8 research outputs found
High-resolution and low-background Ho spectrum: interpretation of the resonance tails
The determination of the effective electron neutrino mass via kinematic analysis of beta and electron capture spectra is considered to be model-independent since it relies on energy and momentum conservation. At the same time the precise description of the expected spectrum goes beyond the simple phase space term. In particular for electron capture processes, many-body electron-electron interactions lead to additional structures besides the main resonances in calorimetrically measured spectra. A precise description of the Ho spectrum is fundamental for understanding the impact of low intensity structures at the endpoint region where a finite neutrino mass affects the shape most strongly. We present a low-background and high-energy resolution measurement of the Ho spectrum obtained in the framework of the ECHo experiment. We study the line shape of the main resonances and multiplets with intensities spanning three orders of magnitude. We discuss the need to introduce an asymmetric line shape contribution due to Auger–Meitner decay of states above the auto-ionisation threshold. With this we determine an enhancement of count rate at the endpoint region of about a factor of 2, which in turn leads to an equal reduction in the required exposure of the experiment to achieve a given sensitivity on the effective electron neutrino mass
Mutagenicity of chlorinated cyclopentadienes due to metabolic activation.
Chlorinated cyclopentadienes of which hexachlorocyclopentadiene is used for pesticide synthesis is suggested to undergo metabolic conversion forming acylating and possibly mutagenic tetrachlorocyclopentadienone. Tetra-, penta-, and hexachlorocyclopentadiene differ in the chlorine substitution at C-1. Oxygen insertion into C-1, which results in the formation of the dienone should depend on the degree of substitution at this position. The dienone is not stable and can only be isolated as the dimer. To detect its formation an in vitro test system, comprising mouse liver microsomes for metabolic activation and E. coli K 12 (343/113) to detect mutagenicity, has been used. According to the previous suggestions tetrachlorocyclopentadiene and pentachlorocyclopentadiene were highly mutagenic after metabolic activation, whereas hexachlorocyclopentadiene was not
Results of mutagenicity tests with the new salmonella strains TA 102 and TA 97
Presented on the workshop 'Gesellschaft fuer Umwelt-Mutationsforschung' (GUM). Also published in: MvP Hefte 3/1984, p. 66-79SIGLECopy held by FIZ Karlsruhe; available from UB/TIB Hannover / FIZ - Fachinformationszzentrum Karlsruhe / TIB - Technische InformationsbibliothekDEGerman
Entwicklung und Erprobung eines kombinierten Untersuchungsverfahrens zum Nachweis und zur Bewertung mutagener Stoffe in Wasser Abschlussbericht
With 37 refs., 42 tabs., 67 figs.TIB Hannover: FR 1461+a / FIZ - Fachinformationszzentrum Karlsruhe / TIB - Technische InformationsbibliothekSIGLEDEGerman
Entwicklung und Erprobung eines kombinierten Untersuchungsverfahrens zum Nachweis und zur Bewertung mutagener Stoffe im Wasser. Bd. 2 Ausfuehrliche Beschreibung der Untersuchungsmethoden und deren Ergebnisse
SIGLETIB: FR 1461(2) / FIZ - Fachinformationszzentrum Karlsruhe / TIB - Technische InformationsbibliothekDEGerman
Positive GABAA receptor modulators from Acorus calamus L. , and structural analysis of (+) dioxosarcoguaiacol by 1D and 2D NMR and molecular modeling
[Image: see text] In a two-microelectrode voltage clamp with Xenopus laevis oocytes, a petroleum ether extract of Acorus calamus rhizomes enhanced the GABA-induced chloride current through GABA(A) receptors of the α(1)β(2)γ(2S) subtype by 277% ± 9.7% (100 μg/mL). β-Asarone (1), (+)-dioxosarcoguaiacol (2), (+)-shyobunone (3), and (+)-preisocalamenediol (4) were subsequently identified as main active principles through HPLC-based activity profiling and targeted isolation. The compounds induced maximum potentiation of the chloride current ranging from 588% ± 126% (EC(50): 65.3 ± 21.6 μM) (2) to 1200% ± 163% (EC(50): 171.5 ± 34.6 μM) (1), whereas (−)-isoshyobunone (5) and (−)-acorenone (6) exhibited weak GABA(A) modulating properties (5: 164% ± 42.9%; EC(50): 109.4 ± 46.6 μM and 6: 241% ± 23.1%; EC(50): 34.0 ± 6.7 μM). The relative configuration of 2 was established as 4R*8S*10R* by NOESY experiments and conformational analysis