63 research outputs found
The interaction of Thrombospondins with extracellular matrix proteins
The thrombospondins (TSPs) are a family of five matricellular proteins that appear to function as adapter molecules to guide extracellular matrix synthesis and tissue remodeling in a variety of normal and disease settings. Various TSPs have been shown to bind to fibronectin, laminin, matrilins, collagens and other extracellular matrix (ECM) proteins. The importance of TSP-1 in this context is underscored by the fact that it is rapidly deposited at the sites of tissue damage by platelets. An association of TSPs with collagens has been known for over 25Β years. The observation that the disruption of the TSP-2 gene in mice leads to collagen fibril abnormalities provided important in vivo evidence that these interactions are physiologically important. Recent biochemical studies have shown that TSP-5 promotes collagen fibril assembly and structural studies suggest that TSPs may interact with collagens through a highly conserved potential metal ion dependent adhesion site (MIDAS). These interactions are critical for normal tissue homeostasis, tumor progression and the etiology of skeletal dysplasias
Loss of expression of TGF-Ξ²s and their receptors in chronic skin lesions induced by sulfur mustard as compared with chronic contact dermatitis patients
<p>Abstract</p> <p>Background</p> <p>Sulfur mustard (SM) is a blister-forming agent that has been used as a chemical weapon. Sulfur mustard can cause damage in various organs, especially the skin, respiratory system, and eyes. Generally, the multiple complications of mustard gas result from its alkalizing potency; it reacts with cellular components like DNA, RNA, proteins, and lipid membranes.</p> <p>TGF-Ξ² is a multi-functional cytokine with multiple biological effects ranging from cell differentiation and growth inhibition to extracellular matrix stimulation, immunosuppression, and immunomodulation. TGF-Ξ² has 3 isoforms (TGF-Ξ² 1, 2, 3) and its signaling is mediated by its receptors: R1, R2 and intracellular Smads molecules.</p> <p>TGF-Ξ² has been shown to have anti-inflammatory effects. TGF-Ξ²s and their receptors also have an important role in modulation of skin inflammation, proliferation of epidermal cells, and wound healing, and they have been implicated in different types of skin inflammatory disorders.</p> <p>Methods</p> <p>Seventeen exposed SM individuals (48.47 Β± 9.3 years), 17 chronic dermatitis patients (46.52 Β± 14.6 years), and 5 normal controls (44.00 Β± 14.6 years) were enrolled in this study.</p> <p>Evaluation of TGF-Ξ²s and their receptors expressions was performed by semiquantitative RT-PCR. Only TGF1was analyzed immunohistochemically.</p> <p>Results</p> <p>Our results showed significant decreases in the expression percentages of TGF-Ξ² 1, 2 and R1, R2 in chemical victims in comparison with chronic dermatitis and normal subjects and significant decreases in the intensity of R1 and R2 expressions in chemical victims in comparison with chronic dermatitis and normal controls. (P value < 0.05)</p> <p>Conclusions</p> <p>TGF-Ξ²s and their receptors appear to have a noticeable role in chronic inflammatory skin lesions caused by sulfur mustard.</p
Demonstration of the Blood-Stage Plasmodium falciparum Controlled Human Malaria Infection Model to Assess Efficacy of the P. falciparum Apical Membrane Antigen 1 Vaccine, FMP2.1/AS01
We study whether the relationship between the state unemployment rate at the time of conception
and infant health, infant mortality and maternal characteristics in the United States
has changed over the years 1980-2004. We use microdata on births and deaths for years
1980-2004 and find that the relationship between the state unemployment rate at the time of
conception and infant mortality and birthweight changes over time and is stronger for blacks
than whites. For years 1980-1989 increases in the state unemployment rate are associated
with a decline in infant mortality among blacks, an effect driven by mortality from gestational
development and birth weight, and complications of placenta while in utero. In contrast,
state economic conditions are unrelated to black infant mortality in years 1990-2004 and
white infant mortality in any period, although effects vary by cause of death. We explore potential
mechanisms for our findings and, including mothers younger than 18 in the analysis,
uncover evidence of age-related maternal selection in response to the business cycle. In
particular, in years 1980-1989 an increase in the unemployment rate at the time of conception
is associated with fewer babies born to young mothers. The magnitude and direction of
the relationship between business cycles and infant mortality differs by race and period.
Age-related selection into motherhood in response to the business cycle is a possible explanation
for this changing relationship
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