Depleted skeletal muscle mitochondrial DNA, hyperlactatemia, and decreased oxidative capacity in HIV‐infected patients on highly active antiretroviral therapy

Haugaard, Steen B.; Andersen, Ove; Pedersen, Steen B.; Dela, Flemming; Richelsen, Bjørn; Nielsen, Jens; Madsbad, Sten; Iversen, Johan

doi:10.1002/jmv.20410

Cited by 34 publications

(31 citation statements)

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“…Although most of these studies focussed on fat distribution and adipocyte function, it is reasonable to assume that mitochondrial liver function would also be improved by switching to a less toxic NRTI backbone. One year after ddrug switching, 13 C-exhalation had recovered and almost…”

Section: Discussionmentioning

confidence: 99%

“…MeBT measurements were performed at the time of diagnosis and also 12, 24 and 48 weeks later. 13 C-exhalation was dramatically decreased at the diagnosis of acute HCV infection compared with baseline (cPDR 1.5h 1.572 and 1.146 compared with 4.813 and 6.985, respectively, at baseline). Both patients showed spontaneous viral elimination within 12 weeks without specific treatment.…”

Section: Effect Of Acute Hcv Infection On Hepatic Mitochondrial Functionmentioning

confidence: 93%

“…Briefly, each patient received 2 mg/kg body weight [methyl- C isotope ratio of the breath samples were analysed by nondispersive isotope selective infrared spectroscopy (IRIS; Wagner Analysen Technik, Bremen, Germany). To measure the proportion of metabolized substrate, the results were expressed as cumulative percentage dose of 13 C recovered (cPDR 1.5h ) after a test time of 90 min. Additional biochemical evaluations included HIV viral load, CD4 cell count, alanine aminotransferase (ALT) levels and serological testing for HCV or hepatitis B virus (HBV) coinfection.…”

Section: Mebt Biochemical Parameters and Virological Markersmentioning

confidence: 99%

“…Mitochondrial toxicity plays a major role in the pathogenesis of fatty liver disease irrespective of the specific trigger, and subclinical changes in mitochondrial integrity may precede the common phenotype of steatosis/ steatohepatitis [6,7]. The 13 C-methionine breath test (MeBT) is a noninvasive diagnostic instrument for assessment of hepatic mitochondrial function in vivo [8]. Our previously published study examined metabolically well-characterized HIV-infected patients receiving different treatment modalities [9].…”

Section: Introductionmentioning

confidence: 99%

“…For the first time we have demonstrated a significant negative association between HIV viral load and breath test performance in naïve patients as well as a time-dependent decrease in 13 C-exhalation within a group of ARTexperienced patients with STI at baseline and follow-up. It is widely accepted that HIV itself can have toxic effects on mitochondrial function in lymphocytes and probably other tissues by creating a proinflammatory/proapoptotic environment, although the precise mechanisms underpinning this are not clear [11][12][13][14].Most of the patients with d4T-or ddI-containing regimens at baseline breath test measurement (MeBT1) later switched therapies for less toxic NRTIs (tenofovir or abacavir) for the purpose of preventing or reversing lipoatrophy. Several recent studies have confirmed the metabolically beneficial effects of d4T switching [15][16][17].…”

mentioning

confidence: 99%

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Impact of antiretroviral treatment on 13C-methionine metabolism as a marker of hepatic mitochondrial function: a longitudinal study

et al. 2010

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ObjectivesUncontrolled viral replication and antiretroviral treatment (ART) may independently contribute to hepatic mitochondrial toxicity. The present study was designed to explore the longitudinal effects of treatment modifications on hepatic mitochondrial function by means of noninvasive 13 C-methionine breath test (MeBT) diagnostics. MethodsA total of 113 HIV-infected patients underwent two consecutive MeBTs over an interval of 11.8 AE 3.5 months. Forty-nine patients remained on stable ART or no therapy; 28 participants switched ART; 27 patients (re)initiated ART, and nine individuals underwent a structured treatment interruption (STI) of ART between MeBTs 1 and 2. Breath test results were expressed as cumulative percentage dose of 13 CO 2 recovered after 1.5 h test time (cPDR 1.5h ). ResultsInitiation of ART in treatment-naïve individuals and patients on STI was associated with a significant improvement of hepatic mitochondrial function (Po0.05). Cessation of ART or a prolonged delay in initiating therapy in treatment-naïve patients in turn led to a significant decline of 13 C-exhalation compared with baseline (Po0.05). A marked increase in 13 C-exhalation was observed in individuals who switched from stavudine or ddI to tenofovir or abacavir ( 1 170%; Po0.001), while no differences between MeBTs 1 and 2 were found in individuals on ART who had remained on stable regimens or in those who changed a protease inhibitor (PI) or nonnucleoside reverse transcriptase inhibitor (NNRTI) component. ConclusionThe present data suggest that hepatic mitochondrial function in HIV disease is a dynamic process with a high regenerative capacity and highlight the pathogenic relevance of HIV replication. Our findings suggest that modern ART per se does not negatively impact hepatic mitochondrial function. Keywords:13 C-methionine breath test, drug toxicity, HIV, mitochondrial toxicity IntroductionIncreasingly, deaths among HIV-infected persons are caused by hepatic complications [1,2]. Indeed, the majority of liver-related morbidity within the D:A:D cohort has been attributed to viral hepatitis coinfection. In the next few decades, a shift of morbidity to metabolic liver diseases is likely, analogous to the rising prevalence of the metabolic syndrome within the HIV-negative population [3]. The putative pathogenic role of antiretroviral therapy (ART) in this context is contested. Although the introduction of combination ART (cART) has reduced overall hepatic morbidity in both HIV-monoinfected and HIV/hepatitis C virus (HCV)-coinfected individuals, data on the long-term hepatotoxic effects of ART are absent. Two recently published cross-sectional trials showed a prevalence of DOI: 10.1111/j.1468-1293.2010.00847.x HIV Medicine (2011 r 2010 British HIV Association 40 nonalcoholic fatty liver disease in HIV-monoinfected patients of about 30%, which seems to be higher than calculated for the age-adjusted HIV-negative population [4,5]. Mitochondrial toxicity plays a major role in the pathogenesis of fatty liver disease irrespective...

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Section: Discussionmentioning

confidence: 99%

Section: Effect Of Acute Hcv Infection On Hepatic Mitochondrial Functionmentioning

confidence: 93%

Section: Mebt Biochemical Parameters and Virological Markersmentioning

confidence: 99%