Gold sodium thiomalate toxicity in cadmium-sensitive and cadmium-resistant Chinese hamster ovary cells

Gold sodium thiomalate was incubated with one cadmium-sensitive cell line and two cadmium-resistant variants. The resistant lines have been reported to synthesize metallothionein (MT) in response to both cadmium and zinc, whereas the sensitive line does not. All cell lines showed a dose-dependent inhibition of growth as a result of gold sodium thiomalate treatment. However, daily comparisons of cell numbers indicate that the cadmium-resistant lines actually increase in number at the highest gold concentrations, whereas numbers of cells in the nonresistant line decrease. MT biosynthesis was measured by monitoring the incorporation of [35S )cysteine into low molecular weight protein. None of the cells synthesized MT in response to gold. When incubated with both zinc and gold, MT was synthesized by both of the cadmium resistant lines; however, the amount of MT synthesized was reduced in the presence of gold which appears to inhibit the uptake of [35S]cysteine by all the cell lines. Although MT is synthesized in the presence of zinc and gold sodium thiomalate, the MT does not have a significant effect on the ability of these cells to withstand high concentrations of gold.     

Investigation into the experimental kinetic support of the two-state model of the cell cycle

Five previously published cell generation-time distribution functions have been examined in an effort to elucidate the parameters of the two-state model of the cell cycle. These parameters are the fractional number of cells that bypass the G0 state, the probability of exit from G0, and the distribution of traversal times through the active state. To explain observed beta-curve behavior of cell populations, it is necessary to define the parameters in terms of pairwise behavior of newborn sister cells. From the beta-curve, we demonstrate that at least 50% of the cells must pass through the G0 state. The alpha-curve is consistent with any positive fraction of newborn cells passing through the G0 state, and provides no further information. We explore a possible method for resolving the remaining indeterminacy regarding the number of cells bypassing the G0 state, namely, examination of the generation-time distribution functions of fast sister cells only. Such an approach, although theoretically attractive, presents formidable experimental difficulties, however. If it should turn out that indeed only 50% of the cells are apparently passing through a random-exiting phase of the cell cycle, then an alterative plausible biological mechanism for the observed variability in generation times is supplied by Prescott's hypothesis: variability is a consequence of the inequality in the metabolic content of sister cells at birth.     

Quantitative PCR: Procedures and precisions

We develop a multitype branching-process model for the Polymerase Chain Reaction (PCR). We apply the model to a comparison of three methods for estimating the initial number of molecules of target present in a PCR. These three methods are: one which uses a coamplified, internal control; one which uses an external control series; and one which uses simple extrapolation of log outputvs time (no control). We identify assumptions for each method which permit mathematical analysis of bias and precision. All three methods perform well if: (1) replication efficiencies are stable among reactions; (2) other method-specific conditions on efficiencies are met; and (3) product accumulates exponentially throughout the range where it is observed. When replication efficiencies vary among reactions but other optimal conditions for each method hold, the no-control and external-control methods lose precision relative to the internal control method, but they may still perform satisfactorily for many applications. The internal control method continues to perform well even if accumulation of product plateaus. This method depends, however, on a condition we call equivalence of replication efficiencies, the attainability of which in practice remains to be proven.     

Facilitated diffusion of oxygen and carbon monoxide in the large affinity regime

Wyman's equation for facilitated diffusion of a ligand through a solution slab containing a carrier is recast and solved by means of a regular perturbation expansion in the parameter representing the driving force for facilitation. This new solution is complementary to the previously exploited singular perturbation solution due to Murray and represents facilitation in the low facilitation parameter regime. The most significant physical realization of this regime occurs when there is a large affinity between ligand and carrier, as in the carbon monoxide-hemoglobin system.The validity domains of the regular perturbation solution and the singular perturbation solution of Mitchell and Murray and Rubinow and Dembo are delineated. The equation for facilitated diffusion is solved numerically for parameter values appropriate to the oxygen-myoglobin experiments of Wittenberg, and to the carbon monoxide-hemoglobin experiments of Mochizuki and Forster, and Wittenberg. This solution provides a norm for comparison of the utility of the perturbation solutions.We show how the theory explains the apparent contradiction between the positive observations of Mochizuki and Forster and the negative observations of Wittenberg on facilitation of carbon monoxide transport through a slab of hemoglobin solution.Supported in part by the National Science Foundation under Grant No. PCM77-03344In partial fulfillment of the Ph.D. degree at Cornell UniversityProfessor S. I. Rubinow has passed away on February 22, 1981Computations were performed at the Courant Mathematics and Computing Laboratory, supported by DOE under contract #EY-76-C-02-3077.     

Correlating changes in lung function with patient outcomes in chronic obstructive pulmonary disease: a pooled analysis

Background

Relationships between improvements in lung function and other clinical outcomes in chronic obstructive pulmonary disease (COPD) are not documented extensively. We examined whether changes in trough forced expiratory volume in 1 second (FEV₁) are correlated with changes in patient-reported outcomes.

Methods

Pooled data from three indacaterol studies (n = 3313) were analysed. Means and responder rates for outcomes including change from baseline in Transition Dyspnoea Index (TDI), St. George''s Respiratory Questionnaire (SGRQ) scores (at 12, 26 and 52 weeks), and COPD exacerbation frequency (rate/year) were tabulated across categories of ΔFEV₁. Also, generalised linear modelling was performed adjusting for covariates such as baseline severity and inhaled corticosteroid use.

Results

With increasing positive ΔFEV₁, TDI and ΔSGRQ improved at all timepoints, exacerbation rate over the study duration declined (P < 0.001). Individual-level correlations were 0.03-0.18, but cohort-level correlations were 0.79-0.95. At 26 weeks, a 100 ml increase in FEV₁ was associated with improved TDI (0.46 units), ΔSGRQ (1.3-1.9 points) and exacerbation rate (12% decrease). Overall, adjustments for baseline covariates had little impact on the relationship between ΔFEV₁ and outcomes.

Conclusions

These results suggest that larger improvements in FEV₁ are likely to be associated with larger patient-reported benefits across a range of clinical outcomes.

Trial Registration

ClinicalTrials.gov {"type":"clinical-trial","attrs":{"text":"NCT00393458","term_id":"NCT00393458"}}NCT00393458, {"type":"clinical-trial","attrs":{"text":"NCT00463567","term_id":"NCT00463567"}}NCT00463567, and {"type":"clinical-trial","attrs":{"text":"NCT00624286","term_id":"NCT00624286"}}NCT00624286     

Error analysis in flow microfluorometry

Sources of error in a typical algorithm for the analysis of single flow-microfluorometric histograms are identified. A new statistical model for such data is presented, by means of which the error sources are quantitatively investigated. These theoretical investigations lead to three practical observations: A more detailed characterization of the fluorescence dispersion process is needed for a more refined algorithm. Levels of dispersion typically experienced are such that from a single histogram the distribution of cells within S-phase cannot be finely resolved; but the crude distribution of cells among the three phases G₁, S, and G₂-M may be accurately estimated. If currently typical levels of dispersion can be halved, then the S-phase distribution can be finely resolved.     

Use of Anisotropy, 3D Segmented Atlas,and Computational Analysis to Identify Gray Matter Subcortical Lesions Common to Concussive Injury from Different Sites on the Cortex

Traumatic brain injury (TBI) can occur anywhere along the cortical mantel. While the cortical contusions may be random and disparate in their locations, the clinical outcomes are often similar and difficult to explain. Thus a question that arises is, do concussions at different sites on the cortex affect similar subcortical brain regions? To address this question we used a fluid percussion model to concuss the right caudal or rostral cortices in rats. Five days later, diffusion tensor MRI data were acquired for indices of anisotropy (IA) for use in a novel method of analysis to detect changes in gray matter microarchitecture. IA values from over 20,000 voxels were registered into a 3D segmented, annotated rat atlas covering 150 brain areas. Comparisons between left and right hemispheres revealed a small population of subcortical sites with altered IA values. Rostral and caudal concussions were of striking similarity in the impacted subcortical locations, particularly the central nucleus of the amygdala, laterodorsal thalamus, and hippocampal complex. Subsequent immunohistochemical analysis of these sites showed significant neuroinflammation. This study presents three significant findings that advance our understanding and evaluation of TBI: 1) the introduction of a new method to identify highly localized disturbances in discrete gray matter, subcortical brain nuclei without postmortem histology, 2) the use of this method to demonstrate that separate injuries to the rostral and caudal cortex produce the same subcortical, disturbances, and 3) the central nucleus of the amygdala, critical in the regulation of emotion, is vulnerable to concussion.