Publications by authors named "A Wille"

Members of the phospholipase D (PLD) superfamily found in Loxosceles spider venoms are potent toxins with inflammatory and necrotizing activities. They degrade phospholipids in cell membranes, generating bioactive molecules that activate skin cells. These skin cells, in turn, activate leukocytes involved in dermonecrosis, characterized by aseptic coagulative necrosis.

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Loxoscelism is the pathological condition triggered by a brown spider bite. The venom of these spiders is rich in phospholipases D (PLDs), which can induce virtually all local and systemic manifestations. Recombinant mutated PLDs from clinically relevant Loxosceles species in South America have been investigated as potential antigens to develop novel therapeutic strategies for loxoscelism.

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Article Synopsis
  • Auto-injectors typically require refrigeration, and if not warmed, they may not deliver the full drug dose due to their mechanical design not compensating for changes in drug viscosity.
  • A new piezoelectric micro diaphragm pump has been developed to effectively deliver high-viscosity liquids (up to 25 mPa·s) using a specialized design, achieving fluid pressures of up to 368 kPa.
  • Experimental results show that this micropump can produce maximum flow rates of 2 mL/min through 27G needles, paving the way for more advanced auto-injectors capable of handling thick medications.
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Sphingosine-1-phosphate (S1P) plays multiple roles in bone metabolism and regeneration. Here, we have identified a novel S1P-regulated osteoanabolic mechanism functionally connecting osteoblasts (OBs) to the highly specialized bone vasculature. We demonstrate that S1P/S1PR3 signaling in OBs stimulates vascular endothelial growth factor a (VEGFa) expression and secretion to promote bone growth in an autocrine and boost osteogenic H-type differentiation of bone marrow endothelial cells in a paracrine manner.

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