Publications by authors named "Marissa Braff"

is an important cause of acute bacterial pneumonia. Toll-like receptor 2 (TLR2) recognizes multiple components of the bacterial cell wall and activates innate immune responses to gram-positive bacteria. We hypothesized that TLR2 would have an important role in pulmonary host defense against TLR null (TLR2) mice and wild type (WT) C57BL/6 controls were challenged with aerosolized at a range of inocula for kinetic studies of cytokine and antimicrobial peptide expression, lung inflammation, bacterial killing by alveolar macrophages, and bacterial clearance.

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The increasing prevalence of Staphylococcus aureus strains isolated from hospital- and community-acquired respiratory tract infections is an important public health concern worldwide. The majority of S. aureus strains produce staphylokinase, a plasminogen activator capable of inactivating neutrophil alpha-defensins and of impairing phagocytosis via opsonin degradation.

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Cathelicidins are antimicrobial peptides of the innate immune system that establish an antimicrobial barrier at epithelial interfaces and have been proposed to have a proinflammatory function. We studied the role of cathelicidin in allergic contact dermatitis, a model requiring dendritic cells of the innate immune response and T cells of the adaptive immune response. Deletion of the murine cathelicidin gene Cnlp enhanced an allergic contact response, whereas local administration of cathelicidin before sensitization inhibited the allergic response.

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Article Synopsis
  • Immune defense at the skin interface relies on the physical and chemical barriers provided by epithelial and immune cells, primarily through antimicrobial peptides produced by keratinocytes and neutrophils.
  • Research shows that keratinocyte-derived cathelicidin plays a crucial role in protecting against infections like group A streptococcus and Staphylococcus aureus.
  • This study emphasizes the importance of understanding epithelial antimicrobial functions in improving the diagnosis and treatment of skin infections.
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The skin actively contributes to host defense by mounting an innate immune response that includes the production of antimicrobial peptides. These peptides, which include but are not limited to the cathelicidin and defensin gene families, provide rapid, broad-spectrum defense against infection by acting as natural antibiotics and by participating in host cell processes involved in immune defense. This review discusses the biology and clinical relevance of antimicrobial peptides expressed in the skin.

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Cathelicidins and other antimicrobial peptides are deployed at epithelial surfaces to defend against infection. These molecules have broad-spectrum killing activity against microbes and can have effects on specific mammalian cell types, potentially stimulating additional immune defense through direct chemotactic activity or induction of cytokine release. In humans, the cathelicidin hCAP18/LL-37 is processed to LL-37 in neutrophils, but on skin it can be further proteolytically processed to shorter forms.

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Article Synopsis
  • The innate immune system uses physical barriers and immune cells to defend against microbial pathogens, with antimicrobial peptides (like cathelicidin) playing a crucial role.
  • Cathelicidin production is particularly significant in the skin, as shown by studies on mice lacking this peptide, which are more prone to infections.
  • Research indicates that cathelicidin primarily resides in certain cellular granules in skin cells (keratinocytes), and its distribution and processing are critical for enhancing skin's immune defense against pathogens.
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The production of antimicrobial peptides and proteins is essential for defense against infection. Many of the known human antimicrobial peptides are multifunctional, with stimulatory activities such as chemotaxis while simultaneously acting as natural antibiotics. In humans, eccrine appendages express DCD and CAMP, genes encoding proteins processed into the antimicrobial peptides dermcidin and LL-37.

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