Cytomegalovirus infection in HIV-infected and uninfected individuals is characterized by circulating regulatory T cells of unconstrained antigenic specificity

被引:9
作者
Tovar-Salazar, Adriana [1 ]
Weinberg, Adriana [1 ]
机构
[1] Univ Colorado Denver, Anschutz Med Ctr, Sch Med, Aurora, CO 80045 USA
关键词
IMMUNODEFICIENCY VIRUS-INFECTION; ACTIVE ANTIRETROVIRAL THERAPY; PERSISTENT VIRUS; CUTTING EDGE; IN-VITRO; RISK; DISEASE; CD4(+); AIDS; CMV;
D O I
10.1371/journal.pone.0180691
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Cytomegalovirus (CMV) infection is associated with immune-suppression in immune-compromised hosts and old adults. We previously showed that ex vivo CMV restimulation of peripheral blood mononuclear cells (PBMC) of CMV-seropositive volunteers expanded CD4+CD27-CD28-regulatory T cells (Tregs). Here we evaluate the phenotype and function of circulating CD4+CD27-CD28-T cells of CMV-seropositive adults. Compared with CMV-seronegative, CMV-seropositive adults had 10-fold higher CD4+CD27-CD28-% T cells in PBMC. Circulating CD4+CD27-CD28-T cells from both CMV-seropositive and seronegative donors expressed higher levels of TGF beta, granzyme B, CD39, CD147 and IL-35, and lower levels of CD127, compared with their parent circulating CD4+T cells. However, only CMV-seropositive circulating CD4+CD27-CD28-had increased FOXP3 expression. CD4+CD27-CD28-sorted from the PBMC of CMV-seropositive donors expanded ex vivo in the presence of rhIL2 and inhibited ex vivo proliferation of autologous PBMC restimulated with CMV, varicella-zoster virus or C. albicans antigens. CD4+CD27CD28- sorted from CMV-seronegative PBMC did not expand in the presence of rhIL2 and did not inhibit autologous PBMC proliferation. CD3+CD27-CD28-circulating T cells (>= 80% CD8+) from CMV-seropositive HIV-infected donors also inhibited ex vivo proliferation of autologous PBMC restimulated with CMV or HIV. These data indicate that CMVseropositive individuals have circulating Tregs that inhibit cell-mediated immune responses to CMV and other antigens and may be contribute to an immune-suppressive effect of CMV infection. Moreover, the phenotypic similarity between circulating CD4 +CD27-CD28-Tregs with differentiated effector T cells suggests that the two T-cell subsets might evolve in parallel or in sequence from the same progenitor cells in response to CMV stimulation during reactivations.
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