1,826 research outputs found
Small-Angle Scattering and Diffusion: Application to Relativistic Shock Acceleration
We investigate ways of accurately simulating the propagation of energetic
charged particles over small times where the standard Monte Carlo approximation
to diffusive transport breaks down. We find that a small-angle scattering
procedure with appropriately chosen step-lengths and scattering angles gives
accurate results, and we apply this to the simulation of propagation upstream
in relativistic shock acceleration.Comment: 4 pages, 2 figures, proceedings of World Space Environment Forum
(WSEF2002) to appear in Space Science Reviews, accepte
Answers in a flash; optical analysis of exocytosis in human cultured endothelial cells
Endothelial cells line all of our blood vessels. They monitor and respond to
signals generated during injury, infection and disease by releasing a wide range of
molecules that regulate blood flow, coagulation, inflammatory responses and
vessel growth. Protein mediators are released by exocytosis of intracellular
organelles, and a major trigger for this type of secretion is an increase in
intracellular free calcium ion concentration ([Ca2+]i). Mitochondria are thought to
influence Ca2+ homeostasis through local Ca2+ buffering. Due to a lack of
sensitive and time-resolved assays for endothelial exocytosis little is known about
the precise relationship between Ca2+-signalling and exocytosis, and the influence
of Ca2+ buffering by mitochondria.
Using fluorescence and biochemical techniques I have investigated the
relationship between secretagogue-evoked Ca2+-signalling and the influence of
mitochondrial function on the exocytosis of two distinct organelle populations in
cultures of Human Umbilical Vein Endothelial Cells (HUVEC); 1) the Weibel-Palade body (WPB) the main storage organelle for pro-coaguland and
inflammatory mediators, and 2) the non-WPB, a non-stored and morphologically distinct organelle that can contain a range of inflammatory and anti-coagulant
molecules.
These two distinct organelle populations were labeled for fluorescence
microscopy by targeted expression of chimeras of green (EGFP) or red (mRFP)
fluorescent proteins in living HUVEC. Exocytosis was evoked by both
physiological and pharmacological secretogogues that increase [Ca2+]i. The times
of exocytosis of individual organelles were monitored by flashes of light from
granule EGFP, produced by pH changes within the organelle upon fusion. In the
same experiments, [Ca2+]i and intra-mitochondrial Ca2+ concentration ([Ca2+]m)
were monitored using fluorescent Ca2+-indicators.
The data obtained has defined more precisely the relationship between
agonist-evoked changes in [Ca2+]i and secretory vesicle exocytosis in HUVEC.
These studies will contribute to a better understanding of the processes that
regulate secretion of biomolecules from the endothelium
Particle-in-cell simulation of a mildly relativistic collision of an electron-ion plasma carrying a quasi-parallel magnetic field: Electron acceleration and magnetic field amplification at supernova shocks
Plasma processes close to SNR shocks result in the amplification of magnetic
fields and in the acceleration of electrons, injecting them into the diffusive
acceleration mechanism. The acceleration of electrons and the B field
amplification by the collision of two plasma clouds, each consisting of
electrons and ions, at a speed of 0.5c is investigated. A quasi-parallel
guiding magnetic field, a cloud density ratio of 10 and a plasma temperature of
25 keV are considered. A quasi-planar shock forms at the front of the dense
plasma cloud. It is mediated by a circularly left-hand polarized
electromagnetic wave with an electric field component along the guiding
magnetic field. Its propagation direction is close to that of the guiding field
and orthogonal to the collision boundary. It has a low frequency and a
wavelength that equals several times the ion inertial length, which would be
indicative of a dispersive Alfven wave close to the ion cyclotron resonance
frequency of the left-handed mode (ion whistler), provided that the frequency
is appropriate. However, it moves with the super-alfvenic plasma collision
speed, suggesting that it is an Alfven precursor or a nonlinear MHD wave such
as a Short Large-Amplitude Magnetic Structure (SLAMS). The growth of the
magnetic amplitude of this wave to values well in excess of those of the
quasi-parallel guiding field and of the filamentation modes results in a
quasi-perpendicular shock. We present evidence for the instability of this mode
to a four wave interaction. The waves developing upstream of the dense cloud
give rise to electron acceleration ahead of the collision boundary. Energy
equipartition between the ions and the electrons is established at the shock
and the electrons are accelerated to relativistic speeds.Comment: 16 pages, 18 figures, Accepted for publication by Astron & Astrophy
New perspectives on the potential role of aquaporins (AQPs) in the physiology of inflammation
Aquaporins (AQPs) are emerging, in the last few decades, as critical proteins regulating
water fluid homeostasis in cells involved in inflammation. AQPs represent a family of
ubiquitous membrane channels that regulate osmotically water flux in various tissues
and sometimes the transport of small solutes, including glycerol. Extensive data indicate
that AQPs, working as water channel proteins, regulate not only cell migration, but also
common events essential for inflammatory response. The involvement of AQPs in several
inflammatory processes, as demonstrated by their dysregulation both in human and
animal diseases, identifies their new role in protection and response to different noxious
stimuli, including bacterial infection. This contribution could represent a new key to clarify
the dilemma of host-pathogen communications, and opens up new scenarios regarding
the investigation of the modulation of specific AQPs, as target for new pharmacological
therapies. This review provides updated information on the underlying mechanisms of
AQPs in the regulation of inflammatory responses in mammals and discusses the broad
spectrum of options that can be tailored for different diseases and their pharmacological
treatment
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