Instability Proof for Einstein-Yang-Mills Solitons and Black Holes with Arbitrary Gauge Groups

We prove that static, spherically symmetric, asymptotically flat soliton and black hole solutions of the Einstein-Yang-Mills equations are unstable for arbitrary gauge groups, at least for the ``generic" case. This conclusion is derived without explicit knowledge of the possible equilibrium solutions.Comment: 26 pages, LATEX, no figure

Energy barrier in the two-Higgs model

The electroweak model is extended by a second Higgs doublet and a numerical investigation of static, finite energy classical solutions is performed. The results indicate that for a large domain of the parameters of the Higgs potential, the energy barrier between topologically distinct vacua of the Lagrangian is constituted by a bisphaleron.Comment: 19 pages, including 4 eps figures, LaTex format, new results include

Reduced expression of Toll-like receptor 4 contributes to impaired cytokine response of monocytes in uremic patients

Toll-like receptors (TLRs) play a pivotal role in pathogen recognition and subsequent cytokine synthesis by immune cells. Uremic patients have a high infectious morbidity, but it remains unclear if this arises from the defective innate immune responses related to TLRs. We studied TLR4 expression in monocytes and their intracellular cytokine synthesis in response to lipopolysaccharide (LPS) stimulation in 35 predialysis patients with chronic kidney disease (CKD) with or without predisposition to bacterial infections and 16 age-matched controls. Expression of TLR4 in unstimulated peripheral monocytes was determined by staining with anti-TLR4 antibody and analysis with flow cytometry. Monocytes were then stimulated by LPS, labeled with anti-CD14 antibody, and subjected to intracellular cytokine staining and flow cytometry. Tumor necrosis factor (TNF)-α, interleukin (IL)-1β, IL-6, and IL-8 synthesis was examined in CD14+ monocytes. TLR4 expression was constitutively diminished in CKD patients with reduced expression being more severe in those CKD patients who were predisposed to infections. Monocytes from these infection prone CKD patients exhibited significantly reduced synthesis of TNF-α, IL-1β, IL-6, and IL-8 in response to LPS challenge compared with those from control subjects. The intensity of synthesis of each cytokine significantly correlated with TLR4 expression levels in monocytes (P<0.01). The capacity of monocytes to synthesize proinflammatory cytokines was significantly reduced in infection prone CKD patients, and this may possibly be due to the reduced monocyte expression of TLR4. Abnormal TLR4 expression by monocytes may play a role in the susceptibility of such patients to bacterial infections

The Born-Infeld Sphaleron

We study the SU(2) electroweak model in which the standard Yang-Mills coupling is supplemented by a Born-Infeld term. The deformation of the sphaleron and bisphaleron solutions due to the Born-Infeld term is investigated and new branches of solutions are exhibited. Especially, we find a new branch of solutions connecting the Born-Infeld sphaleron to the first solution of the Kerner-Gal'tsov series.Comment: 8 pages, 5 Postscript figures; new results on Bisphalerons added; minor modification

Lafutidine, a Protective H2 Receptor Antagonist, Enhances Mucosal Defense in Rat Esophagus

Luminal acid or CO2 induces a hyperemic response in the esophagus, via activation of acid sensors on capsaicin-sensitive afferent nerves (CSAN). Since disruption of the hyperemic response to luminal CO2 acidifies the interstitium of the esophageal mucosa, the hyperemic response may maintain interstitial pH (pHint). We hypothesized that acid-related hyperemia maintains pHint, preventing acid-induced injury in the esophageal mucosa. We examined the effects of capsaicin (Cap) or lafutidine (Laf), a mucosal protective H2 antagonist, on the regulation of pHint and blood flow in rat esophagus using ratiometric microimaging and laser-Doppler measurements of the lower esophageal mucosa of living rats. The esophagus was topically superfused with pH 7.0 buffer, or a pH 1.0 or pH 1.0 + pepsin (1 mg/ml) solution with or without Laf. Cap (30 or 100 µM) or Laf (0.1 or 1 mM) dose-dependently increased blood flow, accompanied by increased pHint. The pH 1.0 solution increased blood flow without pHint change, whereas Laf (1 mM) increased blood flow and pHint during acid exposure. The effects of Laf were abolished by ablation of CSAN. Perfusion of the acidified pepsin solution gradually decreased pHint, inhibited by Laf perfusion. Activation of CSAN by Laf with or without acid, accompanied by hyperemia, increased pHint, preventing acidified pepsin-induced interstitial acidification. Stimulation of the capsaicin pathway with compounds such as Laf enhances mucosal protection from acid-related injury in the upper gastrointestinal tract