2,029 research outputs found
Reimann's "Habitual Hyperthermia" Responding to Hormone Therapy.
A 25-year-old woman presented with fever of unknown origin, exhibiting malaise and low-grade fevers in evenings. These fevers exhibited a pattern of starting mid-menstrual cycle with resolution around the onset of menses, matching a pattern of "habitual hyperthermia" reported by H. Reimann in the 1930s. Extensive workup was unremarkable, and the fevers improved on oral synthetic estrogen and progesterone therapy
A stochastic multi-scale model of HIV-1 transmission for decision-making: application to a MSM population.
BackgroundIn the absence of an effective vaccine against HIV-1, the scientific community is presented with the challenge of developing alternative methods to curb its spread. Due to the complexity of the disease, however, our ability to predict the impact of various prevention and treatment strategies is limited. While ART has been widely accepted as the gold standard of modern care, its timing is debated.ObjectivesTo evaluate the impact of medical interventions at the level of individuals on the spread of infection across the whole population. Specifically, we investigate the impact of ART initiation timing on HIV-1 spread in an MSM (Men who have Sex with Men) population.Design and methodsA stochastic multi-scale model of HIV-1 transmission that integrates within a single framework the in-host cellular dynamics and their outcomes, patient health states, and sexual contact networks. The model captures disease state and progression within individuals, and allows for simulation of therapeutic strategies.ResultsEarly ART initiation may substantially affect disease spread through a population.ConclusionsOur model provides a multi-scale, systems-based approach to evaluate the broader implications of therapeutic strategies
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Determinant of HIV-1 mutational escape from cytotoxic T lymphocytes.
CD8+ class I-restricted cytotoxic T lymphocytes (CTLs) usually incompletely suppress HIV-1 in vivo, and while analogous partial suppression induces antiretroviral drug-resistance mutations, epitope escape mutations are inconsistently observed. However, escape mutation depends on the net balance of selective pressure and mutational fitness costs, which are poorly understood and difficult to study in vivo. Here we used a controlled in vitro system to evaluate the ability of HIV-1 to escape from CTL clones, finding that virus replicating under selective pressure rapidly can develop phenotypic resistance associated with genotypic changes. Escape varied between clones recognizing the same Gag epitope or different Gag and RT epitopes, indicating the influence of the T cell receptor on pressure and fitness costs. Gag and RT escape mutations were monoclonal intra-epitope substitutions, indicating limitation by fitness constraints in structural proteins. In contrast, escape from Nef-specific CTL was more rapid and consistent, marked by a polyclonal mixture of epitope point mutations and upstream frameshifts. We conclude that incomplete viral suppression by CTL can result in rapid emergence of immune escape, but the likelihood is strongly determined by factors influencing the fitness costs of the particular epitope targeted and the ability of responding CTL to recognize specific epitope variants
Dysfunctional HDL and progression of atherosclerosis in HIV-1-infected and -uninfected adults
Background: HDL function rather than absolute level may be a more accurate indicator for risk of developing atherosclerosis. Dysfunctional HDL has increased redox activity and reduced antioxidant properties, but it is unknown whether abnormal HDL function is associated with progression of atherosclerosis in HIV-1-infected subjects. Findings: We retrospectively measured serum HDL function in 91 subjects from a prospective 3-year study of carotid artery intima-media thickness (CIMT), which enrolled triads of risk factor-matched persons that were HIV-1-uninfected (n=36) or HIV-1+ with (n=29) or without (n=26) protease inhibitor (PI)-based therapy for â„ 2 years. HDL function was assessed using a biochemical assay that measures the oxidation of dihydrorhodamine 123 (DHR oxidation rate, DOR), in which higher DOR readout corresponds to dysfunctional HDL phenotype. There were no significant associations between DOR and HIV-1 infection. In univariate analysis of 55 HIV-1-infected subjects, greater waist circumference and lower serum HDL were significantly associated with higher baseline levels of DOR (p=0.01). These subjects had significant increases in levels of DOR over time (3 years) that were associated with white race (p=0.03), higher nadir CD4 count (p0.1) (DOR), were significantly associated (p=0.02) with progression of CIMT. Conclusion: In a small matched cohort study of HIV-1-infected subjects who had a low cardiovascular risk profile, HDL function changed over time and was independently associated with anthropometric parameters of obesity but not with progression of CIMT
Decreased perforin and granzyme B expression in senescent HIV-1-specific cytotoxic T lymphocytes
AbstractCytotoxic T lymphocyte (CTL) senescence may be an important mechanism of immune failure in HIV-1 infection. We find that senescence of HIV-1-specific CTL clones causes loss of killing activity, preventable by transduction with telomerase. Furthermore, senescence is associated with reduced expression of the effector molecules granzyme and perforin, suggesting CTL âexhaustionâ can result in hypofunction. These results agree with other studies showing that HIV-1-specific CTL exhibit abnormal phenotypes in vivo, and suggest the possibility that chronic turnover is an important mechanism of antiviral failure in HIV-1 infection
Galactic S Stars: Investigations of Color, Motion, and Spectral Features
Known bright S stars, recognized as such by their enhanced s-process
abundances and C/O ratio, are typically members of the asymptotic giant branch
(AGB) or the red giant branch (RGB). Few modern digital spectra for these
objects have been published, from which intermediate resolution spectral
indices and classifications could be derived. For published S stars we find
accurate positions using the Two-Micron All Sky Survey (2MASS), and use the
FAST spectrograph of the Tillinghast reflector on Mt. Hopkins to obtain the
spectra of 57 objects. We make available a digital S star spectral atlas
consisting of 14 spectra of S stars with diverse spectral features. We define
and derive basic spectral indices that can help distinguish S stars from
late-type (M) giants and carbon stars. We convolve all our spectra with the
SDSS bandpasses, and employ the resulting gri magnitudes together with 2MASS
JHK mags to investigate S star colors. S stars have colors similar to carbon
and M stars, and are therefore difficult to distinguish by color alone. Using
near and mid-infrared colors from IRAS and AKARI, we identify some of the stars
as intrinsic (AGB) or extrinsic (with abundances enhanced by past
mass-transfer). We also use V band and 2MASS magnitudes to calculate a
temperature index for stars in the sample. We analyze the proper motions and
parallaxes of our sample stars to determine upper and lower limit absolute
magnitudes and distances, and confirm that most are probably giants.Comment: 11 pages. Accepted for publication in ApJS July 19, 2011. Spectra
available as http://hea-www.harvard.edu/~pgreen/SStarAtlas.ta
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