The process of categorizing the antigenic molecules and epitopes associated with human white cells, via the collaborative study of monoclonal antibodies, dates back to the early 1980s, when the first HLDA (Human Leucocyte Differentiation Antigen) Workshop was held in Paris. This initial meeting listed only 15 molecular entities, but it created an internationally agreed basis for the nomenclature of leukocyte molecules (the CD scheme) and also provided a forum for reporting studies on their function and practical relevance. A further six HLDA meetings have been held since the first Paris meeting. The most recent of these (“HLDA7”) took place in 2000 in Harrogate, United Kingdom, and the proceedings of the meeting (Leucocyte Typing VII1) have recently been published.
The aims and approaches of HLDA7. It was apparent at the previous meeting, HLDA6, held in Kobe, Japan, in 1996, that the technique of detecting molecular entities by screening coded panels of monoclonal antibodies against human cells was becoming obsolescent. Antibodies to the most immunogenic molecules had already been produced, and fewer laboratories than in the early days were prepared to devote resources to raising new antibodies, since the probability of finding novel reagents becomes ever less likely. In consequence many antibodies in the sixth workshop were reagents (submitted by laboratories that were not equipped to characterize them) that proved to be of known specificity.
With these considerations in mind, HLDA7 adopted a different approach. Instead of screening poorly characterized antibodies, reagents were selected (and actively solicited) for which at least some molecular data were already available. A substantial number of monoclonal antibodies reactive with leukocyte-associated molecules exist that do not meet the traditional criterion for establishing a new CD specificity (ie, the existence of at least 2 independent antibodies of the same specificity). This rule dates from the first HLDA workshop 2 decades ago; since that time biochemical and molecular biological techniques for characterizing the targets of new antibodies have come to be widely used. Consequently, it is now considered appropriate to establish a CD designation for a molecule if its gene has been cloned and at least one specific monoclonal antibody has been studied in the workshop.
Four new sections were introduced in HLDA7 to add to the traditional list from past meetings: Dendritic Cells, Stem/Progenitor Cells, Erythroid Cells, and Carbohydrate Structures. Although it has been recognized for many years that monoclonal antibodies reactive with human leukocytes can be specific for carbohydrate epitopes (eg, the carbohydrate CD category CD15 was identified at the first HLDA workshop), they had not received specific attention at any workshop. The inclusion of erythroid molecules, although it may seem out of place in a leukocyte workshop, was justified by the number of molecules shared between white and red cells (eg, cytokine receptors) that hint at unexplored functions of red cells.
The yield of new CD specificities in HLDA7. This more active approach to the identification of new CD specificities represented a break with tradition, but the results justified the new approach since a total of well over 80 new entities were added to the list of CD specificities. This compares favorably with previous workshops (an average of fewer than 30 CD specificities per workshop), and it also largely avoided the laborious screening in multiple laboratories of antibodies that often prove to be directed against known CD molecules.
Tables 1 and2 list the new specificities established at HLDA7. Full details can be found in Leucocyte Typing VII,1 and molecular, functional, and other data can be found for many of these new specificities on the PROW site.2
New CD designations
| Designation . | Name . | Section . | Locus link . |
|---|---|---|---|
| CD15u | Sulphated CD15 | Carbohydrate structures | NA |
| CD60a | GD3 | Carbohydrate structures | NA |
| CD60b | 9-O-acetyl-GD3 | Carbohydrate structures | NA |
| CD60c | 7-O-acetyl-GD3 | Carbohydrate structures | NA |
| CD75 | Lactosamines | Carbohydrate structures | NA |
| CD75s | Alpha-2,6-sialylated lactosamines (formerly CDw75 and CDw76) | Carbohydrate structures | NA |
| CD85 | ILT/LIR family (see Table 2) | Dendritic cells | NA |
| CD110 | MPL, TPO R | Platelets | 4352 |
| CD111 | PRR1/Nectin1 | Myeloid cells | 5818 |
| CD112 | PRR2 | Myeloid cells | 5819 |
| CD133 | AC133 | Stem/progenitor cells | 8842 |
| CD156b | TACE/ADAM17 | Adhesion structures | 6868 |
| CD158 | KIR family (see Table 2) | NK cells | NA |
| CD159a | NKG2A | NK cells | 3821 |
| CD160 | BY55 | T cells | 11126 |
| CD162R | PEN5 | NK cells | 6404 |
| CD167a | Discoidin domain R (DDR1) | Adhesion structures | 780 |
| CD168 | RHAMM | Adhesion structures | 3161 |
| CD169 | Sialoadhesin | Adhesion structures | 6614 |
| CD170 | Siglec-5 | Adhesion structures | 8778 |
| CD171 | L1 | Adhesion structures | 3897 |
| CD172a | SIRP alpha | Adhesion structures | 8194 |
| CD173 | Blood group H type 2 | Carbohydrate structures | NA |
| CD174 | Lewis y | Carbohydrate structures | NA |
| CD175 | Tn | Carbohydrate structures | NA |
| CD175s | Sialyl-Tn | Carbohydrate structures | NA |
| CD176 | TF | Carbohydrate structures | NA |
| CD177 | NB1 | Myeloid cells | NA |
| CD178 | Fas ligand | Cytokine/chemokine receptors | 356 |
| CD179a | Vpre-B | B cells | 7441 |
| CD179b | Lambda 5 | B cells | 3543 |
| CD180 | RP105 | B cells | 4064 |
| CD183 | CXCR3 | Cytokine/chemokine receptors | 2833 |
| CD184 | CXCR4 | Cytokine/chemokine receptors | 7852 |
| CD195 | CCR5 | Cytokine/chemokine receptors | 1234 |
| CDw197 | CCR7 | Cytokine/chemokine receptors | 1236 |
| CD200 | OX2 | Nonlineage molecules | 4345 |
| CD201 | EPC R | Endothelial cells | 10544 |
| CD202b | Tie2 (Tek) | Endothelial cells | 7010 |
| CD203c | NPP3/PDNP3 | Myeloid cells | 5169 |
| CD204 | Macrophage scavenger R | Myeloid cells | 4481 |
| CD205 | DEC205 | Dendritic cells | 4065 |
| CD206 | Macrophage mannose R | Dendritic cells | 4360 |
| CD207 | Langerin | Dendritic cells | 50489 |
| CD208 | DC-LAMP | Dendritic cells | NA |
| CD209 | DC-SIGN | Dendritic cells | 30385 |
| CDw210 | IL-10 R | Cytokine/chemokine receptors | 3587; 3588 |
| CD212 | IL-12 R | Cytokine/chemokine receptors | 3594 |
| CD213a1 | IL-13 R alpha 1 | Cytokine/chemokine receptors | 3597 |
| CD213a2 | IL-13 R alpha 2 | Cytokine/chemokine receptors | 3598 |
| CDw217 | IL-17 R | Cytokine/chemokine receptors | 23765 |
| CD220 | Insulin R | Nonlineage molecules | 3643 |
| CD221 | IGF1 R | Nonlineage molecules | 3480 |
| CD222 | Mannose-6-phosphate/IGF2 R | Nonlineage molecules | 3482 |
| CD223 | LAG-3 | Nonlineage molecules | 3902 |
| CD224 | Gamma-glutamyl transferase | Nonlineage molecules | 2678 |
| CD225 | Leu13 | Nonlineage molecules | 8519 |
| CD226 | DNAM-1 (PTA1) | T cells | 10666 |
| CD227 | MUC.1 | Nonlineage molecules | 4582 |
| CD228 | Melanotransferrin | Nonlineage molecules | 4241 |
| CD229 | Ly9 | Nonlineage molecules | 4063 |
| CD230 | Prion protein | Nonlineage molecules | 5621 |
| CD231 | TALLA-1/A15 | Nonlineage molecules | 7102 |
| CD232 | VESP R | Nonlineage molecules | 10154 |
| CD233 | Band 3 | Erythroid cells | 6521 |
| CD234 | Fy-glycoprotein (DARC) | Erythroid cells | 2532 |
| CD235a | Glycophorin A | Erythroid cells | 2993 |
| CD235b | Glycophorin B | Erythroid cells | 2994 |
| CD235ab | Glycophorin A/B crossreactive mabs | Erythroid cells | NA |
| CD236 | Glycophorin C/D | Erythroid cells | NA |
| CD236R | Glycophorin C | Erythroid cells | 2995 |
| CD238 | Kell | Erythroid cells | 3792 |
| CD239 | B-CAM | Erythroid cells | 4059 |
| CD240CE | Rh30CE | Erythroid cells | 6006 |
| CD240D | Rh30D | Erythroid cells | 6007 |
| CD240DCE | Rh30D/CE crossreactive mabs | Erythroid cells | NA |
| CD241 | RhAg | Erythroid cells | 6005 |
| CD242 | ICAM-4 | Erythroid cells | 3386 |
| CD243 | MDR-1 | Stem/progenitor cells | NA |
| CD244 | 2B4 | NK cells | 51744 |
| CD245 | p220/240 | T cells | NA |
| CD246 | Anaplastic lymphoma kinase | T cells | 238 |
| CD247 | Zeta chain | T cells | 919 |
| Designation . | Name . | Section . | Locus link . |
|---|---|---|---|
| CD15u | Sulphated CD15 | Carbohydrate structures | NA |
| CD60a | GD3 | Carbohydrate structures | NA |
| CD60b | 9-O-acetyl-GD3 | Carbohydrate structures | NA |
| CD60c | 7-O-acetyl-GD3 | Carbohydrate structures | NA |
| CD75 | Lactosamines | Carbohydrate structures | NA |
| CD75s | Alpha-2,6-sialylated lactosamines (formerly CDw75 and CDw76) | Carbohydrate structures | NA |
| CD85 | ILT/LIR family (see Table 2) | Dendritic cells | NA |
| CD110 | MPL, TPO R | Platelets | 4352 |
| CD111 | PRR1/Nectin1 | Myeloid cells | 5818 |
| CD112 | PRR2 | Myeloid cells | 5819 |
| CD133 | AC133 | Stem/progenitor cells | 8842 |
| CD156b | TACE/ADAM17 | Adhesion structures | 6868 |
| CD158 | KIR family (see Table 2) | NK cells | NA |
| CD159a | NKG2A | NK cells | 3821 |
| CD160 | BY55 | T cells | 11126 |
| CD162R | PEN5 | NK cells | 6404 |
| CD167a | Discoidin domain R (DDR1) | Adhesion structures | 780 |
| CD168 | RHAMM | Adhesion structures | 3161 |
| CD169 | Sialoadhesin | Adhesion structures | 6614 |
| CD170 | Siglec-5 | Adhesion structures | 8778 |
| CD171 | L1 | Adhesion structures | 3897 |
| CD172a | SIRP alpha | Adhesion structures | 8194 |
| CD173 | Blood group H type 2 | Carbohydrate structures | NA |
| CD174 | Lewis y | Carbohydrate structures | NA |
| CD175 | Tn | Carbohydrate structures | NA |
| CD175s | Sialyl-Tn | Carbohydrate structures | NA |
| CD176 | TF | Carbohydrate structures | NA |
| CD177 | NB1 | Myeloid cells | NA |
| CD178 | Fas ligand | Cytokine/chemokine receptors | 356 |
| CD179a | Vpre-B | B cells | 7441 |
| CD179b | Lambda 5 | B cells | 3543 |
| CD180 | RP105 | B cells | 4064 |
| CD183 | CXCR3 | Cytokine/chemokine receptors | 2833 |
| CD184 | CXCR4 | Cytokine/chemokine receptors | 7852 |
| CD195 | CCR5 | Cytokine/chemokine receptors | 1234 |
| CDw197 | CCR7 | Cytokine/chemokine receptors | 1236 |
| CD200 | OX2 | Nonlineage molecules | 4345 |
| CD201 | EPC R | Endothelial cells | 10544 |
| CD202b | Tie2 (Tek) | Endothelial cells | 7010 |
| CD203c | NPP3/PDNP3 | Myeloid cells | 5169 |
| CD204 | Macrophage scavenger R | Myeloid cells | 4481 |
| CD205 | DEC205 | Dendritic cells | 4065 |
| CD206 | Macrophage mannose R | Dendritic cells | 4360 |
| CD207 | Langerin | Dendritic cells | 50489 |
| CD208 | DC-LAMP | Dendritic cells | NA |
| CD209 | DC-SIGN | Dendritic cells | 30385 |
| CDw210 | IL-10 R | Cytokine/chemokine receptors | 3587; 3588 |
| CD212 | IL-12 R | Cytokine/chemokine receptors | 3594 |
| CD213a1 | IL-13 R alpha 1 | Cytokine/chemokine receptors | 3597 |
| CD213a2 | IL-13 R alpha 2 | Cytokine/chemokine receptors | 3598 |
| CDw217 | IL-17 R | Cytokine/chemokine receptors | 23765 |
| CD220 | Insulin R | Nonlineage molecules | 3643 |
| CD221 | IGF1 R | Nonlineage molecules | 3480 |
| CD222 | Mannose-6-phosphate/IGF2 R | Nonlineage molecules | 3482 |
| CD223 | LAG-3 | Nonlineage molecules | 3902 |
| CD224 | Gamma-glutamyl transferase | Nonlineage molecules | 2678 |
| CD225 | Leu13 | Nonlineage molecules | 8519 |
| CD226 | DNAM-1 (PTA1) | T cells | 10666 |
| CD227 | MUC.1 | Nonlineage molecules | 4582 |
| CD228 | Melanotransferrin | Nonlineage molecules | 4241 |
| CD229 | Ly9 | Nonlineage molecules | 4063 |
| CD230 | Prion protein | Nonlineage molecules | 5621 |
| CD231 | TALLA-1/A15 | Nonlineage molecules | 7102 |
| CD232 | VESP R | Nonlineage molecules | 10154 |
| CD233 | Band 3 | Erythroid cells | 6521 |
| CD234 | Fy-glycoprotein (DARC) | Erythroid cells | 2532 |
| CD235a | Glycophorin A | Erythroid cells | 2993 |
| CD235b | Glycophorin B | Erythroid cells | 2994 |
| CD235ab | Glycophorin A/B crossreactive mabs | Erythroid cells | NA |
| CD236 | Glycophorin C/D | Erythroid cells | NA |
| CD236R | Glycophorin C | Erythroid cells | 2995 |
| CD238 | Kell | Erythroid cells | 3792 |
| CD239 | B-CAM | Erythroid cells | 4059 |
| CD240CE | Rh30CE | Erythroid cells | 6006 |
| CD240D | Rh30D | Erythroid cells | 6007 |
| CD240DCE | Rh30D/CE crossreactive mabs | Erythroid cells | NA |
| CD241 | RhAg | Erythroid cells | 6005 |
| CD242 | ICAM-4 | Erythroid cells | 3386 |
| CD243 | MDR-1 | Stem/progenitor cells | NA |
| CD244 | 2B4 | NK cells | 51744 |
| CD245 | p220/240 | T cells | NA |
| CD246 | Anaplastic lymphoma kinase | T cells | 238 |
| CD247 | Zeta chain | T cells | 919 |
New CD nomenclature for ILT/LIR and KIR molecules
| Designation . | Name . |
|---|---|
| The ILT/LIR family | |
| CD85a | ILT5/LIR3 |
| CD85b | ILT8 |
| CD85c | LIR8 |
| CD85d | ILT4/LIR2, MIR10 |
| CD85e | ILT6/LIR4 |
| CD85f | ILT11 |
| CD85g | ILT7 |
| CD85h | ILT1/LIR7 |
| CD85i | LIR6 |
| CD85j | ILT2/LIR1, MIR7 |
| CD85k | ILT3/LIR5 |
| CD85l | ILT9 |
| CD85m | ILT10 |
| The KIR family | |
| CD158z | KIR3DL7/KIRC1 |
| CD158b1 and CD158b2 | KIR2DL2/p58.2 and KIR2DL3/p58.3 |
| CD158a | KIR2DL1/p58.1 |
| CD158c | KIR2DS6/KIRX |
| CD158d | KIR2DL4 |
| CD158e1 and CD158e2 | KIR3DL1/p70 and KIR3DS1/p70 |
| CD158f | KIR2DL5 |
| CD158g | KIR2DS5 |
| CD158h | KIR2DS1/p50.1 |
| CD158i | KIR2DS4/p50.3 |
| CD158j | KIR2DS2/p50.2 |
| CD158k | KIR3DL2/p140 |
| Designation . | Name . |
|---|---|
| The ILT/LIR family | |
| CD85a | ILT5/LIR3 |
| CD85b | ILT8 |
| CD85c | LIR8 |
| CD85d | ILT4/LIR2, MIR10 |
| CD85e | ILT6/LIR4 |
| CD85f | ILT11 |
| CD85g | ILT7 |
| CD85h | ILT1/LIR7 |
| CD85i | LIR6 |
| CD85j | ILT2/LIR1, MIR7 |
| CD85k | ILT3/LIR5 |
| CD85l | ILT9 |
| CD85m | ILT10 |
| The KIR family | |
| CD158z | KIR3DL7/KIRC1 |
| CD158b1 and CD158b2 | KIR2DL2/p58.2 and KIR2DL3/p58.3 |
| CD158a | KIR2DL1/p58.1 |
| CD158c | KIR2DS6/KIRX |
| CD158d | KIR2DL4 |
| CD158e1 and CD158e2 | KIR3DL1/p70 and KIR3DS1/p70 |
| CD158f | KIR2DL5 |
| CD158g | KIR2DS5 |
| CD158h | KIR2DS1/p50.1 |
| CD158i | KIR2DS4/p50.3 |
| CD158j | KIR2DS2/p50.2 |
| CD158k | KIR3DL2/p140 |
For further details of this classification, based on the position of the genes on chromosome 19q;13.4 from centromeric to telomeric loci, see André et al.3
The eighth workshop. Plans are well advanced for the eighth workshop, to be organized in Adelaide, Australia, in 2004 under the aegis of Professor H. Zola (see http://www.hlda8.org). It is sometimes assumed that the catalogue of surface molecules associated with human hemopoietic cells is now essentially complete, but there is abundant evidence in the literature for novel surface molecules that would merit study at HLDA8, and that could provide the basis for new CD designations. Table 3 comprises both a list of potential new molecules reported following the production of monoclonal antibodies and also a longer list of surface molecules identified via gene cloning, for which in most instances, no antibodies are available. Specific and well-characterized reagents, whether monoclonal or polyclonal, are needed not only for detecting these new “virtual” molecules but also for defining functional domains, for characterizing 3-dimensional protein structure, and for analyzing protein-protein interactions. It may be added that cloning of gene sequences often reveals multiple members of new or existing molecular families (eg, the Toll-like receptors) and may identify surface receptors that bind more than one ligand or vice versa (eg, the TALL-1 and APRIL ligands for TACI and BCMA). Furthermore, a number of leukocyte-associated markers have been cloned from mice and other species, and almost all will have human homologues. HLDA8 will provide a forum for a range of antibody-based studies relating to this accumulating corpus of genomic and proteomic data. As in HLDA7, in which 4 new sections were added, it may be possible to include new cell types in HLDA8. For example, many neuronal cells express surface proteins found on leukocytes and vice versa (eg, CD56, CD100, CD168, CD171). Furthermore, the guidance cues used by neuronal cells share similarities to those involved in leukocyte extravasation, and the expression of these molecules in common may reflect shared biological processes. It may also be noted that other molecules such as the mucins, thought to be primarily associated with epithelial cells, are now being described on leukocytes.
Examples of possible future CD specificities
| Molecule . | Molecule size . | Cell types . | Comments . | Reference(s) . |
|---|---|---|---|---|
| Identified following antibody production | ||||
| AM-3K antigen | 70 & 120 kd | Macrophages | — | 4 |
| BDCA-2, BDCA-3, & BDCA-4 antigens | ND | Dendritic cells | Identifies subsets of dendritic cells | 5 |
| BENE | 17 kd | Endothelium | “Raft-associated” member of MAL family; interacts with caveolin-1 | 6 |
| CMRF-44 | ND | Dendritic cells | Differentiation/activation marker | 7, 8 |
| CMRF-56 | 95 kd | Dendritic cells | Differentiation/activation marker | 7, 8 |
| H47 antigen | 100 kd3-150(120 kd) | T cells & most NK cells, B cells, and monocytes | Involved in T cell activation? | 9 |
| Hal-1 | 200 kd3-150 (100 kd) | T cells, EBV-transformed B-cells, myelomonocytic cells, anaplastic large cell lymphoma | New lymphoma marker? | 10 |
| LAK1 antigen | 120 kd | LGL and LAK cells | — | 11 |
| LAK2 antigen | 110 + 140 kd | LGL and LAK cells | — | 11 |
| NKp80 | 80 kd dimer | NK cells and CD56-positive T cells | Novel member of the killer cell lectinlike receptor gene family, encoded by KLRF1 gene; triggers NK cell cytotoxicity | 12, 13 |
| VAP-13-151 | 90 kd | Endothelium | Mediates lymphocyte-endothelial adhesion; has monoamine oxidase activity | 14, 15 |
| Wue-1 antigen | 94 kd | Plasma cells | Stimulates growth of plasma cells | 16 |
| Identified via gene cloning | ||||
| BCMA3-152 | 184 aa | B cells | TNFR family member; receptor for TALL-1 and APRIL | 17, 18 |
| B7-H2 | 302 aa | Dendritic cells | New member of B7 family; binds ICOS on activated T cells | 19 |
| CLEC-1 | 280 aa | Dendritic cells | Novel C-type lectin-like receptor with cytoplasmic tyrosine-based motif | 20 |
| CMRF-35A | 224 aa | NK cells, neutrophils, monocytes, dendritic cells and subset of T lymphocytes | Novel Ig superfamily receptors; CMRF-35H contains 3 cytoplasmic tyrosine based motifs | 21, 22 |
| CMRF-35H | 300 aa | NK cells, neutrophils, monocytes, dendritic cells and subset of T lymphocytes | Novel Ig superfamily receptors; CMRF-35H contains 3 cytoplasmic tyrosine based motifs | 21,22 |
| CS1 | ND | NK cells | Novel receptor belonging to CD2 subset of Ig superfamily | 23 |
| DC-STAMP | 470 aa | Dendritic cells | Novel protein containing 7 putative transmembrane domains | 24 |
| EMR3 | 652 aa | Mainly leucocyte restricted. Highest levels on neutrophils, monocytes and macrophages | Novel EGF-TM7 molecule; interacts with a surface ligand on myeloid cells | 25 |
| Flt-1 (VEGFR-1) | ND | Endothelial cells, monocytes | — | 26 |
| GPRv53 | 390 aa | Leukocytes | G-protein-coupled histamine receptor | 27 |
| IRTA1, IRTA2 | ND | Subpopulations of B cells | Homologous to the Fc and inhibitory receptor families | 28 |
| M160 | 1453 aa | Macrophages | New member of scavenger receptor cysteine-rich superfamily | 29 |
| MARCO3-153 | 520 aa | Macrophages | Class A scavenger receptor; involved in bacterial clearance in vivo | 30, 31 |
| TACI | 293 aa | B cells | TNFR family member; receptor for TALL-1 and APRIL | 32 |
| TREM-13-155 | ND | Neutrophils and subset of monocytes | Novel Ig superfamily receptor; triggers neutrophil secretion (eg, IL-8) and degranulation; associates with DAP12 | 33, 34 |
| TREM-23-155 | ND | Neutrophils and subset of macrophages | Novel Ig superfamily receptor; activates macrophages; associates with DAP12 | 33, 34 |
| Molecule . | Molecule size . | Cell types . | Comments . | Reference(s) . |
|---|---|---|---|---|
| Identified following antibody production | ||||
| AM-3K antigen | 70 & 120 kd | Macrophages | — | 4 |
| BDCA-2, BDCA-3, & BDCA-4 antigens | ND | Dendritic cells | Identifies subsets of dendritic cells | 5 |
| BENE | 17 kd | Endothelium | “Raft-associated” member of MAL family; interacts with caveolin-1 | 6 |
| CMRF-44 | ND | Dendritic cells | Differentiation/activation marker | 7, 8 |
| CMRF-56 | 95 kd | Dendritic cells | Differentiation/activation marker | 7, 8 |
| H47 antigen | 100 kd3-150(120 kd) | T cells & most NK cells, B cells, and monocytes | Involved in T cell activation? | 9 |
| Hal-1 | 200 kd3-150 (100 kd) | T cells, EBV-transformed B-cells, myelomonocytic cells, anaplastic large cell lymphoma | New lymphoma marker? | 10 |
| LAK1 antigen | 120 kd | LGL and LAK cells | — | 11 |
| LAK2 antigen | 110 + 140 kd | LGL and LAK cells | — | 11 |
| NKp80 | 80 kd dimer | NK cells and CD56-positive T cells | Novel member of the killer cell lectinlike receptor gene family, encoded by KLRF1 gene; triggers NK cell cytotoxicity | 12, 13 |
| VAP-13-151 | 90 kd | Endothelium | Mediates lymphocyte-endothelial adhesion; has monoamine oxidase activity | 14, 15 |
| Wue-1 antigen | 94 kd | Plasma cells | Stimulates growth of plasma cells | 16 |
| Identified via gene cloning | ||||
| BCMA3-152 | 184 aa | B cells | TNFR family member; receptor for TALL-1 and APRIL | 17, 18 |
| B7-H2 | 302 aa | Dendritic cells | New member of B7 family; binds ICOS on activated T cells | 19 |
| CLEC-1 | 280 aa | Dendritic cells | Novel C-type lectin-like receptor with cytoplasmic tyrosine-based motif | 20 |
| CMRF-35A | 224 aa | NK cells, neutrophils, monocytes, dendritic cells and subset of T lymphocytes | Novel Ig superfamily receptors; CMRF-35H contains 3 cytoplasmic tyrosine based motifs | 21, 22 |
| CMRF-35H | 300 aa | NK cells, neutrophils, monocytes, dendritic cells and subset of T lymphocytes | Novel Ig superfamily receptors; CMRF-35H contains 3 cytoplasmic tyrosine based motifs | 21,22 |
| CS1 | ND | NK cells | Novel receptor belonging to CD2 subset of Ig superfamily | 23 |
| DC-STAMP | 470 aa | Dendritic cells | Novel protein containing 7 putative transmembrane domains | 24 |
| EMR3 | 652 aa | Mainly leucocyte restricted. Highest levels on neutrophils, monocytes and macrophages | Novel EGF-TM7 molecule; interacts with a surface ligand on myeloid cells | 25 |
| Flt-1 (VEGFR-1) | ND | Endothelial cells, monocytes | — | 26 |
| GPRv53 | 390 aa | Leukocytes | G-protein-coupled histamine receptor | 27 |
| IRTA1, IRTA2 | ND | Subpopulations of B cells | Homologous to the Fc and inhibitory receptor families | 28 |
| M160 | 1453 aa | Macrophages | New member of scavenger receptor cysteine-rich superfamily | 29 |
| MARCO3-153 | 520 aa | Macrophages | Class A scavenger receptor; involved in bacterial clearance in vivo | 30, 31 |
| TACI | 293 aa | B cells | TNFR family member; receptor for TALL-1 and APRIL | 32 |
| TREM-13-155 | ND | Neutrophils and subset of monocytes | Novel Ig superfamily receptor; triggers neutrophil secretion (eg, IL-8) and degranulation; associates with DAP12 | 33, 34 |
| TREM-23-155 | ND | Neutrophils and subset of macrophages | Novel Ig superfamily receptor; activates macrophages; associates with DAP12 | 33, 34 |
ND indicates not determined.
The nonreduced size; reduced size given in parentheses.
Vascular adhesion protein.
B cell maturation factor.
Macrophage receptor with collagenous structure.
Triggering receptor expressed on myeloid cells.
Finally, it remains to be established how the eighth and subsequent HLDA workshops should deal with lineage- or stage-restricted leukocyte molecules that are localized within the cell cytoplasm (or nucleus). Given the importance of many of these molecules in signaling pathways initiated via known surface CD molecules, their identification and study is an inevitable extension of the work of the first seven HLDA workshops. Whether or not a new “intracellular CD” categorization scheme is devised for such molecules, they are of interest for many laboratories studying human hematopoietic cells, and their investigation will be among the aims of the next workshop.
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