Open access

Ten-year anniversary of CD3δ deficiency

Publication: LymphoSign Journal
3 February 2015

Abstract

CD3δ deficiency was first identified a decade ago by using differential expression libraries derived from thymocytes of patients with severe combined immunodeficiency. The phenotype was surprisingly severe unlike the mouse model or other human CD3 deficiencies known at that time.
The T-cell receptor (TCR) complex consists of a variable surface TCR heterodimer (αβ or γδ), 2 invariant heterodimers that include the CD3γɛ chain and the CD3δɛ chains, as well as a single invariant homodimer called ξ (Call et al. 2002). The variable chains recognize antigens, whereas the role of the invariant chains is to effectively transmit signals into the cytoplasm. This is done through a series of tyrosine phosphorylation events leading to activation of downstream signaling pathways including the PLCγ, PI3K, and MAPK pathways. These signals trigger cytoskeletal changes (actin assembly), secretion of growth factors, and expression of growth and cell contact receptors. This process culminates in differentiation, clonal expansion, or when necessary, apoptosis of T cells.
A decade ago, CD3δ deficiency was first described in Roifman's laboratory (Dadi et al. 2003). Infants of Mennonite descent presented with typical features of severe combined immunodeficiency (SCID), yet they had a detectable thymus gland that was bigger than is usually seen in traditional cases of SCID (Roifman 2005). Evaluation of a thymus biopsy from the patient surprisingly revealed a gland heavily populated with thymocytes. Yet, although not completely dysplastic, the thymus had no visible Hassall's corpuscles, which is the hallmark of primary immunodeficiency.
In the pre-Whole Exome Sequencing era, there could be 2 potential routes to follow to define the genetic basis of this disease. One was the traditional linkage analysis method, which at that time required multiple subjects, and the other was using the candidate gene approach. The number of subjects was very limited in this cohort and several candidate genes that had been tested were found normal. We therefore decided to undertake a novel approach.
Our method relied on the comparison of mRNA expression (expression libraries) between patient cells and controls. Usually this would have been a monumental task of sorting through too many variables with a low success rate of gene discovery. In this case, we hypothesized that by comparing 2 very “clean” cell types, i.e., age-matched thymocytes derived from patient thymus biopsy or from a normal thymus (infants who undergo thymectomy during heart surgery), the number of potential genes to be assessed could be manageable. Strikingly, significant immune-related mRNA expression variations were fewer than 15 gene products. CD3δ was one of the possible candidates, yet it was not chosen as a first candidate for several reasons.
First, previous descriptions of other CD3 chain deficiencies were associated with a spectrum of clinical and immunological presentations ranging from leaky SCID (<10) to normal healthy subjects for complete CD3γ deficiency (Arnaiz-Villena et al. 1992) or leaky SCID for CD3ɛ deficiency (Soudais et al. 1993).
Second, the CD3δ-null mouse appeared to be very leaky, similar to the human CD3γ deficiency (Dave et al. 1997). In contrast, CD3δ deficiency in our cohort resulted in complete absence of circulating T cells and a typical SCID phenotype. It was therefore a surprise to find the disease causing the mutation in the gene for CD3δ. This clearly indicated that in humans CD3δ, but not CD3γ, is critical for T-cell maturation and emigration out of the thymus. This is consistent with the finding that CD3δ can replace CD3γ but the reverse is ineffective (Zapata et al. 2004).
Third, the set of experiments leading to the discovery of CD3δ deficiency were possible only because of the availability of the patient's thymus tissue.
Complete CD3δ deficiency is fatal during infancy unless rescued with hematopoetic stem cell therapy (Marcus et al. 2011).
Our personal experience, as well as the experiences of others, indicates that using matched-related or unrelated donors is highly successful. Indeed, follow-up beyond 15 years post-transplantation reveals that all patients are well, and an assessment of the immune system shows a robust–normal immune reconstitution. In contrast, haplo-identical transplants failed in most attempts in these patients and should be avoided (Rieux-Laucat et al. 2006; Roberts et al. 2007; Marcus et al. 2011).
Recently, cases with partial CD3δ deficiency (Garcillán et al. 2014) have been described as well as deficiencies in other CD3 and TCR chains. This issue includes an excellent review by Marin et al. (p. 3) that summarizes all new discoveries.

REFERENCES

Arnaiz-Villena A., Timon M., Corell A., Perez-Aciego P., Martin-Villa J.M., and Regueiro J.R. Brief report: primary immunodeficiency caused by mutations in the gene encoding the CD3-gamma subunit of the T-lymphocyte receptor N. Engl. J. Med. 1992 327 8 529 -533
Call M.E., Pyrdol J., Wiedmann M., and Wucherpfennig K.W. The organizing principle in the formation of the T cell receptor-CD3 complex Cell. 2002 111 7 967 -979
Dadi H., Simon A.J., and Roifman C.M. Effect of CD3d deficiency on maturation of ab and gd T-cell lineages in Severe Combined Immunodeficiency N. Engl. J. Med. 2003 349 19 1821 -1828
Dave V.P., Cao Z., Browne C., Alarcon B., Fernandez-Miguel G., Lafaille J., de la Hera A., Tonegawa S., and Kappes D.J. CD3 delta deficiency arrests development of the alpha beta but not the gamma delta T cell lineage EMBO. J. 1997 16 6 1360 -1370
Garcillán B., Mazariegos M.S., Fisch P., Res P.C., Muñoz-Ruiz M., Gil J., Lopez-Granados E., Fernandez-Malave E., and Regueiro J.R. Enrichment of the rare CD4+γδ T-cell subset in patients with atypical CD3δ deficiency J. Allergy Clin. Immunol. 2014 133 4 1205 -1208.e9
Marcus N., Takada H., Law J., Cowan M.J., Gil J., Regueiro J.R., Plaza Lopez de Sabando D., Lopez-Granados E., Dalal J., Friedrich W., Manfred H., Hanson I.C., Grunebaum E., Shearer W.T., and Roifman C.M. Hematopoietic stem cell transplantation for CD3delta deficiency J. Allergy Clin. Immunol. 2011 128 5 1050 -1057
Rieux-Laucat F., Hivroz C., Lim A., Mateo V., Pellier I., Selz F., Fischer A., and Le Deist F. Inherited and somatic CD3zeta mutations in a patient with T-cell deficiency N. Engl. J. Med. 2006 354 18 1913 -1921
Roberts J.L., Lauritsen J.P., Cooney M., Parrott R.E., Sajaroff E.O., Win C.M., Keller M.D., Carpenter J.H., Carabana J., Krangel M.S., Sarzotti M., Zhong X.P., Wiest D.L., and Buckley R.H. T-B+NK+ severe combined immunodeficiency caused by complete deficiency of the CD3zeta subunit of the T-cell antigen receptor complex Blood. 2007 109 8 3198 -3206
Roifman C.M. Studies of patients’ thymi aid in the discovery and characterization of immunodeficiency in humans Immunol. Rev. 2005 203 1 143 -155
Soudais C., de Villartay J.P., Le Deist F., Fischer A., and Lisowska-Grospierre B. Independent mutations of the human CD3-epsilon gene resulting in a T cell receptor/CD3 complex immunodeficiency Nat. Genet. 1993 3 1 77 -81
Zapata D.A., Schamel W.W., Torres P.S., Alarcon B., Rossi N.E., Navarro M.N., Toribio M.L., and Regueiro J.R. Biochemical differences in the alphabeta T cell receptor.CD3 surface complex between CD8+ and CD4+ human mature T lymphocytes J. Biol. Chem. 2004 279 23 24485 -24492
Chaim Roifman, MD, FRCP, FCACB
Editor-in-Chief

Information & Authors

Information

Published In

cover image LymphoSign Journal
LymphoSign Journal
Volume 2Number 1March 2015
Pages: 1 - 2

History

Accepted manuscript online: 3 February 2015

Authors

Affiliations

Chaim Roifman MD, FRCP, FCACB [email protected]

Metrics & Citations

Metrics

Other Metrics

Citations

Cite As

Export Citations

If you have the appropriate software installed, you can download article citation data to the citation manager of your choice. Simply select your manager software from the list below and click Download.

There are no citations for this item

View Options

View options

PDF

View PDF

Login options

Check if you access through your login credentials or your institution to get full access on this article.

Subscribe

Click on the button below to subscribe to LymphoSign Journal

Purchase options

Purchase this article to get full access to it.

Restore your content access

Enter your email address to restore your content access:

Note: This functionality works only for purchases done as a guest. If you already have an account, log in to access the content to which you are entitled.

Media

Media

Other

Tables

Share Options

Share

Share the article link

Share on social media