Objective

To characterize immune phenotype and thymic function in HIV-1-infected adults with excellent virologic and poor immunologic responses to highly active antiretroviral therapy (HAART).

Methods

Cross-sectional study of patients with CD4 T cell rises of≥ 200× 10 6 cells/l (CD4 responders; n= 10) or< 100× 10 6 cells/l (poor responders; n= 12) in the first year of therapy.

Results

Poor responders were older than CD4 responders (46 versus 38 years; P< 0.01) and, before HAART, had higher CD4 cell counts (170 versus 35× 10 6 cells/l; P= 0.11) and CD8 cell counts (780 versus 536× 10 6 cells/l; P= 0.02). After a median of 160 weeks of therapy, CD4 responders had more circulating naive phenotype (CD45+ CD62L+) CD4 cells (227 versus 44× 10 6 cells/l; P= 0.001) and naive phenotype CD8 cells (487 versus 174× 10 6 cells/l; P= 0.004) than did poor responders (after 130 weeks). Computed tomographic scans showed minimal thymic tissue in 11/12 poor responders and abundant tissue in 7/10 responders (P= 0.006). Poor responders had fewer CD4 cells containing T cell receptor excision circles (TREC) compared with CD4 responders (2.12 versus 27.5× 10 6 cells/l; P= 0.004) and had shorter telomeres in CD4 cells (3.8 versus 5.3 kb; P= 0.05). Metabolic labeling studies with deuterated glucose indicated that the lower frequency of TREC-containing lymphocytes in poor responders was not caused by accelerated proliferation kinetics.

Conclusion

Poor CD4 T cell increases observed in some patients with good virologic response to HAART may be caused by failure of thymic T cell production.