High prevalence of thymic tissue in adults with human immunodeficiency virus-1 infection.

McCune, Joseph M.; Loftus, Richard A; Schmidt, David J.; Carroll, P. B.; Webster, David; Swor-Yim, L B; Francis, Isaac R.; Gross, Barry H.; Grant, Robert M.

doi:10.1172/jci2834

Cited by 244 publications

(160 citation statements)

References 53 publications

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“…Using this approach, McCunne et al . [10] found abundant thymic tissue measured by a CT slice in half of the untreated adult HIV-1 infected patients over 39 years old. This same group observed that the evolution of naïve T-cells during the follow up was associated with larger thymuses at the end of the treatment period [11].…”

Section: Introductionmentioning

confidence: 90%

Changes in thymus volume in adult HIV-infected patients under HAART: correlation with the T-cell repopulation

Rubio

Martı́nez-Moya

Leal

et al. 2002

Clinical and Experimental Immunology

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SUMMARYAn important thymus role has been suggested in T-cell repopulation after HAART in adult HIV-1 infected patients. Thymus volume increase after treatment has been described in HIV-1 infected children but not in adult patients. The objective of this work was to evaluate the effect of HAART on the thymic volume of adult HIV-1 infected patients and its relation with the T-cell repopulation. Twenty-one adult patients following 24 weeks under HAART were included in the study. All patients underwent a thoracic computed tomography (CT) evaluation for the measurement of thymic volumes at weeks 0, 12 and 24.Baseline thymus volume showed a significant correlation with the patient's age. Thymic volume significantly increased after 24 weeks of HAART. Besides, a significant correlation between changes in the thymus volume and changes in both total and naïve CD4+ cell counts was found. Only patients with increases ≥ 100 CD4+ cell counts after treatment significantly increased the thymic volume.These data show the first evidence of an early change in thymic volume of adult HIV-1 infected patients under HAART. This increase was related to the rise of both total and naïve CD4+ cell counts suggesting a functional role of thymic volume increase.

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Section: Introductionmentioning

confidence: 90%

Changes in thymus volume in adult HIV-infected patients under HAART: correlation with the T-cell repopulation

Rubio

Martı́nez-Moya

Leal

et al. 2002

Clinical and Experimental Immunology

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“…This is the "limited renewal" scenario. 8,10,11,16,35,44 The two scenarios differ in the mechanism for disease progression, and in the relevance of therapies aiming at immune reconstitution. In the limited renewal scenario disease progression is due to insufficient production in the CD4 1 T cell com partment, whereas in the proliferative exhaustion scenario it is the highly stressed homeostatic response that causes the regenerative capacity to ultimately, and irreversibly, burn out.…”

Section: Normal Telomere Lengths In Hiv-1 Infectionmentioning

confidence: 99%

Normal Telomere Lengths in Naive and Memory CD4+ T Cells in HIV Type 1 Infection: A Mathematical Interpretation

Wolthers¹,

Noest²,

Otto³

et al. 1999

AIDS Research and Human Retroviruses

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“…The interest in human thymic function in the elderly has increased after studies showed that (1) the adult thymus of HIV-infected patients without treatment (McCune et al 1998) or under highly active antiretroviral therapy (HAART) (Franco et al 2002;De la Rosa and Leal 2003) maintained or even improved its function, actively contributing to the CD4 lymphocyte repopulation; (2) adult thymopoiesis can be increased with growth hormone administration (Goldberg et al 2007) or pharmacological androgenic blockade (Sutherland et al 2005;Goldberg et al 2007b). Therefore, the capacity of effectively reversing, at least partially, the thymic atrophy opens up new perspectives in order to delay the immunosenescence process.…”

Section: Introductionmentioning

confidence: 99%

Thymopoiesis in elderly human is associated with systemic inflammatory status

Ferrando‐Martínez

Franco

Hernández

et al. 2009

AGE

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Immunosenescence studies of age-related immune system damage focused on clinical lymphopenic situations or androgenic blockade have revealed new insights about adult human immune reconstitution. However, as far as we know, the extent of lymphopoiesis in the thymus of elderly humans remains unclear. To this effect, we have analyzed 65 adult human thymuses (from 36 to 81 years; median age 68.6 years) obtained from patients who underwent cardiac surgery. Our results show a correlation between CD4 + CD8 + double-positive (DP) cells and both the age (inverse) and percentage (direct) of peripheral naive T cells, indicating that the thymus is still able to affect the peripheral lymphocyte pool even in the elderly. We also found significant correlation between the degree of thymopoiesis and the inflammation markers, as shown by the inverse correlations between DP and the percentage of neutrophils and IL-6 levels and the percentage of peripheral lymphocytes. Furthermore, in a multivariate linear regression the percentage of DP and IL-7 levels, but not age, were independently associated with the percentage of neutrophils. In conclusion, the thymus maintains, even in the elderly, an active thymopoiesis that rejuvenates the peripheral naive T-cell pool. Moreover, age-related thymopoietic decay is associated with the peripheral inflammation markers.

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High prevalence of thymic tissue in adults with human immunodeficiency virus-1 infection.

Cited by 244 publications

References 53 publications

Changes in thymus volume in adult HIV-infected patients under HAART: correlation with the T-cell repopulation

Changes in thymus volume in adult HIV-infected patients under HAART: correlation with the T-cell repopulation

Normal Telomere Lengths in Naive and Memory CD4+ T Cells in HIV Type 1 Infection: A Mathematical Interpretation

Thymopoiesis in elderly human is associated with systemic inflammatory status

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