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. 2011 Jun;8(3):308-12.
doi: 10.1513/pats.201006-046WR.

Pathogenesis of HIV-associated pulmonary hypertension: potential role of HIV-1 Nef

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Pathogenesis of HIV-associated pulmonary hypertension: potential role of HIV-1 Nef

Sharilyn Almodovar et al. Proc Am Thorac Soc. 2011 Jun.

Abstract

Infection with HIV increases the risk for lung diseases, including noninfectious pulmonary hypertension (PH). HIV-associated PH (HIV-PH) is an important lung disease in HIV-infected persons who live longer with antiretrovirals. The early stages of HIV-PH may be overlooked by healthcare providers due to nonspecific symptoms, including progressive dyspnea and nonproductive cough. HIV-PH may be detected via chest radiographs, CT scans, or electrocardiograms, but Doppler echocardiography is the most useful screening test to identify candidates for right heart catheterization. HIV-PH has a poor prognosis with high mortality; improved biomarkers to identify earlier stages of PH would benefit clinical care. The HIV-PH mechanism remains unknown, but HIV proteins such as Tat and Nef may play a role. HIV-1 Nef is a broad-spectrum adaptor protein that may affect HIV-infected and uninfected pulmonary vascular cells. Studies in macaques suggest that Nef is important in HIV-PH pathogenesis because monkeys infected with a chimeric simian immunodeficiency virus (SIV) expressing HIV-nef (SHIVnef) alleles, but not monkeys infected with the native SIV, develop pulmonary vascular remodeling. Four consistent amino acid mutations arose spontaneously in Nef passaged in the monkeys. To translate these findings to humans, one research endeavor of the Lung HIV Study focuses on the identification of HIV nef mutations in HIV-infected individuals with PH compared with HIV-infected normotensive patients. We present some of the preliminary evidence. Ongoing longitudinal studies will establish the connection between Nef mutations and the propensity for HIV-PH.

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Figures

Figure 1.
Figure 1.
Sensitivity and specificity analyses for an HIV-PH diagnosis based on the number of Nef functional domains with mutations. Data were summarized with a receiver-operator characteristic (ROC) curve; overall discrimination was quantified with area under the curve (AUC). Amino acid residues at each position were analyzed per clone. ROC curve analyses revealed that patients with mutations in Nef were 12 times more likely to exhibit HIV-PH compared with those not having the mutations; AUC of 0.85 (95% confidence interval, 0.68–1.00; P = 0.014).

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