Evaluation of a new semi-automated Hydragel 11 von Willebrand factor multimers assay kit for routine use

BackgroundAccurate diagnosis and classification of von Willebrand disease (VWD) are essential for optimal management. The von Willebrand factor multimers analysis (VWF:MM) is an integral part of the diagnostic process in the phenotypic classification, especially in discrepant cases. The aim of this study was to evaluate the performance of a new Hydragel 11VWF multimer assay (H11VW).MethodsAnalytical performance characteristics such as repeatability (intra-assay variability, in gel between track variation), reproducibility (inter-assay variability, between gel variation), sensitivity, EQA performance and differences between two commercially available VWF:MM kits (H5VW and H11VW) were analysed in healthy volunteers'' plasmas using in-house prepared reference plasma.ResultsRepeatability and reproducibility results of H11VW demonstrated acceptable and equivalent performance with previously verified H5VW. Participation in EQA was successful. No statistically significant difference was detected between H5VW and H11VW kits for different fractions of multimers: LMWM p=0.807; IMWM p=0.183; HMWM p=0.774.ConclusionsH11VW demonstrated acceptable analytical performance characteristics. H11VW kit conveniently offers a more significant number of samples on a single gel. H5VW and H11VW kits can be used in daily practice interchangeably.     

The length of discontinuous gas exchange cycles in lepidopteran pupae may serve as a mechanism for natural selection

Gas exchange is studied in diapausing pupae of Mamestra brassicae L., whose larvae are reared under identical conditions. The release of CO₂ gas is recorded with infrared gaseous analyzers. Oxygen convective uptake into the tracheae and oxygen consumption rates are recorded by means of a constant‐volume coulometric respirometer. Outputs from both of these respirometry systems are combined with infrared actographs. All 3‐month‐old pupae of M. brassicae display a pattern of discontinuous gas exchange (DGE) cycles of CO₂ gas release by bursts, although the lengths of these cycles varies between individuals. Some pupae exhibit long DGE cycles of at least 20 h in duration, with negligible CO₂ gas release during interburst periods, and there is presumed to be a convective gas exchange at this time. As a result of a partial vacuum inside the tracheae, a large oxygen convective uptake always occurs at the start of the spiracular opening phase. Other pupae have short DGE cycles of less than 3 h in duration, with elevated CO₂ gas release during the interburst period, when gas exchange is predominantly diffusive. The spiracular open phase in these pupae consists of frequent separate convective bursts of CO₂ gas release, with the opening–closing rhythms of the spiracles, which are considered as O phase fluttering. The pupae with long DGE cycles exhibit extremely low metabolic rates and very low total water loss rates, whereas those with short DGE cycles have higher metabolic and total water loss rates. The pupae with long DGE cycles live approximately twice as long as those with short cycles; thus, the present study demonstrates that long DGE cycles confer a fitness benefit on pupae as a result of a lower metabolic rate associated with water economy, conferring on them a longer life.     

Immunochemical studies on two DT diaphorase active antigens isolated from rat liver cytosol by affinity chromatography

Two immunologically different DT diaphorases were isolated on an affinity column containing Dicumarol as ligand from the cytosol fraction of rat liver. With a specific antiserum raised in rabbits against the DT diaphorase fraction eluted from the column, the two DT diaphorases were shown with immunodiffusion methods to be present in the microsomal and mitochondrial as well as in the cytosol fraction of rat liver. The NAD(P)H oxidizing activity in the immunoprecipitates containing the two DT diaphorases was found to be inhibited by 10^?4m Dicumarol but not by 10^?3m 2-pivaloyl-1,3-indandione or warfarin. With the anti-DT diaphorase antiserum the two DT diaphorases were also demonstrated to be present in other organs but with a somewhat different distribution. One of them appeared predominantly in kidney and heart and the other in lung, brain, testis, and spleen. The latter DT diaphorase was also found to be retained in four 3-methylcholanthrene-induced rat hepatomas. These findings indicate different physiological functions for the two DT diaphorases which at present are unknown.     

A non-filamentous configuration of intermediate-sized filament proteins inDrosophila Kc tissue culture cells

Summary Using monoclonal antibodies against the major intermediate filament (10 nm) cytoskeletal proteins ofDrosophila tissue culture cells, we showed by indirect immunofluorescence and ammuno-electron microscopy that this cytoskeletal material also occurs in a non-filamentous configuration. Patches of fine granular material are detected in the cytoplasm of Kc cells but are absent in anotherDrosophila cell line (Schneider, line 2). These patches are surrounded by membranes with bound ribosomes, resembling endoplasmic reticulum, and are found throughout the cytoplasm. We suggest that these aggregates are caused by overproduction of intermediate filament material in the Kc cell line. This work was supported by a Fogarty International Fellowship from the NIH to M.F.W., and by a Heinsenberg Fellowship from the Deutsche Forschungsgemeinschaft, Bonn, to. H.B.