall survival and disease recurrence after surgery. The multivariate Cox regression analysis identified ACCα as an effective predictor of poor prognosis. Conclusion : These results present novel mechanistic insight into a pivotal role of ACCα in maintaining HCCs survival under metabolic stress. It could be exploited as novel diagnostic marker and therapeutic target. This article is protected by copyright. All rights reserved.
    Print ISSN: 0270-9139
    Electronic ISSN: 1527-3350
    Topics: Medicine
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