mortality/aging
• unlike similarly treated wild-type mice, treatment with LPS or pIpC does not induce lethality
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immune system
• B cells exhibit severe attenuation of the prosurvival effects of LPS, pIpC, and CpG
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• following treatment with LPS or pIpC, B cell proliferation is decreased compared to in similarly treated wild-type mice
• CpG- and CSK4-induced B cell proliferation are partially inhibited compared to in similarly treated wild-type mice
• however, B cell proliferation induced by R-837, MALP-2, IgM, CD40, or PGN is normal
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• compared with similarly treated wild-type mice following treatment with LPS or pIpC
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• in LPS, pIpC, or CpG treated bone marrow-derived dendritic cells
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• compared with similarly treated wild-type mice following treatment with LPS, pIpC, or IL1beta
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• compared with similarly treated wild-type mice following treatment with LPS or pIpC
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• in LPS, pIpC, or CpG treated bone marrow-derived dendritic cells
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• unlike similarly treated wild-type mice, treatment with LPS or pIpC leads to attenuated proinflammatory cytokine (TNF, IL6, IL12b, and IFN-beta) production, leads to decreased proliferation of B cells, and fails to induce lethality
• CpG- and CSK4-induced B cell proliferation are partially inhibited compared to in similarly treated wild-type mice
• however, B cell proliferation induced by R-837, MALP-2, IgM, CD40, or PGN is normal
• B cells exhibit severe attenuation of the prosurvival effects of LPS, pIpC, and CpG
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homeostasis/metabolism
• compared with similarly treated wild-type mice following treatment with LPS or pIpC
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• in LPS, pIpC, or CpG treated bone marrow-derived dendritic cells
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• compared with similarly treated wild-type mice following treatment with LPS, pIpC, or IL1beta
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• compared with similarly treated wild-type mice following treatment with LPS or pIpC
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• unlike similarly treated wild-type mice, treatment with LPS or pIpC does not induce lethality
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hematopoietic system
• B cells exhibit severe attenuation of the prosurvival effects of LPS, pIpC, and CpG
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• following treatment with LPS or pIpC, B cell proliferation is decreased compared to in similarly treated wild-type mice
• CpG- and CSK4-induced B cell proliferation are partially inhibited compared to in similarly treated wild-type mice
• however, B cell proliferation induced by R-837, MALP-2, IgM, CD40, or PGN is normal
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cellular
• B cells exhibit severe attenuation of the prosurvival effects of LPS, pIpC, and CpG
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• following treatment with LPS or pIpC, B cell proliferation is decreased compared to in similarly treated wild-type mice
• CpG- and CSK4-induced B cell proliferation are partially inhibited compared to in similarly treated wild-type mice
• however, B cell proliferation induced by R-837, MALP-2, IgM, CD40, or PGN is normal
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