Isolation and preliminary characterization of 1-O-Octadec-cis-11-enyl glycerol from Paramecium phospholipids

1-O-Octadec-$\text{cis}$-11-enyl glycerol, paramecyl alcohol, was isolated from $\text{Paramecium}\text{tetraurelia}$ and $\text{P.}\text{caudatum}$ phospholipids. This isomer of 1-O-octadec-9-enyl glycerol, selachyl alcohol, had not been previously reported as a component of naturally-occurring phospholipids. The preliminary characterization of the structure of this compound was determined by 1) gas chromatography of the parent compound as well as the products following hydrogenation, ozonolysis and oxidation, 2) mass spectrometry of the parent compound and an oxidation product, 3) infrared spectroscopy, and 4) proton magnetic resonance.     

Ryanodine does not affect the potassium channel from the sarcoplasmic reticulum of skeletal muscle

Single K channels from skeletal muscle sarcoplasmic reticulum were incorporated into artificial membranes. Ryanodine applied to either side of the membrane did not affect the gating nor the conductance properties of those channels. These results suggest that the site of action of ryanodine is limited only to the calcium channels present in the membrane of sarcoplasmic reticulum (1).     

SRY sequence in maternal plasma: Implications for non-invasive prenatal diagnosis: First report from India

AIM:

The presence of circulatory cell-free fetal DNA in maternal plasma has found new applications in non-invasive risk-free prenatal diagnosis.

MATERIALS AND METHODS:

We made use of a size separation approach along with real time polymerase chain reaction (PCR) to evaluate the use of fetal DNA in the detection of the sex of the fetus. Cell-free fetal DNA was isolated from the plasma of 30 women (10–20 weeks gestation) using a size separation approach. We made use of Taq Man Chemistry and real time PCR using primers and probes for GAPDH and SRY.

RESULTS:

Only 24 cases could be studied as there was no amplification in six cases. Fetal sex was accurately determined in all of the 24 cases wherein 19 women were carrying male fetuses and five women were carrying female fetuses. An increase in the amount of fetal DNA was observed with an increase in the gestational age.

CONCLUSIONS:

Real time PCR analysis is a highly sensitive and accurate tool for non-invasive prenatal diagnosis, allowing detection of the sex of the fetus as early as 10 weeks of gestation. Non-invasive prenatal diagnosis eliminates the risk of fetal loss associated with the invasive procedure.     

Potentiality of lignin from the Kraft pulping process for removal of trace nickel from wastewater: effect of demineralisation

An industrial raw Kraft lignin was investigated to ascertain its potential use for removal of trace Ni(II) ion from wastewater by using dilute solutions (0.34-1.7 mM) as models. The effect of demineralisation on its metal sorption ability was examined by employing acid pre-treated samples. Under fixed pre-established equilibrium conditions, the raw lignin exhibited a lower effectiveness than the demineralised one, with the latter attaining an almost complete removal of Ni(II) ions. For both lignins, sorption kinetics was properly described by a pseudo-second order rate model. Equilibrium isotherms were also determined and adequately represented by conventional two-parameter models. The higher nickel sorption capacity for the demineralised lignin compared to the raw sample was consistent with enhancements in the negative magnitude of zeta potential, sodium sorption capacity, and content of phenolic hydroxyl groups occasioned by the acid pre-treatment. Accordingly, demineralisation appears as a readily convenient strategy to improve the behaviour of industrial Kraft lignin for potential use as a biosorbent of trace nickel from polluted water.     

In Vivo Dynamical Interactions between CD4 Tregs,CD8 Tregs and CD4+CD25? Cells in Mice

Background

Regulatory T cells (Tregs) were shown to be central in maintaining immunological homeostasis and preventing the development of autoimmune diseases. Several subsets of Tregs have been identified to date; however, the dynamics of the interactions between these subsets, and their implications on their regulatory functions are yet to be elucidated.

Methodology/Principal Findings

We employed a combination of mathematical modeling and frequent in vivo measurements of several T cell subsets. Healthy BALB/c mice received a single injection of either hCDR1 - a tolerogenic peptide previously shown to induce Tregs, a control peptide or vehicle alone, and were monitored for 16 days. During this period, splenocytes from the treated mice were analyzed for the levels of CD4, CD25, CD8, CD28 and Foxp3. The collected data were then fitted to mathematical models, in order to test competing hypotheses regarding the interactions between the followed T cell subsets. In all 3 treatment groups, a significant, lasting, non-random perturbation of the immune system could be observed. Our analysis predicted the emergence of functional CD4 Tregs based on inverse oscillations of the latter and CD4⁺CD25⁻ cells. Furthermore, CD4 Tregs seemed to require a sufficiently high level of CD8 Tregs in order to become functional, while conversion was unlikely to be their major source. Our results indicated in addition that Foxp3 is not a sufficient marker for regulatory activity.

Conclusions/Significance

In this work, we unraveled the dynamics of the interplay between CD4, CD8 Tregs and effector T cells, using, for the first time, a mathematical-mechanistic perspective in the analysis of Treg kinetics. Furthermore, the results obtained from this interdisciplinary approach supported the notion that CD4 Tregs need to interact with CD8 Tregs in order to become functional. Finally, we generated predictions regarding the time-dependent function of Tregs, which can be further tested empirically in future work.     

Sulindac Enhances the Killing of Cancer Cells Exposed to Oxidative Stress

Background

Sulindac is an FDA-approved non-steroidal anti-inflammatory drug (NSAID) that affects prostaglandin production by inhibiting cyclooxygenases (COX) 1 and 2. Sulindac has also been of interest for more than decade as a chemopreventive for adenomatous colorectal polyps and colon cancer.

Principal Findings

Pretreatment of human colon and lung cancer cells with sulindac enhances killing by an oxidizing agent such as tert-butyl hydroperoxide (TBHP) or hydrogen peroxide. This effect does not involve cyclooxygenase (COX) inhibition. However, under the conditions used, there is a significant increase in reactive oxygen species (ROS) within the cancer cells and a loss of mitochondrial membrane potential, suggesting that cell death is due to apoptosis, which was confirmed by Tunel assay. In contrast, this enhanced killing was not observed with normal lung or colon cells.

Significance

These results indicate that normal and cancer cells handle oxidative stress in different ways and sulindac can enhance this difference. The combination of sulindac and an oxidizing agent could have therapeutic value.