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Antibodies from IMGENEX: Dendritic Cells

 

Dendritic Cells
 

The first dendritic cells (DCs) to be discovered, in 1868 were the Langerhans cells of human epidermis. It took however until the 1970s to demonstrate that these cells belong to the immune system. Simultaneously, in 1973, the pioneering work of Steinman and Cohn permitted the identification of dendritic cells in lymphoid tissue and their functional relationship with Langerhans cells. Realization of the extraordinary capacity of DCs for antigen -presentation set the stage for an exponentially rising interest in their biology. Major advances in the early 1990s subsequently led to the ability to generate dendritic cells in vitro from myeloid hematopoietic progenitors or from monocytes, and greatly facilitated their study. The initial unified model of dendritic cell's life history held that immature DCs patrol peripheral tissues and upon encounter with microbial products or other danger signals undergo maturation as they migrate to lymphoid tissue where they present antigen and activate naive T cells (16).

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While most elements of this model still hold true, in particular the unique capacity of dendritic cells to initiate adaptive immunity, many different and contrasting facets of DCs have since been discovered (17). One aspect that has become clearly appreciated is the great diversity of DC Subtypes with considerable functional differences. Part of this heterogeneity is intrinsic (eg “conventional” versus plasmacytoid DCs), but a high degree of plasticity is also characteristic of the dendritic cell system. For instance, DCs can be instructed by the nature of the early signals they receive, with greatly divergent consequences on the immune response. Thus, in addition to their classic function to drive strong Th1-type adaptive responses, dendritic cells can be polarized by microbial products towards a Th2- type response, or towards peripheral immune tolerance via the induction of regulatory T cells (18, 19).


Today, dendritic cells are thus positioned as the master regulators of immunity. Pharmacological intervention to exploit the full range of dendritic cell regulatory potential will undoubtedly lead to a variety of therapeutic applications to either boost, suppress or repolarize the immune system (20, 21). Another recently recognized important function of dendritic cells is to link the innate and adaptive immune response. This is illustrated by antiviral responses of plasmacytoid DCs (22), and by crosstalk between DCs and NK cells (23). A major breakthrough in dendritic cells  biology has been the recent unraveling of the mechanisms responsible for their

     Dendritic Cells: regulators of the immune response

regulatory functions, an advance made possible by the molecular cloning of genes expressed by DCs. Thus, it was realized that dendritic cells are remarkably equipped with Pattern -Recognition Receptors (PRRs), the innate sensors that recognize conserved molecular patterns on microbes and self- tissue. Outstanding PRRs are the C- type Lectin Receptors and the Toll - Like Receptors. The key role played by Chemokines and their receptors in the migration patterns of dendritic cells is now well established. Finally, an array of Cytokines and corresponding receptors are known to be responsible for the crosstalk between DCs and a host of other cell types that will determine the net outcome of the immune response. Collectively, this rapidly-evolving knowledge allows for drug-discovery programs to design pharmacological compounds to agonize or antagonize dendritic cell molecules in a number of clinical settings.

 

  1. DC Subtypes
  2. C-type Lectin Receptors (CLRs)
  3. Toll-Like Receptors (TLRs)
  4. Dendritic Cell Migration
  5. Cytokines

  6. References

 

 
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Found 437 results, displaying 1 to 50 | Show all
 
Cat.No Description Format Species Clone Application Publications
IMG-6725A

CLEC9A

Purified Chp, H, Or, RH IMG14N8D7 IHC (p)
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IMG-6801A AIMP1 Purified Ca, Cha, C, D, G, Hs, H, Mr, M, Mk, O, Or, P, Pi, RH, W N/A
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IMG-6802A AIMP1 Purified Chp, Cha, C, Ele, G, Hs, H, Mr, M, Or, Pi, R, RH, W N/A WB
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IMG-6800A AIMP2 Purified Chp, H, Mq, Or, RH, W N/A WB
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DDX0011 ASGPR / CD301 Purified H 121A5.01 IHC, IP
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DDX0011A488 ASGPR / CD301 Alexa FluorŽ 488 H 121A5.01 Flow (CS), Flow (I), IF/ICC
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DDX0011A546 ASGPR / CD301 Alexa FluorŽ 546 H 121A5.01 IF/ICC
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DDX0011B ASGPR / CD301 Biotin H 121A5.01 IP
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DDX0030 Basophil Purified H 212H6.16 Flow (CS), IHC (frozen)
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DDX0030A488 Basophil Alexa FluorŽ 488 H 212H6.16 Flow (CS), IF/ICC
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DDX0030A546 Basophil Alexa FluorŽ 546 H 212H6.16 IF/ICC
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DDX0030A647 Basophil Alexa FluorŽ 647 H 212H6.16 Flow (CS), IF/ICC
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DDX0030A647-50 Basophil Alexa FluorŽ 647 H 212H6.16 Flow (CS), IF/ICC
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DDX0030A546-50 Basophil Alexa FluorŽ 546 H 212H6.16 IF/ICC
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DDX0070 Bet V1 Purified P H.G27E9B1 ELISA
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DDX0071 Bet V1 Purified P H.G26F6B2.06 RIPA
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DDX0072 Bet V1 Purified P H.G11A9F3.03 ELISA, RIPA
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DDX0073 Bet V1 Purified P H.G28C10.01 ELISA, RIPA
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DDX0074 Bet V1 Purified P H.G5F2A4.09 ELISA
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DDX0075 Bet V1 Purified P H.G3A3C2.04 ELISA, RIPA
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DDX0076 Bet V1 Purified P H.G17E7A1 ELISA
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IMG-6731A BST2 Purified A, Chp, H, Mq, M, R N/A IHC (p), WB
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IMG-6850A BST2 Purified H N/A WB
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DDX0450 Bullous Pemphigoid Purified H H5E.Hy.4B IF/ICC, IHC (frozen), WB
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IMG-6845A CADM1 Purified Cha, D, Hs, H, M, Pi, P, Ra, R IMG41N3D3 WB
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DDX0520 Carboxypeptidase M Purified H M27 Flow, IHC (frozen), IP
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DDX0700 CD127/IL-7R Purified H R34-34 FA (N), Flow (CS), IP
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DDX0700A488 CD127/IL-7R Alexa FluorŽ 488 H R34-34 Flow (CS)
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DDX0700A546 CD127/IL-7R Alexa FluorŽ 546 H R34-34 Flow (CS)
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DDX0700A647 CD127/IL-7R Alexa FluorŽ 647 H R34-34 Flow (CS)
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DDX0100 CD14 Purified H MOP9.25 Flow, IHC
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IMG-6541A CD150 Purified H IPO-3 Flow (CS), IF/ICC, IHC (frozen), IP
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DDX0080 CD1a Purified H 214A9.01 Flow (CS), IHC (frozen)
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DDX0081 CD1a Purified H 201B5.08 Flow (CS), IHC (frozen), WB
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DDX0080A488 CD1a Alexa FluorŽ 488 H 214A9.01 Flow (CS), IF/ICC
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DDX0080A546 CD1a Alexa FluorŽ 546 H 214A9.01 IF/ICC
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DDX0080B CD1a Biotin H 214A9.01 Flow (CS), IHC (frozen)
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DDX0080A647 CD1a Alexa FluorŽ 647 H 214A9.01 IHC (frozen)
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DDX0081A488 CD1a Alexa FluorŽ 488 H 201B5.08 Flow (CS), IF/ICC
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DDX0081A546 CD1a Alexa FluorŽ 546 H 201B5.08 Flow (CS), IF/ICC
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DDX0081A647 CD1a Alexa FluorŽ 647 H 201B5.08 Flow (CS), IF/ICC
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DDX0080A488-50 CD1a Alexa FluorŽ 488 H 214A9.01 Flow (CS), IF/ICC
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DDX0080A546-50 CD1a Alexa FluorŽ 546 H 214A9.01 IF/ICC
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DDX0080B-50 CD1a Biotin H 214A9.01 Flow (CS), IHC (frozen)
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DDX0110 CD20 Purified H mAb75 Flow
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DDX0020 CD205 (DEC-205) Purified M NLDC-145 Flow (CS), IHC (frozen)
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DDX0020A488 CD205 (DEC-205) Alexa FluorŽ 488 M NLDC-145 Flow (CS), IHC (frozen)
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DDX0020B CD205 (DEC-205) Biotin M NLDC-145 Flow (CS), IHC (frozen), IHC (p)
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DDX0381 CD206 Purified H 118F2.02 IP, WB
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DDX0361APC CD207 / Langerin APC H, M, R 310F7.02/HD26 Flow (I), IF/ICC
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