Barley seed sensitivity to water stress at germination stage

V. Hosnedl; H. Honsová

doi:10.17221/4370-pse

Barley seed sensitivity to water stress at germination stage

Plant Soil and Environment ◽

10.17221/4370-pse ◽

2011 ◽

Vol 48 (No. 7) ◽

pp. 293-297

Author(s):

V. Hosnedl ◽

H. Honsová

Keyword(s):

Hydrogen Peroxide ◽

Extreme Values ◽

Oxygen Deficiency ◽

Barley Seed ◽

Seed Vigour ◽

Water Sensitivity ◽

The Mean ◽

Laboratory Emergence ◽

Mean Time ◽

Higher Sensitivity

Barley seed sensitivity to water and anoxia was tested. Standard germination, mean time of germination (MTG), germination in sand wetted by water to 100% water capacity (anoxia) or by hydrogen peroxide (wet conditions without anoxia), germination in 0.75% hydrogen peroxide and laboratory emergence (15 and 20°C) were evaluated. Barley seed responds sensitively to stress conditions during germination. Significant germination decrease was found in abundance of water. Percentage of reduction depends on the variety and on the year of seed production. Extreme values of water sensitivity are in interval 4–90%. At wetted sand by 0.75%, solution of H<sub>2</sub>O<sub>2</sub> the germination was significantly less reduced. That means that barley seed is very sensitive to oxygen deficiency above all and is less injured by quick imbibition. Heterogeneity in seed vigour was demonstrated in laboratory emergence tests. Quick test of germination in 0.75% hydrogen peroxide deserves attention for its high correlation coefficient with the seed laboratory emergence. The results significantly demonstrate a higher sensitivity of deteriorated seed to germination in abiotic stresses conditions. Variability in speed of germination is increasing, which unfavourably extends the mean time of germination.

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Predicting Daily Maintenance Dose of Fluindione, an Oral Anticoagulant Drug

Thrombosis and Haemostasis ◽

10.1055/s-0038-1650357 ◽

1996 ◽

Vol 75 (05) ◽

pp. 731-733 ◽

Cited By ~ 13

Author(s):

V Cazaux ◽

B Gauthier ◽

A Elias ◽

D Lefebvre ◽

J Tredez ◽

...

Keyword(s):

Effective Dose ◽

Maintenance Dose ◽

Successive Approximations ◽

Hemorrhagic Complication ◽

Simple Method ◽

Individual Variations ◽

Anticoagulant Drug ◽

The Mean ◽

Mean Time ◽

Daily Maintenance Dose

SummaryDue to large inter-individual variations, the dose of vitamin K antagonist required to target the desired hypocoagulability is hardly predictible for a given patient, and the time needed to reach therapeutic equilibrium may be excessively long. This work reports on a simple method for predicting the daily maintenance dose of fluindione after the third intake. In a first step, 37 patients were delivered 20 mg of fluindione once a day, at 6 p.m. for 3 consecutive days. On the morning of the 4th day an INR was performed. During the following days the dose was adjusted to target an INR between 2 and 3. There was a good correlation (r = 0.83, p<0.001) between the INR performed on the morning of day 4 and the daily maintenance dose determined later by successive approximations. This allowed us to write a decisional algorithm to predict the effective maintenance dose of fluindione from the INR performed on day 4. The usefulness and the safety of this approach was tested in a second prospective study on 46 patients receiving fluindione according to the same initial scheme. The predicted dose was compared to the effective dose soon after having reached the equilibrium, then 30 and 90 days after. To within 5 mg (one quarter of a tablet), the predicted dose was the effective dose in 98%, 86% and 81% of the patients at the 3 times respectively. The mean time needed to reach the therapeutic equilibrium was reduced from 13 days in the first study to 6 days in the second study. No hemorrhagic complication occurred. Thus the strategy formerly developed to predict the daily maintenance dose of warfarin from the prothrombin time ratio or the thrombotest performed 3 days after starting the treatment may also be applied to fluindione and the INR measurement.

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Simultaneous Determination of Alogliptin, Linagliptin, Saxagliptin, and Sitagliptin in Bulk Drug and Formulation by UPLC Q-TOF-MS

Current Pharmaceutical Analysis ◽

10.2174/1573412915666190708162012 ◽

2020 ◽

Vol 17 (1) ◽

pp. 95-105

Author(s):

Ramji Rathod ◽

Faraat Ali ◽

Amrish Chandra ◽

Robin Kumar ◽

Meenakshi Dahiya ◽

...

Keyword(s):

Internal Standard ◽

Gradient Elution ◽

Ultra Performance Liquid Chromatography ◽

Pharmaceutical Dosage Forms ◽

Sensitivity And Selectivity ◽

The Mean ◽

Bulk Drug ◽

Positive Ion ◽

Higher Sensitivity

Background: A simple and sensitive Ultra Performance Liquid Chromatography-Mass Spectrometry method was developed and validated to measure the concentrations of Alogliptin (ALO), Linagliptin (LIN), Saxagliptin (SAX), and Sitagliptin (SIT) using Pioglitazone (PIO) as an internal standard. Methods: Chromatographic separation of six gliptins was achieved on a C-18 column (100×2.1 mm, 2.7 μm) using a mobile phase consisting of formic acid in water, 0.1%v/v: acetonitrile in gradient elution. Electrospray ionization (ESI) source was operated in the positive ion mode. Targeted MS/MS mode on a QTOF MS was used to quantify the drug utilizing the transitions of 340.1(m/z), 473.2 (m/z), 316.2 (m/z), 408.1 (m/z), and 357.1 (m/z) for ALO, LIN, SAX, SIT and PIO respectively. Results: As per ICH Q2R1 guidelines, a detailed validation of the method was carried out and the standard curves were found to be linear over the concentration ranges of 1516.0-4548.1 ng mL-1, 519.8- 1559.4 ng mL-1, 1531.4-4594.3 ng mL-1and 1519.6-4558.8 ng mL-1 for ALO, LIN, SAX and SIT respectively. Precision and accuracy results were within the acceptable limits. The mean recovery was found to be 98.8 _ 0.76 % (GEM), 102.2 _ 1.59 % (LIN), 95.3 _ 2.74 % (SAX) and 99.2 _ 1.75 % (SIT) respectively. Conclusions: The optimized validated UPLC QTOF-MS/MS method offered the advantage of shorter analytical times and higher sensitivity and selectivity. The optimized method is suitable for application in quantitative analysis of pharmaceutical dosage forms for QC laboratory.

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Hydrogen peroxide decomposition on a two-component CuO-Cr2O3 catalyst

Collection of Czechoslovak Chemical Communications ◽

10.1135/cccc19881636 ◽

1988 ◽

Vol 53 (8) ◽

pp. 1636-1646 ◽

Cited By ~ 8

Author(s):

Viliam Múčka ◽

Kamil Lang

Keyword(s):

Hydrogen Peroxide ◽

Catalytic Activity ◽

Extreme Values ◽

Catalytic Properties ◽

Active Components ◽

Catalytic Systems ◽

Heterogeneous Catalytic ◽

Peroxide Decomposition ◽

Two Component ◽

Catalytically Active

Some physical and catalytic properties of the two-component copper(II)oxide-chromium(III)oxide catalyst with different content of both components were studied using the decomposition of the aqueous solution of hydrogen peroxide as a testing reaction. It has been found that along to both basic components, the system under study contains also the spinel structure CuCr2O4, chromate washable by water and hexavalent ions of chromium unwashable by water. The soluble chromate is catalytically active. During the first period of the reaction the equilibrium is being established in both homogeneous and heterogeneous catalytic systems. The catalytic activity as well as the specific surface area of the washed solid is a non-monotonous function of its composition. It seems highly probable that the extreme values of both these quantities are not connected with the detected admixtures in the catalytic system. The system under study is very insensitive with regard to the applied doses of gamma radiation. Its catalytic properties are changed rather significantly after the thermal treatment and particularly after the partial reduction to low degree by hydrogen. The observed changes of the catalytic activity of the system under study are very probably in connection with the changes of the valence state of the catalytically active components of the catalyst.

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Retrospective analysis of mortality within 30 days of systemic anticancer therapy and comparison with a previous audit at an Australian Regional Cancer Centre

Journal of Oncology Pharmacy Practice ◽

10.1177/10781552211016086 ◽

2021 ◽

pp. 107815522110160

Author(s):

Bernadatte Zimbwa ◽

Peter J Gilbar ◽

Mark R Davis ◽

Srinivas Kondalsamy-Chennakesavan

Keyword(s):

Checkpoint Inhibitors ◽

Anticancer Therapy ◽

Mortality Rates ◽

Feedback Process ◽

Time To Death ◽

Cancer Centre ◽

Haematology Patients ◽

The Mean ◽

Regional Cancer Centre ◽

Mean Time

Purpose To retrospectively determine the rate of death occurring within 14 and 30 days of systemic anticancer therapy (SACT), compare this against a previous audit and benchmark results against other cancer centres. Secondly, to determine if the introduction of immune checkpoint inhibitors (ICI), not available at the time of the initial audit, impacted mortality rates. Method All adult solid tumour and haematology patients receiving SACT at an Australian Regional Cancer Centre (RCC) between January 2016 and July 2020 were included. Results Over a 55-month period, 1709 patients received SACT. Patients dying within 14 and 30 days of SACT were 3.3% and 7.0% respectively and is slightly higher than our previous study which was 1.89% and 5.6%. Mean time to death was 15.5 days. Males accounted for 63.9% of patients and the mean age was 66.8 years. 46.2% of the 119 patients dying in the 30 days post SACT started a new line of treatment during that time. Of 98 patients receiving ICI, 22.5% died within 30 days of commencement. Disease progression was the most common cause of death (79%). The most common place of death was the RCC (38.7%). Conclusion The rate of death observed in our re-audit compares favourably with our previous audit and is still at the lower end of that seen in published studies in Australia and internationally. Cases of patients dying within 30 days of SACT should be regularly reviewed to maintain awareness of this benchmark of quality assurance and provide a feedback process for clinicians.

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Vitamin D Level Stability in Dystrophinopathy Patients on Vitamin D Supplementation

Journal of Neuromuscular Diseases ◽

10.3233/jnd-200625 ◽

2021 ◽

pp. 1-7

Author(s):

Naomi Vather-Wu ◽

Matthew D. Krasowski ◽

Katherine D. Mathews ◽

Amal Shibli-Rahhal

Keyword(s):

Vitamin D ◽

Retrospective Cohort ◽

Vitamin D Supplementation ◽

Hydroxyvitamin D ◽

Frequent Monitoring ◽

25 Hydroxyvitamin D ◽

The Mean ◽

Stable Maintenance ◽

Mean Time

Background: Expert guidelines recommend annual monitoring of 25-hydroxyvitamin D (25-OHD) and maintaining 25-OHD ≥30 ng/ml in patients with dystrophinopathies. Objective: We hypothesized that 25-OHD remains stable and requires less frequent monitoring in patients taking stable maintenance doses of vitamin D. Methods: We performed a retrospective cohort study, using the electronic health record to identify 26 patients with dystrophinopathies with a baseline 25-OHD ≥30 ng/mL and at least one additional 25-OHD measurement. These patients had received a stable dose of vitamin D for ≥3 months prior to their baseline 25-OHD measurement and throughout follow-up. The main outcome measured was the mean duration time the subjects spent with a 25-OHD ≥30 ng/mL. Results: Only 19% of patients dropped their 25-OHD to < 30 ng/ml, with a mean time to drop of 33 months and a median nadir 25-OHD of 28 ng/mL. Conclusions: These results suggest that measurement of 25-OHD every 2–2.5 years may be sufficient in patients with a baseline 25-OHD ≥30 ng/mL and who are on a stable maintenance dose of vitamin D. Other patients may require more frequent assessments.

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Carbon–nitrogen conjugate-composited Cu1.8S with enhanced peroxidase-like activity for the colorimetric detection of hydrogen peroxide and glutathione

Analytical Methods ◽

10.1039/d1ay00166c ◽

2021 ◽

Vol 13 (14) ◽

pp. 1706-1714

Author(s):

Nianlu Li ◽

Mingquan Zhu ◽

Zhenyu Feng ◽

Wenhui Lu ◽

Jing Chen ◽

...

Keyword(s):

Hydrogen Peroxide ◽

Colorimetric Detection ◽

Colorimetric Analysis ◽

Higher Sensitivity

In this work, cystine–glucose Maillard conjugates were composited with Cu1.8S microspheres (Cu1.8S–cgmc) to achieve higher sensitivity for the colorimetric analysis.

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Surveillance System in Smart Cities: A Dependability Evaluation Based on Stochastic Models

Electronics ◽

10.3390/electronics10080876 ◽

2021 ◽

Vol 10 (8) ◽

pp. 876

Author(s):

Igor Gonçalves ◽

Laécio Rodrigues ◽

Francisco Airton Silva ◽

Tuan Anh Nguyen ◽

Dugki Min ◽

...

Keyword(s):

Surveillance System ◽

Smart Cities ◽

Heterogeneous Data ◽

Time To Failure ◽

Video Streams ◽

Dependability Evaluation ◽

The Mean ◽

Mean Time ◽

The Internet Of Things

Surveillance monitoring systems are highly necessary, aiming to prevent many social problems in smart cities. The internet of things (IoT) nowadays offers a variety of technologies to capture and process massive and heterogeneous data. Due to the fact that (i) advanced analyses of video streams are performed on powerful recording devices; while (ii) surveillance monitoring services require high availability levels in the way that the service must remain connected, for example, to a connection network that offers higher speed than conventional connections; and that (iii) the trust-worthy dependability of a surveillance system depends on various factors, it is not easy to identify which components/devices in a system architecture have the most impact on the dependability for a specific surveillance system in smart cities. In this paper, we developed stochastic Petri net models for a surveillance monitoring system with regard to varying several parameters to obtain the highest dependability. Two main metrics of interest in the dependability of a surveillance system including reliability and availability were analyzed in a comprehensive manner. The analysis results show that the variation in the number of long-term evolution (LTE)-based stations contributes to a number of nines (#9s) increase in availability. The obtained results show that the variation of the mean time to failure (MTTF) of surveillance cameras exposes a high impact on the reliability of the system. The findings of this work have the potential of assisting system architects in planning more optimized systems in this field based on the proposed models.

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The impact of COVID-19 infection on hip fracture 30-day mortality

Trauma ◽

10.1177/1460408620949725 ◽

2021 ◽

pp. 146040862094972

Author(s):

Ahmed Fadulelmola ◽

Rob Gregory ◽

Gavin Gordon ◽

Fiona Smith ◽

Andrew Jennings

Keyword(s):

Hip Fracture ◽

Hip Fractures ◽

Hospital Admissions ◽

The Elderly ◽

Primary Outcome Measure ◽

Time To Death ◽

Significant Difference ◽

The Mean ◽

The Impact ◽

Mean Time

Introduction: A novel virus, SARS-CoV-2, has caused a fatal global pandemic which particularly affects the elderly and those with comorbidities. Hip fractures affect elderly populations, necessitate hospital admissions and place this group at particular risk from COVID-19 infection. This study investigates the effect of COVID-19 infection on 30-day hip fracture mortality. Method: Data related to 75 adult hip fractures admitted to two units during March and April 2020 were reviewed. The mean age was 83.5 years (range 65–98 years), and most (53, 70.7%) were women. The primary outcome measure was 30-day mortality associated with COVID-19 infection. Results: The COVID-19 infection rate was 26.7% (20 patients), with a significant difference in the 30-day mortality rate in the COVID-19-positive group (10/20, 50%) compared to the COVID-19-negative group (4/55, 7.3%), with mean time to death of 19.8 days (95% confidence interval: 17.0–22.5). The mean time from admission to surgery was 43.1 h and 38.3 h, in COVID-19-positive and COVID-19-negative groups, respectively. All COVID-19-positive patients had shown symptoms of fever and cough, and all 10 cases who died were hypoxic. Seven (35%) cases had radiological lung findings consistent of viral pneumonitis which resulted in mortality (70% of mortality). 30% ( n = 6) contracted the COVID-19 infection in the community, and 70% ( n = 14) developed symptoms after hospital admission. Conclusion: Hip fractures associated with COVID-19 infection have a high 30-day mortality. COVID-19 testing and chest X-ray for patients presenting with hip fractures help in early planning of high-risk surgeries and allow counselling of the patients and family using realistic prognosis.

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On the absorption probabilities and mean time for absorption for discrete Markov chains

Monte Carlo Methods and Applications ◽

10.1515/mcma-2021-2084 ◽

2021 ◽

Vol 0 (0) ◽

Author(s):

Nikolaos Halidias

Keyword(s):

Markov Chain ◽

Random Walk ◽

Markov Chains ◽

Generating Function ◽

Discrete Time ◽

Probability Generating Function ◽

The Mean ◽

Mean Time ◽

Absorption Probabilities

Abstract In this note we study the probability and the mean time for absorption for discrete time Markov chains. In particular, we are interested in estimating the mean time for absorption when absorption is not certain and connect it with some other known results. Computing a suitable probability generating function, we are able to estimate the mean time for absorption when absorption is not certain giving some applications concerning the random walk. Furthermore, we investigate the probability for a Markov chain to reach a set A before reach B generalizing this result for a sequence of sets A 1 , A 2 , … , A k {A_{1},A_{2},\dots,A_{k}} .

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Voxelwise Principal Component Analysis of Dynamic [S-Methyl-11C]Methionine PET Data in Glioma Patients

Cancers ◽

10.3390/cancers13102342 ◽

2021 ◽

Vol 13 (10) ◽

pp. 2342

Author(s):

Corentin Martens ◽

Olivier Debeir ◽

Christine Decaestecker ◽

Thierry Metens ◽

Laetitia Lebrun ◽

...

Keyword(s):

Principal Component Analysis ◽

Principal Component ◽

Component Analysis ◽

Added Value ◽

Time Activity ◽

Positron Emission ◽

Activity Curve ◽

The Mean ◽

Mean Time ◽

Met Pet

Recent works have demonstrated the added value of dynamic amino acid positron emission tomography (PET) for glioma grading and genotyping, biopsy targeting, and recurrence diagnosis. However, most of these studies are based on hand-crafted qualitative or semi-quantitative features extracted from the mean time activity curve within predefined volumes. Voxelwise dynamic PET data analysis could instead provide a better insight into intra-tumor heterogeneity of gliomas. In this work, we investigate the ability of principal component analysis (PCA) to extract relevant quantitative features from a large number of motion-corrected [S-methyl-11C]methionine ([11C]MET) PET frames. We first demonstrate the robustness of our methodology to noise by means of numerical simulations. We then build a PCA model from dynamic [11C]MET acquisitions of 20 glioma patients. In a distinct cohort of 13 glioma patients, we compare the parametric maps derived from our PCA model to these provided by the classical one-compartment pharmacokinetic model (1TCM). We show that our PCA model outperforms the 1TCM to distinguish characteristic dynamic uptake behaviors within the tumor while being less computationally expensive and not requiring arterial sampling. Such methodology could be valuable to assess the tumor aggressiveness locally with applications for treatment planning and response evaluation. This work further supports the added value of dynamic over static [11C]MET PET in gliomas.

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