Reconstitution of γδ T cell repertoire diversity after human allogeneic hematopoietic cell transplantation and the role of peripheral expansion of mature T cell population in the graft

Hirokawa, Makoto; Horiuchi, Takahiro; Kawabata, Yoshinari; Kitabayashi, Atsushi; Miura, Asako

doi:10.1038/sj.bmt.1702478

Cited by 36 publications

(40 citation statements)

References 45 publications

(36 reference statements)

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“…47 The predominant mechanism of gd reconstitution seems to be peripheral expansion of donor gd clones, which can persist for more than 1.5 years after transplantation. 48 Unlike ab T cells, gd T cells can reconstitute via an alternative, thymusindependant pathway. 49,50 However, the precise regulatory and cytotoxic functions of gd T cells after transplantation are not fully understood, and further investigation is required to define the role and importance of gd T cells as potential targets for post transplantation immunotherapy.…”

Section: Discussionmentioning

confidence: 99%

A prospective comparison of immune reconstitution in pediatric recipients of positively selected CD34+ peripheral blood stem cells from unrelated donors vs recipients of unmanipulated bone marrow from related donors

Eyrich

Leiler

Lang

et al. 2003

Bone Marrow Transplant

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Summary:Positively selected CD34 + hematopoietic stem cells from unrelated donors (UD-HSCT) have been successfully transplanted, but little is known about immune reconstitution in this setting. Here we report a prospective comparison of immune reconstitution in recipients of UD-HSCT and of unmanipulated bone marrow from matched sibling donors (MSD-BMT). T-cell reconstitution occurred more than 100 days later in the UD-HSCT than in the MSD-BMT group. The first T cells after UD-HSCT were almost exclusively CD45RO + HLA-DR + , whereas early-emerging T cells after MSD-BMT more frequently expressed CD62L, CD28, and CD25. In both groups, numbers of CD45RA + naive T cells increased after 180 days. After UD-HSCT, the T-cell-receptor (TCR)-repertoire was severely skewed and showed significantly reduced diversity during the first year, but only minor abnormalities were seen after MSD-BMT. TCR-diversity increased simultaneously with the number of naive T cells. In both groups, we observed transient expansions of cd T cells. B cells were reconstituted more rapidly in UD-HSCT than in MSD-BMT recipients, whereas the rapidity of NK-cell reconstitution was similar in the two groups. In summary, T-cell reconstitution was slower after UD-HSCT than after MSD-BMT because of the delayed recovery of early memory-type T cells with reduced TCR-diversity, whereas naive T-, NK-, and B cells were reconstituted similarly in the two groups.

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Section: Discussionmentioning

confidence: 99%

A prospective comparison of immune reconstitution in pediatric recipients of positively selected CD34+ peripheral blood stem cells from unrelated donors vs recipients of unmanipulated bone marrow from related donors

Eyrich

Leiler

Lang

et al. 2003

Bone Marrow Transplant

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“…2,3 We also found that TCR usage appears to be limited, and that amino acid sequences frequently contain an arginine residue followed by acidic amino acid residues in the complementarity-determining region 3 (CDR3) of TCR-␤ chains containing BV24S1, suggesting that skewing of the TCRAV and TCRBV repertoires is antigen-driven. 1 These features of post-transplant T cell regeneration are similar to those during extrathymic differentiation of T cell progenitors and peripheral expansion of mature T cell populations, which have been demonstrated by murine bone marrow transplantation studies.…”

mentioning

confidence: 94%

“…The PCR products of the TCR-␤ chain were cloned into the PCR2.1 TA cloning vector (Invitrogen, Carlsbad, CA, USA) and sequenced using a Big-Dye Terminator Cycle Sequencing Kit (Perkin-Elmer Applied Biosystems) 3 and an Applied Biosystems 377A automated DNA sequencer.…”

Section: Sequencing Cdr3 Regions In Tcr-␤ Chainsmentioning

confidence: 99%

Extensive clonal expansion of T lymphocytes causes contracted diversity of complementarity-determining region 3 and skewed T cell receptor repertoires after allogeneic hematopoietic cell transplantation

Hirokawa

Matsutani

Horiuchi

et al. 2001

Bone Marrow Transplant

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Summary:We previously described skewed repertoires of the T cell receptor-␤ chain variable region (TCRBV) and the TCR-␣ chain variable region (TCRAV) soon after allogeneic hematopoietic cell transplantation. To determine the characteristics of skewed TCRBV after transplantation, we examined the clonality of T lymphocytes carrying skewed TCRBV subfamilies and determined the CDR3 sequences of expanded T cell clones. In all 11 recipients examined, TCR repertoires were skewed, with an increase of certain TCRBV subfamilies that differed among individuals. In nine of 11 patients, clonal/oligoclonal T cell expansion was observed, although the expanded T cells were not necessarily oligoclonal. The extent of expansion after transplantation appeared to predict clonality. The arginine (R)-X-X-glycine (G) sequence was identified in clonally expanded T cells from four of five recipients examined, and glutamic acid (E), aspartic acid (D) and alanine (A) were frequently inserted between R and G. These results suggest that T lymphocyte expansion may result from the response to antigens widely existing in humans, and that the extensive clonal expansion of a limited number of T cells leads to contracted CDR3 diversity and post-transplant skewed TCR repertoires. Bone Marrow Transplantation (2001) 27, 607-614. Keywords: T cell clonality; CDR3; allogeneic hematopoietic cell transplantationWe have found skewed TCRAV and TCRBV repertoires soon after allogeneic hematopoietic cell transplantation in virtually all tested recipients. 1 Furthermore, we demonstrated that reconstitution of the ␣␤ T cell, but not the ␥␦ T cell repertoire was incomplete for at least 2 months after transplantation, and that the delayed reconstitution of TCR repertoire diversity was more profound in immunocompro- mised hosts. 2,3 We also found that TCR usage appears to be limited, and that amino acid sequences frequently contain an arginine residue followed by acidic amino acid residues in the complementarity-determining region 3 (CDR3) of TCR-␤ chains containing BV24S1, suggesting that skewing of the TCRAV and TCRBV repertoires is antigen-driven. 1 These features of post-transplant T cell regeneration are similar to those during extrathymic differentiation of T cell progenitors and peripheral expansion of mature T cell populations, which have been demonstrated by murine bone marrow transplantation studies. 4 Extrathymic differentiation of T cell progeny in bone marrow generates TCR␥␦ ϩ and CD4 Ϫ CD8 Ϫ TCR␣␤ ϩ T cells. 5,6 Peripheral expansion of mature T lymphocytes is driven by the antigenic milieu of the host 7,8 and gives rise to substantial numbers of TCR␣␤ ϩ CD4 ϩ and TCR␣␤ ϩ CD8 ϩ T cells. 5,9 However, an infusion of a limited number of T cells into athymic mice results in skewed TCR repertoires. 5 Clonal expansion of T lymphocytes is the principal mechanism of antigen-specific immune responses. 10,11 The CDR3 regions of TCRBV and TCRAV make the principal contact with an antigenic peptide that is bound to the major histocompatibility complex (MHC) and the...

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“…Studies also reveal TCR gd T cells can be classified into Th1 cells and Th2 cells. In the different stages of respiratory allergic inflammation, different TCR gd T cells exert positive or negative regulatory effects on the immune function, and specific immunotherapy (SIT) can rectify the imbalance between T cell subsets (3)(4)(5)(6)(7)(8). The knowledge on TCR gd T cells is still insufficient as compared to TCR ab T cells, and few studies report the role of TCR gd T cells in allergic rhinitis (AR) and SIT.…”

Section: Introductionmentioning

confidence: 99%

“…Ten AR patients undergoing SIT with house-dust-mite extract for 1 year were recruited. Quanti tative analysis of immunofluorescence was performed to detect the serum specific IgE (sIgE) level before and after SIT; RT-PCR-genescan analysis was employed to detect the mRNA expressions of TCR Vg (I-III) and Vd (1)(2)(3)(4)(5)(6)(7)(8) in the peripheral mononuclear cells followed by analysis of T cell clonality. Real-time quantitative PCR was applied to detect the expressions of TCR Vg I-III genes.…”

mentioning

confidence: 99%

Effects of Immunotherapy on the Distribution and Clonality of TCR Vγ and Vδ Subfamily T Cells in Allergic Rhinitis Patients

Yang¹,

Li²,

Wu³

et al. 2012

Journal of Medical Biochemistry

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Summary: The aim of this study was to investigate the changes in the peripheral specific IgE level, distribution of TCR Vg and Vd subfamily T cells and mRNA expressions of TCR Vg I-III following specific immunotherapy (SIT) with house-dust-mite extract in allergic rhinitis (AR) patients. Ten AR patients undergoing SIT with house-dust-mite extract for 1 year were recruited. Quanti tative analysis of immunofluorescence was performed to detect the serum specific IgE (sIgE) level before and after SIT; RT-PCR-genescan analysis was employed to detect the mRNA expressions of TCR Vg (I-III) and Vd (1-8) in the peripheral mononuclear cells followed by analysis of T cell clonality. Real-time quantitative PCR was applied to detect the expressions of TCR Vg I-III genes. Ten healthy volunteers served as controls. For AR patients, SIT treatment could improve the symptoms, but the serum sIgE level was not markedly decreased. Before SIT, the expressions of TCR Vg I-III gene were similar between AR patients and controls (P>0.05) but markedly decreased after SIT in AR patients (P<0.05 in TCR VgI and VgII). The expressions of TCR Vd (1-8) before and after SIT were 5.3±0.82 and 4.9±0.57, respectively, and that in healthy controls was 5.2±1.40. Vd1, 2, 3 and 6 were the most common genes found in these patients. Significant difference in the TCR Vd6 subfamily T cells was found between the two groups. Polyclonal or biclonal proliferation was found in the T cells of patients before SIT and in healthy controls, but oligoclonal proliferation in only 1 subject before SIT. After SIT, the proportion of patients with oligoclonal proliferation of T cells (6/10) was markedly increased (P<0.05). SIT for 1 year could alter the expressions of TCR Vg I-III genes, the Kratak sadr`aj: Cilj ove studije bio je da se istra`e promene u nivou specifi~nog IgE u perifernoj krvi, distribuciji T }elija iz potporodice TCR Vg i Vd i ekspresiji TCR Vg I-III u mRNK posle specifi~ne imunoterapije (SIT) sa ekstraktom grinja iz ku}ne pra{ine kod pacijenata sa alergijskim rinitisom (AR). Uklju~eno je 10 pacijenata sa AR le~enih specifi~nom imunoterapijom sa ekstraktom grinja iz ku}ne pra{ine tokom 1 godine. Obavljena je kvantitativna analiza imunofluorescencijom kako bi se odredio nivo specifi~nog IgE (sIgE) u serumu pre i posle SIT; primenjena je RT-PCRgenescan analiza radi odre|ivanja ekspresije TCR Vg (I-III) i Vd (1-8) u mRNK u perifernim mononuklearnim }elijama posle ~ega je obavljena analiza klonalnosti T }elija. Kvantitativna PCR analiza u realnom vremenu sprovedena je kako bi se odredila ekspresija TCR Vg I-III gena. Deset zdravih dobrovoljaca slu`ilo je kao kontrolna grupa. Kod pacijenata sa AR, tretman SIT olak{ao je simptome, ali nivo sIgE u serumu nije se zna~ajno snizio. Pre SIT, ekspresija TCR Vg I-III gena bila je sli~na kod pacijenata sa AR i kontrolnih subjekata (P>0,05), ali se zna~ajno snizila posle SIT kod pacijenata sa AR (P>0,05 u TCR VgI i VgII). Ekspresija TCR Vd (1-8) pre i posle SIT bila je 5,3±0,82 i 4,9±0,57, a kod zdravih subjekata 5,2±1...

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Reconstitution of γδ T cell repertoire diversity after human allogeneic hematopoietic cell transplantation and the role of peripheral expansion of mature T cell population in the graft

Cited by 36 publications

References 45 publications

A prospective comparison of immune reconstitution in pediatric recipients of positively selected CD34+ peripheral blood stem cells from unrelated donors vs recipients of unmanipulated bone marrow from related donors

A prospective comparison of immune reconstitution in pediatric recipients of positively selected CD34+ peripheral blood stem cells from unrelated donors vs recipients of unmanipulated bone marrow from related donors

Extensive clonal expansion of T lymphocytes causes contracted diversity of complementarity-determining region 3 and skewed T cell receptor repertoires after allogeneic hematopoietic cell transplantation

Effects of Immunotherapy on the Distribution and Clonality of TCR Vγ and Vδ Subfamily T Cells in Allergic Rhinitis Patients

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