Benefits of Using CD45RA and CD28 to Investigate CD8 Subsets in Kidney Transplant Recipients

Yap, Michelle; Tilly, Gaëlle; Giral, Magali; Brouard, Sophie; Degauque, Nicolas

doi:10.1111/ajt.13581

Cited by 9 publications

(14 citation statements)

References 26 publications

(66 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…For a more granular analysis of the heterogeneous and functionally distinct memory and effector populations within CD3 + T cell compartment, we included additional conventional memory markers CD45RA and CCR7 (19, 25–27). Utilizing a gating strategy involving these four memory markers (Supplemental Figure 6) revealed belatacept resistant rejection was highly associated with elevated pre-transplant frequencies of CD28 + CD95 + CD45RA + CCR7 − CD8 T cells, so-called CD28 + CD8 + T EMRA (Figure 4c–d, P<0.0001).…”

Section: Resultsmentioning

confidence: 99%

“…The use of CD28 and CD95 is a standard approach for identifying na€ ıve (CD28 + CD95 À ), central memory (CD28 + CD95 + ), and effector/effector memory (CD28 À CD95 + ) T cells when phenotyping subsets in primates (21,22,25). For a more granular analysis of the heterogeneous and functionally distinct memory and effector populations within CD3 + T cell compartment, we included additional conventional memory markers CD45RA and CCR7 (19,(25)(26)(27). Utilizing a gating strategy involving these four memory markers ( Figure S6) revealed that belatacept-resistant rejection was highly associated with elevated pretransplant frequencies of CD28 + CD95 + CD45RA + CCR7 À CD8 T cells, so-called CD28 + CD8 + T EMRA ( Figure 4C Belatacept-and tacrolimus-based immunosuppression gave rise to two distinct study populations: those animals that were "susceptible" to therapy (gray lines) and those that were "resistant" to treatment (black lines).…”

Section: Elevated Frequency Of Cd28 + Cd8 + T Emra Is Associated Withmentioning

confidence: 99%

“…Classic models of memory classification define CD4 and CD8 T cells by CCR7 and CD45RA or by CD28 and CD95 (20)(21)(22). Multiparametric flow cytometry has revealed the phenotypic and functional heterogeneity of T cell subsets (23)(24)(25)(26)(27). These studies reveal functional differences between subsets defined by four or more phenotypic markers at a time, with a potentially critical transition marked by CD28 loss (28).…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Belatacept-Resistant Rejection Is Associated With CD28+ Memory CD8 T Cells

Mathews

Wakwe

Kim

et al. 2017

American Journal of Transplantation

View full text Add to dashboard Cite

Recently newer therapies have been designed to more specifically target rejection in an effort to improve efficacy and limit unwanted toxicity. Belatacept, a CD28-CD80/86 specific reagent is associated with superior patient survival and graft function than traditional therapy but its adoption as a mainstay immunosuppressive therapy has been tempered by increased rejection rates. It is essential that the underlying mechanisms associated with this rejection be elucidated before belatacept is more widely employed. To that end we designed a study in a non-human primate kidney transplant model where animals were treated with either a belatacept- or a tacrolimus-based immunosuppressive regimen. Interestingly we found that elevated pre-transplant frequencies of CD28+CD8+TEMRA cells are associated with rejection on belatacept but not tacrolimus treatment. Further analysis showed that the CD28+CD8+TEMRA cells rapidly lose CD28 expression after transplant in those animals that go on to reject with the allograft infiltrate being predominantly CD28−. These data suggest that CD28+ memory T cells may be resistant to belatacept, capable of further differentiation including loss of CD28 expression while maintaining effector function. The unique signaling requirements of CD28+ memory T cells provide opportunities for the development of targeted therapies, which may synergize with belatacept to prevent costimulation independent rejection.

show abstract

Section: Resultsmentioning

confidence: 99%

Section: Elevated Frequency Of Cd28 + Cd8 + T Emra Is Associated Withmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Belatacept-Resistant Rejection Is Associated With CD28+ Memory CD8 T Cells

Mathews

Wakwe

Kim

et al. 2017

American Journal of Transplantation

View full text Add to dashboard Cite

show abstract

“…Given the low expression of costimulatory molecules CD28 and CD27 by TEMRA CD8 T cells (25), we hypothesize that the effector functions of TEMRA CD8 T cells are triggered by pro-inflammatory cytokines such as IL-15, which are expressed and transpresented by conventional dendritic cells and macrophages (26, 27). Of note, CD45RA and CD28 markers were used to identify NAÏVE (CD45RA + CD28 + ), EM (CD45RA − CD28 + ), and TEMRA (CD45RA + CD28 − ) CD8 subsets (Figure S1 in Supplementary Material) (25). Stimulation with plate-bound anti-CD3 and IL-15 results in the upregulation of the activation marker CD25 and early proliferation marker CD69 by TEMRA CD8 from KT recipients (mean ± SEM 79.0 ± 5.4 and 67.8 ± 4.6%, respectively; p < 0.0001 vs. no stimulation; Figure 1A).…”

Section: Resultsmentioning

confidence: 99%

“…IL-15 favors the migration of memory CD8 T cells toward inflamed tissues (11) and supports the proliferation and the survival of CCR7 − memory CD8 T cell pool (30). The CCR7 − memory CD8 include EM and TEMRA with a heterogeneous frequency across HV and in patients with strong immune stimulation such as kidney transplantation (25). By investigating the reactivity of TEMRA and EM CD8 and by characterizing their metabolic profiles, we aimed to assess whether TEMRA and EM CD8 respond in similar manner to IL-15 stimulation.…”

Section: Discussionmentioning

confidence: 99%

IL-15 Harnesses Pro-inflammatory Function of TEMRA CD8 in Kidney-Transplant Recipients

et al. 2017

View full text Add to dashboard Cite

The involvement of TEMRA CD8 is evident in a large array of immunological conditions ranging from auto- to allo-immunity. Nevertheless, the factors leading to their accumulation and activation remain ill-defined and, efficient therapeutics to control their inflammatory response is lacking. Here, we show that IL-15-stimulated TEMRA from kidney-transplant (KT) recipients promote inflammation by inducing the expression of CX3CL1 by endothelial cells in an IFN-γ- and TNF-α-dependent manner. The responsiveness of TEMRA to IL-15 is not restricted to chronic stimulation, as TEMRA from healthy volunteers respond earlier and faster when compared to effector memory (EM). IL-15 induces antiapoptotic signals and promotes proliferation dependent of PI3K/Akt, MAPK, and ERK pathways. Without ex vivo stimulation, TEMRA cells are metabolically more active than naive and EM, as shown by their high ATP reservoir and a high expression of genes involved in glycolysis, glutaminolysis, and the Pentose Phosphate Pathway. Upon stimulation, TEMRA adapt their metabolism by sustaining an increased mitochondrial respiration and glycolysis. Finally, we show that the inhibition of glycolysis is highly effective in preventing endothelial inflammation induced by TEMRA from KT recipients. Together, our findings highlight the metabolic fitness that tightly regulates the immune function of TEMRA in physiological and pathogenic situations.

show abstract

Impact of Immune Cells on Stroke Limited to Specific Subtypes: Evidence from Mendelian Randomization Study

Chen,

Liu,

et al. 2024

Neurol Ther

View full text Add to dashboard Cite

Introduction Stroke is one of the common diseases that pose a severe threat to human health, with immune cells playing a crucial role in its onset and recovery. However, the specific mechanisms and causal relationships of different immune cell groups in various clinical stroke subtypes are unclear. This study explored the causal relationship between immune cells and stroke and its subtypes using Mendelian randomization (MR) analysis. Methods Data from genome-wide association studies were analyzed using inverse-variance weighted (IVW), MR-Egger, and weighted median methods for MR analysis, along with heterogeneity tests, sensitivity analysis, and pleiotropy analysis. Results CD45RA + CD28 − CD8 + T cell %T cell (OR 1.002, 95% CI 1.001–1.003; P FDR = 0.02), CD27 on CD24 + CD27 + B cell (OR 1.127, 95% CI 1.061–1.198; P FDR = 0.04), CD27 on IgD − CD38 dim B cell (OR 1.138, 95% CI 1.076–1.203; P FDR = 0.005), and CD27 on switched memory B cell (OR 1.144, 95% CI 1.076–1.216; P FDR = 0.01) were found to increase the risk of large artery stroke. Switched memory B cell %lymphocyte (OR 1.206, 95% CI 1.103–1.318; P FDR = 0.02) increased the risk of small vessel stroke. Reverse MR analysis did not reveal any reverse causal associations. Furthermore, by substituting the outcome data, a secondary MR analysis was conducted to validate the primary findings. Conclusion Our study reveals several causal links between immune phenotypes and stroke and its different subtypes, highlighting the complex interactions between the immune system and stroke. These findings provide new directions for further uncovering the biological basis of stroke and assist in advancing research on early interventions and treatment strategies. Supplementary Information The online version contains supplementary material available at 10.1007/s40120-024-00592-y.

show abstract

Benefits of Using CD45RA and CD28 to Investigate CD8 Subsets in Kidney Transplant Recipients

Cited by 9 publications

References 26 publications

Belatacept-Resistant Rejection Is Associated With CD28+ Memory CD8 T Cells

Belatacept-Resistant Rejection Is Associated With CD28+ Memory CD8 T Cells

IL-15 Harnesses Pro-inflammatory Function of TEMRA CD8 in Kidney-Transplant Recipients

Impact of Immune Cells on Stroke Limited to Specific Subtypes: Evidence from Mendelian Randomization Study

Contact Info

Product

Resources

About