Immunology/Inflammation
Immunology/Inflammation(免疫及炎症)
The immune and inflammation-related pathway including the Toll-like receptors pathway, the B cell receptor signaling pathway, the T cell receptor signaling pathway, etc.
Toll-like receptors (TLRs) play a central role in host cell recognition and responses to microbial pathogens. TLR4 initially recruits TIRAP and MyD88. MyD88 then recruits IRAKs, TRAF6, and the TAK1 complex, leading to early-stage activation of NF-κB and MAP kinases [1]. TLR4 is endocytosed and delivered to intracellular vesicles and forms a complex with TRAM and TRIF, which then recruits TRAF3 and the protein kinases TBK1 and IKKi. TBK1 and IKKi catalyze the phosphorylation of IRF3, leading to the expression of type I IFN [2].
BCR signaling is initiated through ligation of mIg under conditions that induce phosphorylation of the ITAMs in CD79, leading to the activation of Syk. Once Syk is activated, the BCR signal is transmitted via a series of proteins associated with the adaptor protein B-cell linker (Blnk, SLP-65). Blnk binds CD79a via non-ITAM tyrosines and is phosphorylated by Syk. Phospho-Blnk acts as a scaffold for the assembly of the other components, including Bruton’s tyrosine kinase (Btk), Vav 1, and phospholipase C-gamma 2 (PLCγ2) [3]. Following the assembly of the BCR-signalosome, GRB2 binds and activates the Ras-guanine exchange factor SOS, which in turn activates the small GTPase RAS. The original RAS signal is transmitted and amplified through the mitogen-activated protein kinase (MAPK) pathway, which including the serine/threonine-specific protein kinase RAF followed by MEK and extracellular signal related kinases ERK 1 and 2 [4]. After stimulation of BCR, CD19 is phosphorylated by Lyn. Phosphorylated CD19 activates PI3K by binding to the p85 subunit of PI3K and produce phosphatidylinositol-3,4,5-trisphosphate (PIP3) from PIP2, and PIP3 transmits signals downstream [5].
Central process of T cells responding to specific antigens is the binding of the T-cell receptor (TCR) to specific peptides bound to the major histocompatibility complex which expressed on antigen-presenting cells (APCs). Once TCR connected with its ligand, the ζ-chain–associated protein kinase 70 molecules (Zap-70) are recruited to the TCR-CD3 site and activated, resulting in an initiation of several signaling cascades. Once stimulation, Zap-70 forms complexes with several molecules including SLP-76; and a sequential protein kinase cascade is initiated, consisting of MAP kinase kinase kinase (MAP3K), MAP kinase kinase (MAPKK), and MAP kinase (MAPK) [6]. Two MAPK kinases, MKK4 and MKK7, have been reported to be the primary activators of JNK. MKK3, MKK4, and MKK6 are activators of P38 MAP kinase [7]. MAP kinase pathways are major pathways induced by TCR stimulation, and they play a key role in T-cell responses.
Phosphoinositide 3-kinase (PI3K) binds to the cytosolic domain of CD28, leading to conversion of PIP2 to PIP3, activation of PKB (Akt) and phosphoinositide-dependent kinase 1 (PDK1), and subsequent signaling transduction [8].
References
[1] Kawai T, Akira S. The role of pattern-recognition receptors in innate immunity: update on Toll-like receptors[J]. Nature immunology, 2010, 11(5): 373-384.
[2] Kawai T, Akira S. Toll-like receptors and their crosstalk with other innate receptors in infection and immunity[J]. Immunity, 2011, 34(5): 637-650.
[3] Packard T A, Cambier J C. B lymphocyte antigen receptor signaling: initiation, amplification, and regulation[J]. F1000Prime Rep, 2013, 5(40.10): 12703.
[4] Zhong Y, Byrd J C, Dubovsky J A. The B-cell receptor pathway: a critical component of healthy and malignant immune biology[C]//Seminars in hematology. WB Saunders, 2014, 51(3): 206-218.
[5] Baba Y, Matsumoto M, Kurosaki T. Calcium signaling in B cells: regulation of cytosolic Ca 2+ increase and its sensor molecules, STIM1 and STIM2[J]. Molecular immunology, 2014, 62(2): 339-343.
[6] Adachi K, Davis M M. T-cell receptor ligation induces distinct signaling pathways in naive vs. antigen-experienced T cells[J]. Proceedings of the National Academy of Sciences, 2011, 108(4): 1549-1554.
[7] Rincón M, Flavell R A, Davis R A. The Jnk and P38 MAP kinase signaling pathways in T cell–mediated immune responses[J]. Free Radical Biology and Medicine, 2000, 28(9): 1328-1337.
[8] Bashour K T, Gondarenko A, Chen H, et al. CD28 and CD3 have complementary roles in T-cell traction forces[J]. Proceedings of the National Academy of Sciences, 2014, 111(6): 2241-2246.
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Immunology/Inflammation 相关产品(4245)
- GP10100immunoglobulin light chain variable region fragment [Homo sapiens]
Immunoglobulin light chain fragment
- GP10133immunoglobulin light chain variable region fragment [Homo sapiens]/[Mus musculus]
Immunoglobulin light chain fragment
- GP26363Cor a 8.0101
Recombinant Non-specific Lipid-Transfer Protein Cor a 8 produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 11kDa
- GP26365Cor a 14.0101
Recombinant 2S albumin produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 14kDa
- GP26368Tri a 14.0101
Recombinant Non-Specific Lipid-Transfer Protein Tri a 14 produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 13kDa
| 货号 | 产品名称 | CAS号 | 纯度 | 结构 |
|---|---|---|---|---|
| GP10099 | amyloid A protein fragment [Homo sapiens] | - | - | |
Apolipoproteins related to HDL in plasma | ||||
| GP10100 | immunoglobulin light chain variable region fragment [Homo sapiens] | - | - | |
Immunoglobulin light chain fragment | ||||
| GP10114 | Myelopeptide-2 (MP-2) | - | >98.50% / >98.00% | |
用于恢复人T淋巴细胞的肽 | ||||
| GP10116 | Immunoglobulin M heavy chain (IGHM) fragment [Homo sapiens] | - | - | |
Immunoglobulin M heavy chain | ||||
| GP10124 | Anti-Inflammatory Peptide 1 | 118850-71-8 | - | |
PLA2 inhibitor | ||||
| GP10133 | immunoglobulin light chain variable region fragment [Homo sapiens]/[Mus musculus] | - | - | |
Immunoglobulin light chain fragment | ||||
| GP10135 | MHC class II antigen (45-57) [Homo sapiens] | - | - | |
主要组织相容性复合体 | ||||
| GP10136 | egg white lysozyme (19-36) [Gallus gallus] | - | - | |
Dissolution of cell wall | ||||
| GP10138 | hemagglutinin (332-340) [Influenza A virus] | - | - | |
Partial antigenic glycoprotein | ||||
| GP10146 | ferritin heavy chain fragment [Multiple species] | - | - | |
Ferritin heavy chain fragment | ||||
| GP26024 | LGALS2 Mouse, Active | - | - | |
LGALS2 Mouse Recombinant produced in E | ||||
| GP26025 | LGALS3 Mouse, Active | - | - | |
LGALS3 Mouse Recombinant produced in E | ||||
| GP26363 | Cor a 8.0101 | - | - | |
Recombinant Non-specific Lipid-Transfer Protein Cor a 8 produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 11kDa | ||||
| GP26364 | Cor a 9 | - | - | |
The native protein Corylus Avellana Cor a 9 is purified from hazelnut by protein chemical methods | ||||
| GP26365 | Cor a 14.0101 | - | - | |
Recombinant 2S albumin produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 14kDa | ||||
| GP26366 | MALD3 | - | - | |
Recombinant Non-Specific Lipid-Transfer Protein Mal d 3 produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 12kDa | ||||
| GP26367 | Pen a 1.0101 | - | - | |
Recombinant Tropomyosin Pen a 1 | ||||
| GP26368 | Tri a 14.0101 | - | - | |
Recombinant Non-Specific Lipid-Transfer Protein Tri a 14 produced in SF9 is a glycosylated, polypeptide chain having a calculated molecular mass of 13kDa | ||||
| GC10088 | SC75741 | 913822-46-5 | >98.00% | |
An inhibitor of NF-κB | ||||
| GC12372 | SC-514 | 354812-17-2 | >99.50% | |
Selective inhibitor of IKK2 | ||||
| GC12810 | SR 11302 | 160162-42-5 | >98.00% / >95.00% | |
SR 11302是一种类视黄醇类AP-1选择性转录因子抑制剂,能够阻断AP-1活性,而不激活视黄醇反应元件(RARE)转录。 | ||||
