Profiling of Inflammatory Proteins in Plasma of HIV-1-Infected Children Receiving Antiretroviral Therapy

Lemma, Mahlet; Petkov, Stefan; Bekele, Yonas; Petros, Beyene; Howe, Rawleigh; Chiodi, Francesca

doi:10.3390/proteomes8030024

Cited by 9 publications

(14 citation statements)

References 41 publications

(45 reference statements)

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“…Another study using a cohort of PLHIV with dyslipidemia (n = 89) and HC (n = 46) also showed little overlap with our results, with only four inflammatory proteins (4E-BP1, ADA, TNFSF14, and CD40) overlapping with our results (FDR<0.05, same direction) ( deFilippi et al., 2020 ). Of note, a study using 43 children with HIV infection and matched controls showed 15 proteins being downregulated in children with HIV infection compared to HC (FDR<0.01), with none of the proteins being identified in a similar direction compared to our study ( Lemma et al., 2020 ). These differences between studies can be attributed to different cohort characteristics, especially the ethnicities, number of participants, proteins tested, and analysis strategies.…”

Section: Discussioncontrasting

confidence: 42%

“…Assessment of the profile of plasma inflammatory proteins allows the study of complex biological pathways that may lead to the identification of novel therapeutic targets and disease biomarkers. Previous studies that assessed plasma protein profiles were limited by small sample size and/or lack of a proper validation cohort ( Babu et al., 2019a , 2019b ; deFilippi et al., 2020 ; Lemma et al., 2020 ; Sperk et al., 2018 ; Vos et al., 2021 ). In addition, other studies included only patients with central obesity and insulin resistance using statins ( deFilippi et al., 2020 ) or children with HIV infection ( Lemma et al., 2020 ).…”

Section: Introductionmentioning

confidence: 99%

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Targeted plasma proteomics reveals upregulation of distinct inflammatory pathways in people living with HIV

et al. 2022

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Section: Discussioncontrasting

confidence: 42%

Section: Introductionmentioning

confidence: 99%

Targeted plasma proteomics reveals upregulation of distinct inflammatory pathways in people living with HIV

et al. 2022

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“…Lemma et al. ( 25 ) had the same finding in children. OSM is part of the IL-6 family and is active in multiple cell types where it influences cell differentiation and inflammation ( 37 ).…”

Section: Discussionmentioning

confidence: 58%

“…Lemma et al. ( 25 ) included 43 HIV-positive and 43-HIV negative children with a median age of 60 months from Ethiopia. They found in line with our findings, levels of OSM and TRANCE to be significantly lower in HIV-positive participants.…”

Section: Discussionmentioning

confidence: 99%

Patterns of Immune Activation in HIV and Non HIV Subjects and Its Relation to Cardiovascular Disease Risk

et al. 2021

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IntroductionInsight into inflammation patterns is needed to understand the pathophysiology of HIV and related cardiovascular disease (CVD). We assessed patterns of inflammation related to HIV infection and CVD risk assessed with carotid intima media thickness (CIMT).MethodsA cross-sectional study was performed in Johannesburg, South Africa, including participants with HIV who were virally suppressed on anti-retroviral therapy (ART) as well as HIV-negative participants who were family members or friends to the HIV-positive participants. Information was collected on CVD risk factors and CIMT. Inflammation was measured with the Olink panel ‘inflammation’, allowing to simultaneously assess 92 inflammation markers. Differences in inflammation patterns between HIV-positive and HIV-negative participants were explored using a principal component analysis (PCA) and ANCOVA. The impact of differentiating immune markers, as identified by ANCOVA, on CIMT was assessed using linear regression while adjusting for classic CVD risk factors.ResultsIn total, 185 HIV-positive and 104 HIV negative participants, 63% females, median age 40.7 years (IQR 35.4 – 47.7) were included. HIV-positive individuals were older (+6 years, p <0.01) and had a higher CIMT (p <0.01). No clear patterns of inflammation were identified by use of PCA. Following ANCOVA, nine immune markers differed significantly between HIV-positive and HIV-negative participants, including PDL1. PDL1 was independently associated with CIMT, but upon stratification this effect remained for HIV-negative individuals only.ConclusionHIV positive patients on stable ART and HIV negative controls had similar immune activation patterns. CVD risk in HIV-positive participants was mediated by inflammation markers included in this study.

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“…HIV-1 causes dysregulation of the innate immune system, persistent immune activation, dysfunction of the inflammatory response and immune system aging (senescence) early in HIV-1 infection. Successful ART ameliorates, but does not completely correct the major immune dysfunctions [ 2 , 3 , 4 , 5 , 6 ], substantial immunological impairment pertains even on the background of the successful ART [ 7 , 8 ] (for the latest review, see [ 9 ]). Hyper-immunoactivation and inflammation persisting in PLWH is recognized as a major cause of HIV-1 associated malignances.…”

Section: Introductionmentioning

confidence: 99%

Oncogenic Effects of HIV-1 Proteins, Mechanisms Behind

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Bayurova

Avdoshina

et al. 2021

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People living with human immunodeficiency virus (HIV-1) are at increased risk of developing cancer, such as Kaposi sarcoma (KS), non-Hodgkin lymphoma (NHL), cervical cancer, and other cancers associated with chronic viral infections. Traditionally, this is linked to HIV-1-induced immune suppression with depletion of CD4+ T-helper cells, exhaustion of lymphopoiesis and lymphocyte dysfunction. However, the long-term successful implementation of antiretroviral therapy (ART) with an early start did not preclude the oncological complications, implying that HIV-1 and its antigens are directly involved in carcinogenesis and may exert their effects on the background of restored immune system even when present at extremely low levels. Experimental data indicate that HIV-1 virions and single viral antigens can enter a wide variety of cells, including epithelial. This review is focused on the effects of five viral proteins: envelope protein gp120, accessory protein negative factor Nef, matrix protein p17, transactivator of transcription Tat and reverse transcriptase RT. Gp120, Nef, p17, Tat, and RT cause oxidative stress, can be released from HIV-1-infected cells and are oncogenic. All five are in a position to affect “innocent” bystander cells, specifically, to cause the propagation of (pre)existing malignant and malignant transformation of normal epithelial cells, giving grounds to the direct carcinogenic effects of HIV-1.

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Profiling of Inflammatory Proteins in Plasma of HIV-1-Infected Children Receiving Antiretroviral Therapy

Cited by 9 publications

References 41 publications

Targeted plasma proteomics reveals upregulation of distinct inflammatory pathways in people living with HIV

Targeted plasma proteomics reveals upregulation of distinct inflammatory pathways in people living with HIV

Patterns of Immune Activation in HIV and Non HIV Subjects and Its Relation to Cardiovascular Disease Risk

Oncogenic Effects of HIV-1 Proteins, Mechanisms Behind

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