Anaplasma phagocytophilum Induces TLR- and MyD88-Dependent Signaling in In Vitro Generated Murine Neutrophils

Abstract: Anaplasma phagocytophilum is a tick-transmitted obligate intracellular Gram-negative bacterium that replicates in neutrophils. It elicits febrile disease in humans and in animals. In a mouse model, elimination of A. phagocytophilum required CD4+ T cells, but was independent of IFN-γ and other classical antibacterial effector mechanisms. Further, mice deficient for immune recognition and signaling via Toll-like receptor (TLR) 2, TLR4 or MyD88 were unimpaired in pathogen control. In contrast, animals lacking ada… Show more

“…Recently, the link between MyD88-or TRIF-dependent TLRs and inflammation has been explored via in vitro and in vivo approaches. Infected MyD88 −/− , MyD88/ TRIF −/− , and TLR2/3/4/7/9 −/− murine Hoxb8 neutrophils, compared with WT cells, show diminished proinflammatory responses (Nos2 transcripts; TNFα, CCL4, and CCL5 secretion) [98]. Despite differences in inflammation in vitro, no phenotypic differences have been observed in vivo between infected WT C57BL/6 and TRIF −/− mice.…”

“…The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98]. In experiments using Hoxb8 murine neutrophils, no differences in bacterial load or proinflammatory markers have been observed among infected WT, NOD1 −/− , NOD2 −/− , and NLRP3 −/− cells [98]. However, A. phagocytophilum has been shown to activate NLRC4 via a unique mechanism.…”

“…Vacuole NOD2 [98] RIP2 [98] NLRC4 [100] MyD88 [98] TLR2 [96] STAT1 [96] Ehrlichia chaffeensis White-tailed deer*, coyotes, and dogs Unknown Amblyomma*, Ixodes, and Dermacentor…”

“…Thus, NLRs signaling through RIP2 have been speculated to contribute to mounting of the Th1 response to Anaplasma [99]. A separate study by Müller and colleagues has built upon this hypothesis by analyzing the contributions of specific NLRs during infection [98]. The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98].…”

“…A separate study by Müller and colleagues has built upon this hypothesis by analyzing the contributions of specific NLRs during infection [98]. The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98]. In experiments using Hoxb8 murine neutrophils, no differences in bacterial load or proinflammatory markers have been observed among infected WT, NOD1 −/− , NOD2 −/− , and NLRP3 −/− cells [98].…”

Pattern Recognition Receptors in Innate Immunity to Obligate Intracellular Bacteria

“…Recently, the link between MyD88-or TRIF-dependent TLRs and inflammation has been explored via in vitro and in vivo approaches. Infected MyD88 −/− , MyD88/ TRIF −/− , and TLR2/3/4/7/9 −/− murine Hoxb8 neutrophils, compared with WT cells, show diminished proinflammatory responses (Nos2 transcripts; TNFα, CCL4, and CCL5 secretion) [98]. Despite differences in inflammation in vitro, no phenotypic differences have been observed in vivo between infected WT C57BL/6 and TRIF −/− mice.…”

“…The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98]. In experiments using Hoxb8 murine neutrophils, no differences in bacterial load or proinflammatory markers have been observed among infected WT, NOD1 −/− , NOD2 −/− , and NLRP3 −/− cells [98]. However, A. phagocytophilum has been shown to activate NLRC4 via a unique mechanism.…”

“…Vacuole NOD2 [98] RIP2 [98] NLRC4 [100] MyD88 [98] TLR2 [96] STAT1 [96] Ehrlichia chaffeensis White-tailed deer*, coyotes, and dogs Unknown Amblyomma*, Ixodes, and Dermacentor…”

“…Thus, NLRs signaling through RIP2 have been speculated to contribute to mounting of the Th1 response to Anaplasma [99]. A separate study by Müller and colleagues has built upon this hypothesis by analyzing the contributions of specific NLRs during infection [98]. The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98].…”

“…A separate study by Müller and colleagues has built upon this hypothesis by analyzing the contributions of specific NLRs during infection [98]. The authors observed significantly increased A. phagocytophilum loads in the blood and lungs of NOD2 −/− C57BL/6 mice throughout the course of infection, but both NOD2 −/− and WT mice eventually cleared the bacterium at similar rates [98]. In experiments using Hoxb8 murine neutrophils, no differences in bacterial load or proinflammatory markers have been observed among infected WT, NOD1 −/− , NOD2 −/− , and NLRP3 −/− cells [98].…”

Pattern Recognition Receptors in Innate Immunity to Obligate Intracellular Bacteria

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Temporal patterns of gene expression in response to inoculation with a virulent Anaplasma phagocytophilum strain in sheep