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  • 1
    Electronic Resource
    Electronic Resource
    [S.l.] : American Institute of Physics (AIP)
    Review of Scientific Instruments 67 (1996), S. 4290-4293 
    ISSN: 1089-7623
    Source: AIP Digital Archive
    Topics: Physics , Electrical Engineering, Measurement and Control Technology
    Notes: The measurement setup for studying changes of electric permittivity induced in liquids by a strong electric field nonlinear dielectric effect, (NDE) is presented. The construction is based on the idea of frequency modulation of an LC generator (with an inductance L and a capacitance C in resonant circuit), proposed by Malecki [J. Chem. Soc. Faraday Trans. II 72, 104 (1976)]. The strong electric field is applied in the form of rectangular pulses (typically 1–4 ms). The setup enables measurements in a broad range of frequencies (80 kHz–12 MHz) and contains a new calibrating system, minimizing the influence of systematic error on the measured NDE values. We also indicate menthol as a standard, reference liquid in NDE studies. New applications of the NDE technique for studying relaxation processes in critical solution are also presented. They are based on the time resolved analysis of NDE decay after switching off the strong electric field. © 1996 American Institute of Physics.
    Type of Medium: Electronic Resource
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  • 2
    Electronic Resource
    Electronic Resource
    Amsterdam : Elsevier
    Journal of Experimental Marine Biology and Ecology 174 (1993), S. 261-275 
    ISSN: 0022-0981
    Keywords: Benthic invertebrate ; Gonad production ; Growth rate ; Somatic production
    Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002
    Topics: Biology
    Type of Medium: Electronic Resource
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  • 3
    Electronic Resource
    Electronic Resource
    Springer
    Polar biology 11 (1991), S. 169-177 
    ISSN: 1432-2056
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology
    Notes: Summary 108 successful ground and Agassiz trawl catches were taken between 155 and 2031 m depth in the eastern Weddell Sea on board RV Polarstern in spring and summer (October–February) 1985–1989. In addition, 7 hauls were taken with a semipelagic trawl. Only 19 hauls (16.5%) contained no shrimps. The others yielded large numbers of Notocrangon antarcticus, Chorismus antarcticus, and Nematocarcinus lanceopes as well as 20 Lebbeus antarcticus and 11 specimens of an Eualus species new to science. 8 Pasiphaea scotiae were caught in a pelagic krill trawl. No reptant decapod crustaceans were detected in the study area. Shrimp densities determined from trawl catches were lower than estimates derived from underwater photography but in the same order of magnitude. Although yields of the three common shrimp species in some cases exceeded 20 kg per 0.5 h haul, shrimp stocks in the area cannot be considered to be of commercial significance. A wider geographical distribution and greater frequency of shrimps in high Antarctic waters was found than described hitherto. There was considerable variation in numbers, sex composition, occurrence at different depths, and size-frequency distributions. C. antarcticus and N. antarcticus grow to a larger size compared with individuals from the Antarctic Peninsula area. Within the area of investigation, length frequency distributions are skewed towards larger sizes at higher latitudes. In the eastern Weddell Sea larger specimens of the three common species live at greater depths than smaller individuals. Potential reasons for these differences are discussed.
    Type of Medium: Electronic Resource
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  • 4
    Electronic Resource
    Electronic Resource
    Springer
    Cellular and molecular life sciences 31 (1975), S. 238-239 
    ISSN: 1420-9071
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology , Medicine
    Notes: Résumé La technique directe de l'immunofluorescence a permis de mettre en évidence dans un ganglion lymphatique adjacent à la tumeur cancéreuse du rectum la présence de nombreuses cellules sécrétant de IgG monoclonal.
    Type of Medium: Electronic Resource
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  • 5
    Electronic Resource
    Electronic Resource
    Springer
    Polar biology 12 (1992), S. 111-120 
    ISSN: 1432-2056
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology
    Notes: Summary Data on reproductive biology are presented for five benthic caridean shrimps from the high Antarctic (Chorismus antarcticus, Notocrangon antarcticus, Nematocarcinus lanceopes, Lebbeus antarcticus and Eualus kinzeri). The first three species were very common on the Weddell Sea shelf and upper slope, whereas only a few individuals of the other two species were caught-but these did include some ovigerous females. Our measurements include size at first maturity, fecundity (total number and mass of eggs), individual egg mass, egg length, ovary indices, maximum size encountered and documentation of the reproductive cycle in spring and summer. Egg number generally increases with female size, and the largest species (N. lanceopes) also carries the highest number of eggs. The eggs of all high Antarctic species are large, the extreme being L. antarcticus with an egg length of up to 3.3 mm. For C. antarcticus and N. antarcticus, which have wide geographic distributions, a comparison is made with older published and unpublished data from the Subantarctic (South Georgia). High Antarctic representatives of these two species grow to a larger maximum size, attain sexual maturity later in their life cycle, and produce fewer and larger eggs in relation to both carapace length and female mass, than their Subantarctic counterparts.
    Type of Medium: Electronic Resource
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  • 6
    Electronic Resource
    Electronic Resource
    Springer
    The European physical journal 322 (1985), S. 25-36 
    ISSN: 1434-601X
    Keywords: 32.70.Fw ; 34.50.Fa
    Source: Springer Online Journal Archives 1860-2000
    Topics: Physics
    Notes: Abstract Accurate lifetime measurement for the 41 P 1, 41 D 2, 51 D 2 helium and the atomic 2p and 3p states of other noble gases was performed by the low energy electron beam alignment technique. An account of the influence of magnetic field on the electron path was made to obtain the real Hanle signal shape. The influence of the radiation trapping in the collision chamber was analysed with regard to the metastables diffusion. The experimental data were compared with the results of other methods of the lifetime determination.
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  • 7
    Publication Date: 2014-02-07
    Description: Standardized assessments of HIV-1 vaccine-elicited neutralizing antibody responses are complicated by the genetic and antigenic variability of the viral envelope glycoproteins (Envs). To address these issues, suitable reference strains are needed that are representative of the global epidemic. Several panels have been recommended previously, but no clear answers have been available on how many and which strains are best suited for this purpose. We used a statistical model selection method to identify a global panel of reference Env clones from among 219 Env-pseudotyped viruses assayed in TZM-bl cells with sera from 205 HIV-1-infected individuals. The Envs and sera were sampled globally from diverse geographic locations and represented all major genetic subtypes and circulating recombinant forms of the virus. Assays with a panel size of only nine viruses adequately represented the spectrum of HIV-1 serum neutralizing activity seen with the larger panel of 219 viruses. An optimal panel of nine viruses was selected and augmented with three additional viruses for greater genetic and antigenic coverage. The spectrum of HIV-1 serum neutralizing activity seen with the final 12-virus panel closely approximated the activity seen with subtype-matched viruses. Moreover, the final panel was highly sensitive for detection of many of the known broadly neutralizing antibodies. For broader assay applications, all 12 Env clones were converted to infectious molecular clones using a proviral backbone carrying a Renilla luciferase reporter gene (Env.IMC.LucR viruses). This global panel should facilitate highly standardized assessments of vaccine-elicited neutralizing antibodies across multiple HIV-1 vaccine platforms in different parts of the world. IMPORTANCE An effective HIV-1 vaccine will need to overcome the extraordinary genetic variability of the virus, where most variation occurs in the viral envelope glycoproteins that are the sole targets for neutralizing antibodies. Efforts to elicit broadly cross-reactive neutralizing antibodies that will protect against infection by most circulating strains of the virus are guided in part by in vitro assays that determine the ability of vaccine-elicited antibodies to neutralize genetically diverse HIV-1 variants. Until now, little information was available on how many and which strains of the virus are best suited for this purpose. We applied robust statistical methods to evaluate a large neutralization data set and identified a small panel of viruses that are a good representation of the global epidemic. The neutralization properties of this new panel of reference strains should facilitate the development of an effective HIV-1 vaccine.
    Print ISSN: 0022-538X
    Electronic ISSN: 1098-5514
    Topics: Medicine
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  • 8
    Publication Date: 2014-03-27
    Description: Data from the RV144 HIV vaccine trial indicated that gp120 V2 antibodies were associated with a lower risk of infection; thus, the mapping of V2 epitopes can contribute to the design of an effective HIV vaccine. We solved the crystal structure of human monoclonal antibody (MAb) 2158, which targets a conformational V2 epitope overlapping the α4β7 integrin binding site, and constructed a full-length model of V1V2. Comparison of computational energy stability to experimental enzyme-linked immunosorbent assay (ELISA) results identified a hydrophobic core that stabilizes the V2 region for optimal 2158 binding, as well as residues that directly mediate side chain interactions with MAb 2158. These data define the binding surface recognized by MAb 2158 and offer a structural explanation for why a mismatched mutation at position 181 (I181X) in the V2 loop was associated with a higher vaccine efficiency in the RV144 clinical vaccine trial. IMPORTANCE Correlate analysis of the RV144 HIV-1 vaccine trial suggested that the presence of antibodies to the second variable region (V2) of HIV-1 gp120 was responsible for the modest protection observed in the trial. V2 is a highly variable and immunogenic region, and structural information on its antigenic landscape will be important for rational design of an effective HIV-1 vaccine. Using X-ray crystallography, computational design tools, and mutagenesis assays, we carried out a detailed and systematic investigation of the epitope recognition of human V2 MAb 2158 and demonstrated that its epitope region overlaps the integrin binding site within V2. In addition, we propose a structure-based mechanism for mismatching of the isoleucine at position 181 and the increased vaccine efficacy seen in the RV144 vaccine trial.
    Print ISSN: 0022-538X
    Electronic ISSN: 1098-5514
    Topics: Medicine
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  • 9
    Publication Date: 2014-10-07
    Description: Broadly neutralizing antibodies targeting the HIV-1 envelope (Env) are key components for protection against HIV-1. However, many cross-reactive epitopes are often occluded. This study investigates the mechanisms contributing to the masking of V2i (variable loop V2 integrin) epitopes compared to the accessibility of V3 epitopes. V2i are conformation-dependent epitopes encompassing the integrin α4β7-binding motif on the V1V2 loop of HIV-1 Env gp120. The V2i monoclonal antibodies (MAbs) display extensive cross-reactivity with gp120 monomers from many subtypes but neutralize only few viruses, indicating V2i's cryptic nature. First, we asked whether CD4-induced Env conformational changes affect V2i epitopes similarly to V3. CD4 treatment of BaL and JRFL pseudoviruses increased their neutralization sensitivity to V3 MAbs but not to the V2i MAbs. Second, the contribution of N-glycans in masking V2i versus V3 epitopes was evaluated by testing the neutralization of pseudoviruses produced in the presence of a glycosidase inhibitor, kifunensine. Viruses grown in kifunensine were more sensitive to neutralization by V3 but not V2i MAbs. Finally, we evaluated the time-dependent dynamics of the V2i and V3 epitopes. Extending the time of virus-MAb interaction to 18 h before adding target cells increased virus neutralization by some V2i MAbs and all V3 MAbs tested. Consistent with this, V2i MAb binding to Env on the surface of transfected cells also increased in a time-dependent manner. Hence, V2i and V3 epitopes are highly dynamic, but distinct factors modulate the antibody accessibility of these epitopes. The study reveals the importance of the structural dynamics of V2i and V3 epitopes in determining HIV-1 neutralization by antibodies targeting these sites. IMPORTANCE Conserved neutralizing epitopes are present in the V1V2 and V3 regions of HIV-1 Env, but these epitopes are often occluded from Abs. This study reveals that distinct mechanisms contribute to the masking of V3 epitopes and V2i epitopes in the V1V2 domain. Importantly, V3 MAbs and some V2i MAbs display greater neutralization against relatively resistant HIV-1 isolates when the MAbs interact with the virus for a prolonged period of time. Given their highly immunogenic nature, V3 and V2i epitopes are valuable targets that would augment the efficacy of HIV vaccines.
    Print ISSN: 0022-538X
    Electronic ISSN: 1098-5514
    Topics: Medicine
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  • 10
    Publication Date: 2015-08-05
    Description: The V3 region of HIV-1 gp120 is important for virus-coreceptor interaction and highly immunogenic. Although most anti-V3 antibodies neutralize only the sensitive tier 1 viruses, anti-V3 antibodies effective against the more resistant viruses exist, and a better understanding of these antibodies and their epitopes would be beneficial for the development of novel vaccine immunogens against HIV. The HIV-1 isolate JRFL with its cryptic V3 is resistant to most V3-specific monoclonal antibodies (MAbs). However, the V3 MAb 2424 achieves 100% neutralization against JRFL. 2424 is encoded by IGHV3-53 and IGLV2-28 genes, a pairing rarely used by the other V3 MAbs. 2424 also has distinct binding and neutralization profiles. Studies of 2424-mediated neutralization of JRFL produced with a mannosidase inhibitor further revealed that its neutralizing activity is unaffected by the glycan composition of the virus envelope. To understand the distinct activity of 2424, we determined the crystal structure of 2424 Fab in complex with a JRFL V3 peptide and showed that the 2424 epitope is located at the tip of the V3 crown ( 307 IHIGPGRAFYT 319 ), dominated by interactions with His P308 , Pro P313 , and Arg P315 . The binding mode of 2424 is similar to that of the well-characterized MAb 447-52D, although 2424 is more side chain dependent. The 2424 epitope is focused on the very apex of V3, away from nearby glycans, facilitating antibody access. This feature distinguishes the 2424 epitope from the other V3 crown epitopes and indicates that the tip of V3 is a potential site to target and incorporate into HIV vaccine immunogens. IMPORTANCE HIV/AIDS vaccines are crucial for controlling the HIV epidemics that continue to afflict millions of people worldwide. However, HIV vaccine development has been hampered by significant scientific challenges, one of which is the inability of HIV vaccine candidates evaluated thus far to elicit production of potent and broadly neutralizing antibodies. The V3 loop is one of the few immunogenic targets on the virus envelope glycoprotein that can induce neutralizing antibodies, but in many viruses, parts of V3 are inaccessible for antibody recognition. This study examined a V3-specific monoclonal antibody that can completely neutralize HIV-1 JRFL, a virus isolate resistant to most V3 antibodies. Our data reveal that this antibody recognizes the most distal tip of V3, which is not as occluded as other parts of V3. Hence, the epitope of 2424 is in one of the vulnerable sites on the virus that may be exploited in designing HIV vaccine immunogens.
    Print ISSN: 0022-538X
    Electronic ISSN: 1098-5514
    Topics: Medicine
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