Role of the myeloid differentiation primary response (MYD88) and TIR-domain-containing adapter-inducing interferon-β (TRIF) pathways in dengue

The proto-oncogenes c-jun, junB, junD, and c-fos recently have been shown to encode for transcription factors with a leucine zipper that mediates dimerization to constitute active transcription factors; juns were shown to dimerize with each other and with c-fos, whereas fos was shown to dimerize only with juns. After birth, hematopoietic cells of the myeloid lineage, and some other terminally differentiated cell types, express high levels of c-fos. Still, the role of fos/jun transcription factors in normal myelopoiesis or in leukemogenesis has not been established. Recently, c-jun, junB, and junD were identified as myeloid differentiation primary response genes stably expressed following induction of terminal differentiation of myeloblastic leukemia M1 cells. Intriguingly, c-fos, though induced during normal myelopoiesis, was not induced upon M1 differentiation. To gain further insights into the role of fos/jun in normal myelopoiesis and leukemogenicity, M1fos and M1junB cell lines, which constitutively express c-fos and junB, respectively, were established. It was shown that enforced expression of c-fos, and to a lesser extent junB, in M1 cells results in both an increased propensity to differentiate and a reduction in the aggressiveness of the M1 leukemic phenotype. M1fos cells constitutively expressed immediate-early and late genetic markers of differentiated M1 cells. The in vitro differentiation of normal myeloblasts into mature macrophages and granulocytes, as well as the increased propensity of M1fos leukemic myeloblasts to be induced for terminal differentiation, was dramatically impaired with use of c-fos antisense oligomers in the culture media. Taken together, these observations show that the proto-oncogenes which encode for fos/jun transcription factors play important roles in promoting myeloid differentiation. The ability of the M1 leukemic myeloblasts to be induced for terminal differentiation in the absence of apparent fos expression indicates that there is some redundancy among the fos/jun family of transcription factors in promoting myeloid differentiation; however, juns alone cannot completely compensate for the lack of fos. Thus, genetic lesions affecting fos/jun expression may play a role in the development of "preleukemic" myelodysplastic syndromes and their further progression to leukemias.

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Central role of the TIR-domain-containing adaptor-inducing interferon-β (TRIF) adaptor protein in murine sterile liver injury

Hepatology ◽

10.1002/hep.29078 ◽

2017 ◽

Vol 65 (4) ◽

pp. 1336-1351 ◽

Cited By ~ 6

Author(s):

Katherine J. Brempelis ◽

Sebastian Y. Yuen ◽

Nicole Schwarz ◽

Isaac Mohar ◽

Ian N. Crispe

Keyword(s):

Liver Injury ◽

Adaptor Protein ◽

Interferon Β ◽

Tir Domain

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Possible Involvement of MyD88 in Regulating Stress Response in Mice

Frontiers in Neuroscience ◽

10.3389/fnins.2021.621446 ◽

2021 ◽

Vol 15 ◽

Author(s):

Toru Hosoi ◽

Yosuke Yamawaki ◽

Hitomi Kimura ◽

Shoko Honda ◽

Koichiro Ozawa

Keyword(s):

Stress Response ◽

Immobilization Stress ◽

Forced Swim Test ◽

Primary Response ◽

Innate Immune ◽

Myeloid Differentiation ◽

Adapter Protein ◽

Immobility Time ◽

Deficient Mice

Myeloid differentiation primary response 88 (MyD88) is an adapter protein of the toll-like receptor (TLR) family that regulates innate immune function. Here, we identified a novel role of MyD88 in regulating stress response. MyD88 deficiency decreased immobility time in the forced swim test without affecting locomotor activity in mice. Immobilization stress-induced production of serum corticosterone was also completely inhibited by MyD88 deficiency. Stress induced decrease in glucocorticoid receptor in the hippocampus. On the other hand, stress exposure in MyD88 deficient mice did not cause decrease in its level in the hippocampus. Furthermore, immobilization stress-induced reduction of brain-derived neurotrophic factor (BDNF) levels in the hippocampus was ameliorated by MyD88 deficiency. These results suggest that MyD88 deficiency attenuates depression-like behavior by regulating corticosterone and BDNF levels. Overall, these results indicate the key role of MyD88 in regulating stress response in mice.

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Biologically active 1,25-dihydroxyvitamin D3 protects against experimental sepsis by negatively regulating the Toll-like receptor 4/myeloid differentiation primary response gene 88/Toll-IL-1 resistance-domain-containing adapter-inducing interferon-β signaling pathway

International Journal of Molecular Medicine ◽

10.3892/ijmm.2019.4266 ◽

2019 ◽

Author(s):

Ge Zheng ◽

Na Wen ◽

Minli Pan ◽

Yumao Huang ◽

Zhishu Li

Keyword(s):

Primary Response ◽

Biologically Active ◽

Myeloid Differentiation ◽

Experimental Sepsis ◽

Toll Like Receptor ◽

Interferon Β ◽

Toll Like Receptor 4 ◽

Response Gene ◽

Dihydroxyvitamin D3 ◽

Primary Response Gene

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Role of Toll-like receptor/MYD88 signaling in neurodegenerative diseases

Reviews in the Neurosciences ◽

10.1515/revneuro-2014-0067 ◽

2015 ◽

Vol 26 (4) ◽

Cited By ~ 21

Author(s):

Wang Xiang ◽

Zhang-Yong Chao ◽

Du-Yi Feng

Keyword(s):

Intracellular Signaling ◽

Adaptor Proteins ◽

Primary Response ◽

Innate Immune ◽

Myeloid Differentiation ◽

Toll Like Receptor ◽

Intracellular Signaling Pathways ◽

Primary Response Gene ◽

Myd88 Signaling

AbstractToll-like receptors (TLRs) are important innate immune proteins, and the activation of the TLRs results in the activation of intracellular signaling pathways, leading to the expression of proinflammatory cytokines that are essential to the identification and clearance of invading pathogens. TLR signaling occurs through adaptor proteins, most commonly myeloid differentiation primary response gene 88 (

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TIR-Domain-Containing Adaptor-Inducing Interferon-β (TRIF) Mediates Antibacterial Defense during Gram-Negative Pneumonia by Inducing Interferon-γ

Journal of Innate Immunity ◽

10.1159/000430913 ◽

2015 ◽

Vol 7 (6) ◽

pp. 637-646 ◽

Cited By ~ 7

Author(s):

Miriam H.P. van Lieshout ◽

Sandrine Florquin ◽

Cornelis vanʼt Veer ◽

Alex F. de Vos ◽

Tom van der Poll

Keyword(s):

Interferon Γ ◽

Primary Response ◽

Mutant Mice ◽

Klebsiella Pneumonia ◽

Hepatocellular Injury ◽

Interferon Β ◽

Gram Negative ◽

Tir Domain ◽

Ifn Γ

Klebsiella pneumoniae is an important cause of Gram-negative pneumonia and sepsis. Mice deficient for TIR-domain-containing adaptor-inducing interferon-β (TRIF) demonstrate enhanced bacterial growth and dissemination during Klebsiella pneumonia. We show here that the impaired antibacterial defense of TRIF mutant mice is associated with absent interferon (IFN)-γ production in the lungs. IFN-γ production by splenocytes in response to K. pneumoniae in vitro was critically dependent on Toll-like receptor 4 (TLR4), the common TLR adaptor myeloid differentiation primary response gene (MyD88) and TRIF. Reconstitution of TRIF mutant mice with recombinant IFN-γ via the airways reduced bacterial loads in lungs and distant body sites to levels measured in wild-type mice, and partially restored pulmonary cytokine levels. The IFN-γ-induced, improved, enhanced antibacterial response in TRIF mutant mice occurred at the expense of increased hepatocellular injury. These data indicate that TRIF mediates antibacterial defense during Gram-negative pneumonia, at least in part, by inducing IFN-γ at the primary site of infection.

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TLRs in COVID-19: How they drive immunopathology and the rationale for modulation

Innate Immunity ◽

10.1177/17534259211051364 ◽

2021 ◽

pp. 175342592110513

Author(s):

F. Linzee Mabrey ◽

Eric D Morrell ◽

Mark M Wurfel

Keyword(s):

Innate Immune System ◽

Primary Response ◽

Viral Clearance ◽

Innate Immune ◽

Myeloid Differentiation ◽

Tir Domain ◽

Critical Elements ◽

Severity Of Disease ◽

Viral Illness ◽

Myd88 Pathway

COVID-19 is both a viral illness and a disease of immunopathology. Proximal events within the innate immune system drive the balance between deleterious inflammation and viral clearance. We hypothesize that a divergence between the generation of excessive inflammation through over activation of the TLR associated myeloid differentiation primary response (MyD88) pathway relative to the TIR-domain-containing adaptor-inducing IFN-β (TRIF) pathway plays a key role in COVID-19 severity. Both viral elements and damage associated host molecules act as TLR ligands in this process. In this review, we detail the mechanism for this imbalance in COVID-19 based on available evidence, and we discuss how modulation of critical elements may be important in reducing severity of disease.

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Proto-oncogenes of the fos/jun family of transcription factors are positive regulators of myeloid differentiation

Molecular and Cellular Biology ◽

10.1128/mcb.13.2.841-851.1993 ◽

1993 ◽

Vol 13 (2) ◽

pp. 841-851

Author(s):

K A Lord ◽

A Abdollahi ◽

B Hoffman-Liebermann ◽

D A Liebermann

Keyword(s):

Transcription Factors ◽

Leucine Zipper ◽

Culture Media ◽

Terminal Differentiation ◽

Cell Types ◽

Primary Response ◽

Myeloid Differentiation ◽

Active Transcription

The proto-oncogenes c-jun, junB, junD, and c-fos recently have been shown to encode for transcription factors with a leucine zipper that mediates dimerization to constitute active transcription factors; juns were shown to dimerize with each other and with c-fos, whereas fos was shown to dimerize only with juns. After birth, hematopoietic cells of the myeloid lineage, and some other terminally differentiated cell types, express high levels of c-fos. Still, the role of fos/jun transcription factors in normal myelopoiesis or in leukemogenesis has not been established. Recently, c-jun, junB, and junD were identified as myeloid differentiation primary response genes stably expressed following induction of terminal differentiation of myeloblastic leukemia M1 cells. Intriguingly, c-fos, though induced during normal myelopoiesis, was not induced upon M1 differentiation. To gain further insights into the role of fos/jun in normal myelopoiesis and leukemogenicity, M1fos and M1junB cell lines, which constitutively express c-fos and junB, respectively, were established. It was shown that enforced expression of c-fos, and to a lesser extent junB, in M1 cells results in both an increased propensity to differentiate and a reduction in the aggressiveness of the M1 leukemic phenotype. M1fos cells constitutively expressed immediate-early and late genetic markers of differentiated M1 cells. The in vitro differentiation of normal myeloblasts into mature macrophages and granulocytes, as well as the increased propensity of M1fos leukemic myeloblasts to be induced for terminal differentiation, was dramatically impaired with use of c-fos antisense oligomers in the culture media. Taken together, these observations show that the proto-oncogenes which encode for fos/jun transcription factors play important roles in promoting myeloid differentiation. The ability of the M1 leukemic myeloblasts to be induced for terminal differentiation in the absence of apparent fos expression indicates that there is some redundancy among the fos/jun family of transcription factors in promoting myeloid differentiation; however, juns alone cannot completely compensate for the lack of fos. Thus, genetic lesions affecting fos/jun expression may play a role in the development of "preleukemic" myelodysplastic syndromes and their further progression to leukemias.

Download Full-text