CD70

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Structures	Swiss-model
Domains	InterPro

CD70 molecule
CD70 molecule
Identifiers
Symbol	CD70
Alt. symbols	CD27LG, TNFSF7
NCBI gene	970
HGNC	11937
OMIM	602840
RefSeq	NM_001252
UniProt	P32970
Other data
Locus	Chr. 19 p13
Structures
Search for
Structures	Swiss-model
Domains	InterPro

Last updated December 22, 2023

CD70 (Cluster of Differentiation 70) is a protein that in humans is encoded by CD70 gene. CD70 is also known as a ligand for CD27.^[1]

Expression

In physiological condition the expression of CD70 on immune cells is transient and tightly controlled. It is primarily expressed on highly activated T cells and B cells, as well as on NK cells and mature dendritic cells. CD70 expression on T and B cells is stimulated through triggering of T and B cell receptors and can be upregulated by cytokines such as IL-1α, IL-2, IL-12, GM-CSF and TNF-α, while IL-4 and IL-10 can decrease CD70 expression.^[2] Expression of CD70 on mDCs and pDCs is induced with Toll-like receptor (TLR) triggering and CD40 ligation.^[3] Also, CD70 can be induced on NK cells upon stimulation with IL-15.^[4]

Functions

CD70 acts as a costimulatory molecule and plays an important role in the regulation of the immune system activation, specifically by improving T-cell and B-cell activation, proliferation and survival, leading to a more efficient immune response.^[5]

CD70 on activated antigen presenting cells (APC) including dendritic cells and B cells binds to CD27 on T lymphocytes and provides costimulatory signals. The interaction between CD27 and CD70 leads to the recruitment of intracellular adaptor proteins, such as TRAF2 and TRAF5, which then activate signaling pathways, including the NF-κB and JNK pathway.^[6]^[7] CD27 signaling stimulates naïve CD4+ T lymphocytes to differentiate into Th1 cells by activation the transcription factor T-bet.^[7]

In addition to its role in T-cell activation and proliferation, CD70 also plays a role in the regulation of B-cell activation and differentiation. Receptor engagement can also cause reverse signaling through CD70. CD70 reverse signaling activates the phosphatidylinositol-3 kinase (PI3K) and MAP kinase signaling pathways, leading to the activation of various transcription factors and the expression of genes involved in cell growth and survival.^[8]

Clinical significance

Cancer

Some studies have shown that CD70 is overexpressed in several types of cancer, including Hodgkin's lymphoma and non-Hodgkin's lymphoma. CD70 is also found to be overexpressed in some types of solid tumors.^[9]^[10]^[11] This overexpression of CD70 in cancer cells has been shown to promote cell proliferation and survival, and to inhibit apoptosis, leading to the development and progression of the cancer. It is therefore suggested that anti-CD70 antibodies might be a possible treatment for CD70 positive lymphomas as normal lymphocytes have low CD70 expression.^[12]

Drug development

Recent research has focused on the potential therapeutic use of CD70 in cancer treatment. One strategy being investigated is the use of antibodies that target CD70. ARGX-110 is a CD70-specific antibody that is currently under investigation for the treatment of hematological malignancies. It is being developed by the Belgian company arGEN-X. In December 2013 a first part of a phase 1b trial was completed. In January 2014 a safety and efficacy phase of the study started.^[13]

Vorsetuzumab mafodotin is a CD70-targeted antibody-drug conjugate that started clinical trials for renal cell carcinoma.^[14]

Related Research Articles

Interleukin 12 (IL-12) is an interleukin that is naturally produced by dendritic cells, macrophages, neutrophils, and human B-lymphoblastoid cells (NC-37) in response to antigenic stimulation. IL-12 belongs to the family of interleukin-12. IL-12 family is unique in comprising the only heterodimeric cytokines, which includes IL-12, IL-23, IL-27 and IL-35. Despite sharing many structural features and molecular partners, they mediate surprisingly diverse functional effects.

Cluster of differentiation 40, CD40 is a type I transmembrane protein found on antigen-presenting cells and is required for their activation. The binding of CD154 (CD40L) on T_H cells to CD40 activates antigen presenting cells and induces a variety of downstream effects.

Co-stimulation is a secondary signal which immune cells rely on to activate an immune response in the presence of an antigen-presenting cell. In the case of T cells, two stimuli are required to fully activate their immune response. During the activation of lymphocytes, co-stimulation is often crucial to the development of an effective immune response. Co-stimulation is required in addition to the antigen-specific signal from their antigen receptors.

<span class="mw-page-title-main">CD86</span> Mammalian protein found in Homo sapiens

Cluster of Differentiation 86 is a protein constitutively expressed on dendritic cells, Langerhans cells, macrophages, B-cells, and on other antigen-presenting cells. Along with CD80, CD86 provides costimulatory signals necessary for T cell activation and survival. Depending on the ligand bound, CD86 can signal for self-regulation and cell-cell association, or for attenuation of regulation and cell-cell disassociation.

CCL17 is a powerful chemokine produced in the thymus and by antigen-presenting cells like dendritic cells, macrophages, and monocytes. CCL17 plays a complex role in cancer. It attracts T-regulatory cells allowing for some cancers to evade an immune response. However, in other cancers, such as melanoma, an increase in CCL17 is linked to an improved outcome. CCL17 has also been linked to autoimmune and allergic diseases.

B-lymphocyte antigen CD19, also known as CD19 molecule, B-Lymphocyte Surface Antigen B4, T-Cell Surface Antigen Leu-12 and CVID3 is a transmembrane protein that in humans is encoded by the gene CD19. In humans, CD19 is expressed in all B lineage cells. Contrary to some early doubts, human plasma cells do express CD19, as confirmed by others. CD19 plays two major roles in human B cells: on the one hand, it acts as an adaptor protein to recruit cytoplasmic signaling proteins to the membrane; on the other, it works within the CD19/CD21 complex to decrease the threshold for B cell receptor signaling pathways. Due to its presence on all B cells, it is a biomarker for B lymphocyte development, lymphoma diagnosis and can be utilized as a target for leukemia immunotherapies.

B-cell activating factor (BAFF) also known as tumor necrosis factor ligand superfamily member 13B and CD257 among other names, is a protein that in humans is encoded by the TNFSF13B gene. BAFF is also known as B Lymphocyte Stimulator (BLyS) and TNF- and APOL-related leukocyte expressed ligand (TALL-1) and the Dendritic cell-derived TNF-like molecule.

CD137, a member of the tumor necrosis factor (TNF) receptor family, is a type 1 transmembrane protein, expressed on surfaces of leukocytes and non-immune cells. Its alternative names are tumor necrosis factor receptor superfamily member 9 (TNFRSF9), 4-1BB, and induced by lymphocyte activation (ILA). It is of interest to immunologists as a co-stimulatory immune checkpoint molecule, and as a potential target in cancer immunotherapy.

CD27 is a member of the tumor necrosis factor receptor superfamily. It is currently of interest to immunologists as a co-stimulatory immune checkpoint molecule, and is the target of an anti-cancer drug in clinical trials.

Cancer immunology (immuno-oncology) is an interdisciplinary branch of biology and a sub-discipline of immunology that is concerned with understanding the role of the immune system in the progression and development of cancer; the most well known application is cancer immunotherapy, which utilises the immune system as a treatment for cancer. Cancer immunosurveillance and immunoediting are based on protection against development of tumors in animal systems and (ii) identification of targets for immune recognition of human cancer.

C-C chemokine receptor type 7 is a protein that in humans is encoded by the CCR7 gene. Two ligands have been identified for this receptor: the chemokines ligand 19 (CCL19/ELC) and ligand 21 (CCL21). The ligands have similar affinity for the receptor, though CCL19 has been shown to induce internalisation of CCR7 and desensitisation of the cell to CCL19/CCL21 signals. CCR7 is a transmembrane protein with 7 transmembrane domains, which is coupled with heterotrimeric G proteins, which transduce the signal downstream through various signalling cascades. The main function of the receptor is to guide immune cells to immune organs by detecting specific chemokines, which these tissues secrete.

PR domain zinc finger protein 1, or B lymphocyte-induced maturation protein-1 (BLIMP-1), is a protein in humans encoded by the gene PRDM1 located on chromosome 6q21. BLIMP-1 is considered a 'master regulator' of hematopoietic stem cells, and plays a critical role in the development of plasma B cells, T cells, dendritic cells (DCs), macrophages, and osteoclasts. Pattern Recognition Receptors (PRRs) can activate BLIMP-1, both as a direct target and through downstream activation. BLIMP-1 is a transcription factor that triggers expression of many downstream signaling cascades. As a fine-tuned and contextual rheostat of the immune system, BLIMP-1 up- or down-regulates immune responses depending on the precise scenarios. BLIMP-1 is highly expressed in exhausted T-cells – clones of dysfunctional T-cells with diminished functions due to chronic immune response against cancer, viral infections, or organ transplant.

Lymphocyte-activation gene 3, also known as LAG-3, is a protein which in humans is encoded by the LAG3 gene. LAG3, which was discovered in 1990 and was designated CD223 after the Seventh Human Leucocyte Differentiation Antigen Workshop in 2000, is a cell surface molecule with diverse biologic effects on T cell function. It is an immune checkpoint receptor and as such is the target of various drug development programs by pharmaceutical companies seeking to develop new treatments for cancer and autoimmune disorders. In soluble form it is also being developed as a cancer drug in its own right.

Fc fragment of IgG receptor IIb is a low affinity inhibitory receptor for the Fc region of immunoglobulin gamma (IgG). FCGR2B participates in the phagocytosis of immune complexes and in the regulation of antibody production by B lymphocytes.

The Interleukin-2 receptor alpha chain is a protein involved in the assembly of the high-affinity Interleukin-2 receptor, consisting of alpha (IL2RA), beta (IL2RB) and the common gamma chain (IL2RG). As the name indicates, this receptor interacts with Interleukin-2, a pleiotropic cytokine which plays an important role in immune homeostasis.

Marginal-zone B cells are noncirculating mature B cells that in humans segregate anatomically into the marginal zone (MZ) of the spleen and certain other types of lymphoid tissue. The MZ B cells within this region typically express low-affinity polyreactive B-cell receptors (BCR), high levels of IgM, Toll-like receptors (TLRs), CD21, CD1, CD9, CD27 with low to negligible levels of secreted-IgD, CD23, CD5, and CD11b that help to distinguish them phenotypically from follicular (FO) B cells and B1 B cells.

Gene expression profiling has revealed that diffuse large B-cell lymphoma (DLBCL) is composed of at least 3 different sub-groups, each having distinct oncogenic mechanisms that respond to therapies in different ways. Germinal Center B-Cell like (GCB) DLBCLs appear to arise from normal germinal center B cells, while Activated B-cell like (ABC) DLBCLs are thought to arise from postgerminal center B cells that are arrested during plasmacytic differentiation. The differences in gene expression between GCB DLBCL and ABC DLBCL are as vast as the differences between distinct types of leukemia, but these conditions have historically been grouped together and treated as the same disease.

<span class="mw-page-title-main">Centroblast</span>

A centroblast generally refers to an activated B cell that is enlarged and is rapidly proliferating in the germinal center of a lymphoid follicle. They are specifically located in the dark zone of the germinal center. Centroblasts form from naive B cells being exposed to follicular dendritic cell cytokines, such as IL-6, IL-15, 8D6, and BAFF. Stimulation from helper T cells is also required for centroblast development. Interaction between CD40 ligand on an activated T helper cell and the B cell CD40 receptor induces centroblasts to express activation-induced cytidine deaminase, leading to somatic hypermutation, allowing the B cell receptor to potentially gain stronger affinity for an antigen. In the absence of FDC and helper T cell stimulation, centroblasts are unable to differentiate and will undergo CD95-mediated apoptosis.

Immune checkpoints are regulators of the immune system. These pathways are crucial for self-tolerance, which prevents the immune system from attacking cells indiscriminately. However, some cancers can protect themselves from attack by stimulating immune checkpoint targets.

B10 cells are a sub-class of regulatory B-cells that are involved in inhibiting immune responses in both humans and mice. B10 cells are named for their ability to produce inhibitory interleukin: Interleukin-10 (IL-10). One of their unique abilities is that they suppress the innate and adaptive immune signals, making them important for regulating the inflammatory response. Like the B cell, the B10 cell requires antigen specific binding to the surface of CD5 receptor to illicit a response from the T-cell. Once an antigen binds to the CD19 receptor, immediate downregulation in B-cell receptor (BCR) signal expression occurs and mediates the release of IL-10 cytokines. In mice and humans, B10 cells are distinguishable in their expression of measurable IL-10 due to the lack of unique cell surface markers expressed by regulatory B cells. However, IL-10 competence is not limited to any one subset of B cells. B10 cells do not possess unique phenotypic markers or transcription factors for further identification. B10 cells predominantly localize in the spleen, though they are also found in the blood, lymph nodes, Peyer's patches, intestinal tissues, central nervous system, and peritoneal cavity. B10 cells proliferate during inflammatory and disease responses.

References

↑ "NCBI".
↑ Nolte MA, van Olffen RW, van Gisbergen KP, van Lier RA (May 2009). "Timing and tuning of CD27-CD70 interactions: the impact of signal strength in setting the balance between adaptive responses and immunopathology". Immunological Reviews. 229 (1): 216–231. doi:10.1111/j.1600-065X.2009.00774.x. PMID 19426224. S2CID 32860864.
↑ Hashimoto-Okada M, Kitawaki T, Kadowaki N, Iwata S, Morimoto C, Hori T, Uchiyama T (2009). "The CD70–CD27 interaction during the stimulation with dendritic cells promotes naive CD4+ T cells to develop into T cells producing a broad array of immunostimulatory cytokines in humans". International Immunology. 21 (8): 891–904. doi:10.1093/intimm/dxp056. hdl: 2433/86187 . PMID 19556308 . Retrieved 8 February 2023.
↑ Vossen MT, Matmati M, Hertoghs KM, Baars PA, Gent M, Leclercq G, Hamann J, Kuijpers TW, van Lier RA (15 March 2008). "CD27 Defines Phenotypically and Functionally Different Human NK Cell Subsets". The Journal of Immunology. 180 (6): 3739–3745. doi: 10.4049/jimmunol.180.6.3739 . ISSN 0022-1767. PMID 18322179. S2CID 26953338.
↑ Borst J, Hendriks J, Xiao Y (1 June 2005). "CD27 and CD70 in T cell and B cell activation". Current Opinion in Immunology. Lymphocyte activation / Lymphocyte effector functions. 17 (3): 275–281. doi:10.1016/j.coi.2005.04.004. ISSN 0952-7915. PMID 15886117.
↑ Boursalian TE, McEarchern JA, Law C, Grewal IS (2009), Grewal IS (ed.), "Targeting CD70 for Human Therapeutic Use", Therapeutic Targets of the TNF Superfamily, New York, NY: Springer New York, vol. 647, pp. 108–119, doi:10.1007/978-0-387-89520-8_7, ISBN 978-0-387-89519-2, PMID 19760069 , retrieved 8 February 2023
1 2 Han BK, Olsen NJ, Bottaro A (1 February 2016). "The CD27–CD70 pathway and pathogenesis of autoimmune disease". Seminars in Arthritis and Rheumatism. 45 (4): 496–501. doi:10.1016/j.semarthrit.2015.08.001. ISSN 0049-0172. PMID 26359318.
↑ Arens R, Nolte MA, Tesselaar K, Heemskerk B, Reedquist KA, van Lier RA, van Oers MH (15 September 2004). "Signaling through CD70 Regulates B Cell Activation and IgG Production". The Journal of Immunology. 173 (6): 3901–3908. doi: 10.4049/jimmunol.173.6.3901 . ISSN 0022-1767. PMID 15356138. S2CID 31566653.
↑ Junker K, Hindermann W, von EF, Diegmann J, Haessler K, Schubert J (1 June 2005). "Cd70: a new tumor specific biomarker for renal cell carcinoma". Journal of Urology. 173 (6): 2150–2153. doi:10.1097/01.ju.0000158121.49085.ba. PMID 15879877.
↑ Held-Feindt J, Mentlein R (7 March 2002). "CD70/CD27 ligand, a member of the TNF family, is expressed in human brain tumors". International Journal of Cancer. 98 (3): 352–356. doi: 10.1002/ijc.10207 . ISSN 0020-7136. PMID 11920585. S2CID 12298972.
↑ Hishima T, Fukayama M, Hayashi Y, Fujii T, Ooba T, Funata N, Koike M (May 2000). "CD70 Expression in Thymic Carcinoma". The American Journal of Surgical Pathology. 24 (5): 742–746. doi:10.1097/00000478-200005000-00014. ISSN 0147-5185. PMID 10800994.
↑ Israel BF, Gulley M, Elmore S, Ferrini S, Feng WH, Kenney SC (2005). "Anti-CD70 antibodies: a potential treatment for EBV+ CD70-expressing lymphomas". Mol. Cancer Ther. 4 (12): 2037–44. doi:10.1158/1535-7163.MCT-05-0253. PMID 16373719. S2CID 1821535.
↑ "ARGX-110: first-in-class CD70-targeting antibody with unique mode of therapeutic action". arGEN-X. Archived from the original on 9 March 2015. Retrieved 28 February 2015.
↑ Seattle Genetics Third Quarter 2013 Financial Report ^{[ permanent dead link ]}

External links

CD70+Antigens at the U.S. National Library of Medicine Medical Subject Headings (MeSH)

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[1] "NCBI".

[2] Nolte MA, van Olffen RW, van Gisbergen KP, van Lier RA (May 2009). "Timing and tuning of CD27-CD70 interactions: the impact of signal strength in setting the balance between adaptive responses and immunopathology". Immunological Reviews. 229 (1): 216–231. doi:10.1111/j.1600-065X.2009.00774.x. PMID 19426224. S2CID 32860864.

[3] Hashimoto-Okada M, Kitawaki T, Kadowaki N, Iwata S, Morimoto C, Hori T, Uchiyama T (2009). "The CD70–CD27 interaction during the stimulation with dendritic cells promotes naive CD4+ T cells to develop into T cells producing a broad array of immunostimulatory cytokines in humans". International Immunology. 21 (8): 891–904. doi:10.1093/intimm/dxp056. hdl: 2433/86187 . PMID 19556308 . Retrieved 8 February 2023.

[4] Vossen MT, Matmati M, Hertoghs KM, Baars PA, Gent M, Leclercq G, Hamann J, Kuijpers TW, van Lier RA (15 March 2008). "CD27 Defines Phenotypically and Functionally Different Human NK Cell Subsets". The Journal of Immunology. 180 (6): 3739–3745. doi: 10.4049/jimmunol.180.6.3739 . ISSN 0022-1767. PMID 18322179. S2CID 26953338.

[5] Borst J, Hendriks J, Xiao Y (1 June 2005). "CD27 and CD70 in T cell and B cell activation". Current Opinion in Immunology. Lymphocyte activation / Lymphocyte effector functions. 17 (3): 275–281. doi:10.1016/j.coi.2005.04.004. ISSN 0952-7915. PMID 15886117.

[6] Boursalian TE, McEarchern JA, Law C, Grewal IS (2009), Grewal IS (ed.), "Targeting CD70 for Human Therapeutic Use", Therapeutic Targets of the TNF Superfamily, New York, NY: Springer New York, vol. 647, pp. 108–119, doi:10.1007/978-0-387-89520-8_7, ISBN 978-0-387-89519-2, PMID 19760069 , retrieved 8 February 2023

[:0-7] 1 2 Han BK, Olsen NJ, Bottaro A (1 February 2016). "The CD27–CD70 pathway and pathogenesis of autoimmune disease". Seminars in Arthritis and Rheumatism. 45 (4): 496–501. doi:10.1016/j.semarthrit.2015.08.001. ISSN 0049-0172. PMID 26359318.

[8] Arens R, Nolte MA, Tesselaar K, Heemskerk B, Reedquist KA, van Lier RA, van Oers MH (15 September 2004). "Signaling through CD70 Regulates B Cell Activation and IgG Production". The Journal of Immunology. 173 (6): 3901–3908. doi: 10.4049/jimmunol.173.6.3901 . ISSN 0022-1767. PMID 15356138. S2CID 31566653.

[9] Junker K, Hindermann W, von EF, Diegmann J, Haessler K, Schubert J (1 June 2005). "Cd70: a new tumor specific biomarker for renal cell carcinoma". Journal of Urology. 173 (6): 2150–2153. doi:10.1097/01.ju.0000158121.49085.ba. PMID 15879877.

[10] Held-Feindt J, Mentlein R (7 March 2002). "CD70/CD27 ligand, a member of the TNF family, is expressed in human brain tumors". International Journal of Cancer. 98 (3): 352–356. doi: 10.1002/ijc.10207 . ISSN 0020-7136. PMID 11920585. S2CID 12298972.

[11] Hishima T, Fukayama M, Hayashi Y, Fujii T, Ooba T, Funata N, Koike M (May 2000). "CD70 Expression in Thymic Carcinoma". The American Journal of Surgical Pathology. 24 (5): 742–746. doi:10.1097/00000478-200005000-00014. ISSN 0147-5185. PMID 10800994.

[12] Israel BF, Gulley M, Elmore S, Ferrini S, Feng WH, Kenney SC (2005). "Anti-CD70 antibodies: a potential treatment for EBV+ CD70-expressing lymphomas". Mol. Cancer Ther. 4 (12): 2037–44. doi:10.1158/1535-7163.MCT-05-0253. PMID 16373719. S2CID 1821535.

[13] "ARGX-110: first-in-class CD70-targeting antibody with unique mode of therapeutic action". arGEN-X. Archived from the original on 9 March 2015. Retrieved 28 February 2015.

[SG3Q2013-14] Seattle Genetics Third Quarter 2013 Financial Report ^{[ permanent dead link ]}

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v t e Proteins: clusters of differentiation (see also list of human clusters of differentiation)
1–50	CD1 a-c 1A 1B 1D 1E CD2 CD3 γ δ ε CD4 CD5 CD6 CD7 CD8 a CD9 CD10 CD11 a b c d CD13 CD14 CD15 CD16 A B CD18 CD19 CD20 CD21 CD22 CD23 CD24 CD25 CD26 CD27 CD28 CD29 CD30 CD31 CD32 A B CD33 CD34 CD35 CD36 CD37 CD38 CD39 CD40 CD41 CD42 a b c d CD43 CD44 CD45 CD46 CD47 CD48 CD49 a b c d e f CD50
51–100	CD51 CD52 CD53 CD54 CD55 CD56 CD57 CD58 CD59 CD61 CD62 E L P CD63 CD64 A B C CD66 a b c d e f CD68 CD69 CD70 CD71 CD72 CD73 CD74 CD78 CD79 a b CD80 CD81 CD82 CD83 CD84 CD85 a d e h j k CD86 CD87 CD88 CD89 CD90 CD91 - CD92 CD93 CD94 CD95 CD96 CD97 CD98 CD99 CD100
101–150	CD101 CD102 CD103 CD104 CD105 CD106 CD107 a b CD108 CD109 CD110 CD111 CD112 CD113 CD114 CD115 CD116 CD117 CD118 CD119 CD120 a b CD121 a b CD122 CD123 CD124 CD125 CD126 CD127 CD129 CD130 CD131 CD132 CD133 CD134 CD135 CD136 CD137 CD138 CD140b CD141 CD142 CD143 CD144 CD146 CD147 CD148 CD150
151–200	CD151 CD152 CD153 CD154 CD155 CD156 a b c CD157 CD158 (a d e i k) CD159 a c CD160 CD161 CD162 CD163 CD164 CD166 CD167 a b CD168 CD169 CD170 CD171 CD172 a b g CD174 CD177 CD178 CD179 a b CD180 CD181 CD182 CD183 CD184 CD185 CD186 CD191 CD192 CD193 CD194 CD195 CD196 CD197 CDw198 CDw199 CD200
201–250	CD201 CD202b CD204 CD205 CD206 CD207 CD208 CD209 CDw210 a b CD212 CD213a 1 2 CD217 CD218 (a b) CD220 CD221 CD222 CD223 CD224 CD225 CD226 CD227 CD228 CD229 CD230 CD233 CD234 CD235 a b CD236 CD238 CD239 CD240CE CD240D CD241 CD243 CD244 CD246 CD247 - CD248 CD249
251–300	CD252 CD253 CD254 CD256 CD257 CD258 CD261 CD262 CD263 CD264 CD265 CD266 CD267 CD268 CD269 CD271 CD272 CD273 CD274 CD275 CD276 CD278 CD279 CD280 CD281 CD282 CD283 CD284 CD286 CD288 CD289 CD290 CD292 CDw293 CD294 CD295 CD297 CD298 CD299
301–350	CD300A CD301 CD302 CD303 CD304 CD305 CD306 CD307 CD309 CD312 CD314 CD315 CD316 CD317 CD318 CD320 CD321 CD322 CD324 CD325 CD326 CD327 CD328 CD329 CD331 CD332 CD333 CD334 CD335 CD336 CD337 CD338 CD339 CD340 CD344 CD349 CD350