Distinguishing infections<i>vs</i>flares in patients with systemic lupus erythematosus: Table 1

Ospina, Fabio E.; Echeverri, Alex; Zambrano, D.; Suso, Juan-Pablo; Martínez-Blanco, Javier; Cañas, Carlos A.; Tobón, Gabriel J.

doi:10.1093/rheumatology/kew340

Cited by 58 publications

(60 citation statements)

References 89 publications

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“…In our cohort, the CD8CD38 high T cell population was found expanded in patients with SLE who experienced a higher incidence of infections independently of disease activity. Previous reports have pointed to indicators of susceptibility to infections including serum levels of C reactive protein, procalcitonin (Ospina et al, 2017), T cell surface expression of CD64 (Feng et al, 2019), or deletion of Deltex1 (Leu et al, 2019), but they have fallen short in defining correctable molecular pathways.…”

Section: Discussionmentioning

confidence: 99%

The CD38/NAD/SIRTUIN1/EZH2 Axis Mitigates Cytotoxic CD8 T Cell Function and Identifies Patients with SLE Prone to Infections

et al. 2020

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Graphical Abstract Highlights d Expanded CD8CD38 high T cells in SLE patients identify patients with infections d CD8CD38 high T cells express decreased amounts of cytotoxic molecules d CD38 decreases NAD + and SIRT1 activity and releases the activity of EZH2 d Inhibition of EZH2 restores the degranulation capacity of CD8CD38 high T cells In Brief Katsuyama et al. find that an expanded CD8CD38 high T cell population in SLE patients is linked to infections. CD8CD38 high T cells display decreased cytotoxic capacity by suppressing the expression of related molecules through an NAD + /Sirtuin1/EZH2 pathway. EZH2 inhibitors increase cytotoxicity offering a means to mitigate infection rates in SLE. SUMMARYPatients with systemic lupus erythematosus (SLE) suffer frequent infections that account for significant morbidity and mortality. T cell cytotoxic responses are decreased in patients with SLE, yet the responsible molecular events are largely unknown. We find an expanded CD8CD38 high T cell subset in a subgroup of patients with increased rates of infections. CD8CD38 high T cells from healthy subjects and patients with SLE display decreased cytotoxic capacity, degranulation, and expression of granzymes A and B and perforin. The key cytotoxicity-related transcription factors T-bet, RUNX3, and EOMES are decreased in CD8CD38 high T cells. CD38 leads to increased acetylated EZH2 through inhibition of the deacetylase Sirtuin1. Acetylated EZH2 represses RUNX3 expression, whereas inhibition of EZH2 restores CD8 T cell cytotoxic responses. We propose that high levels of CD38 lead to decreased CD8 T cell-mediated cytotoxicity and increased propensity to infections in patients with SLE, a process that can be reversed pharmacologically.

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Section: Discussionmentioning

confidence: 99%

The CD38/NAD/SIRTUIN1/EZH2 Axis Mitigates Cytotoxic CD8 T Cell Function and Identifies Patients with SLE Prone to Infections

et al. 2020

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“…There have been a number of studies on the predictive biological markers of SLE ares, including antidouble-stranded DNA antibodies (anti-dsDNA Ab), the complement system, anti-extractable nuclear antigen antibodies (anti-ENA Ab), cytokines, and chemokines [12,13]. For the prediction of infection in SLE patients, conventional biomarkers (C-reactive protein [CRP], erythrocyte sedimentation rate (ESR), procalcitonin [PCT]) [14][15][16][17][18] and new markers have been developed [19]. Several recent studies have focused on markers for differentiating between disease are and infection in febrile SLE patients [20][21][22].…”

Section: Introductionmentioning

confidence: 99%

“…However, most physicians agreed that no single biomarker had su cient predictive value for both events [8,19]. The neutrophil-to-lymphocyte ratio (NLR) and platelet-to-lymphocyte ratio (PLR) were signi cantly higher in SLE patients compared with healthy controls and were positively correlated with SLEDAI score [23].…”

Section: Introductionmentioning

confidence: 99%

Differential Parameters between Activity Flare and Acute Infection in Pediatric Patients with Systemic Lupus Erythematosus

Luo

Yang

Lin

et al. 2020

Preprint

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Background: Systemic lupus erythematosus (SLE) is a systemic autoimmune disease. SLE patients are vulnerable to infections. Infections might mimic and even trigger SLE flares. To distinguish acute infection from activity flare always remains a clinical challenge.We aim to explore the approach to differentiate active infection from disease activity in pediatric SLE patients.Methods: Fifty pediatric SLE patients presenting with 185 clinical episodes were collected.The associations betweenrelevant data encompassing both clinical and laboratory parameters and the outcome groups were analyzed using generalized estimating equations (GEEs)facilitatingthe analysis of data collected in longitudinal and repeated-measures designs.We also used a multinomial logistic regression model for simultaneous prediction of different outcome groups. Finally, we ran the GLIMMIX procedure to track trends of changes in parameters over time.Results: These 185 episodes were divided into 4 outcome groups: infected-active (n=102), infected-inactive (n=11), noninfected-active (n=59), and noninfected-inactive (n=13) episodes. Multivariate GEE analysis showed that SDI, SLEDAI-2K, neutrophil‐to‐lymphocyte ratio (NLR), hemoglobin, platelet, RDW-to-platelet ratio (RPR), and C3 are predictive of flare (combined calculated AUC of 0.8964 and with sensitivity of 82.2 % and specificity of 90.9%). Multivariate GEE analysis showed that SDI, fever temperature, CRP, procalcitonin, lymphocyte percentage, NLR, hemoglobin, and renal score in SLEDAI-2k are predictive of infection (combinedcalculated AUC of 0.7886 and with sensitivity of 63.5% and specificity of 89.2%). We developed regression equations for simultaneous prediction of 4 different outcome groups.We could differentiate noninfected-active from infected-active episodes by different change patterns of ESR, NLR, lymphocyte, C3, and C4 over time.Conclusions: The proposed approach could differentiateflares from infections in pediatric SLE patients. Combination of parameters from four different domains simultaneously, including inflammation (CRP, ESR, PCT), hematology (Lymphocyte percentage, NLR, PLR), complement (C3, C4), and clinical status (SLEDAI, SDI), is effective to make appropriate judgement and treatment decisions.

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“…El 36,36% de estos pacientes con enfermedad activa presentaban concomitantemente un cuadro infeccioso. Al analizar la relación entre pacientes con puntaje alto de MEX-SLEDAI y VSG acelerada no se halló una relación estadísticamente (5,26) significativa como lo fue con complemento consumido y ANA positivo .…”

Section: Infecciones Frecuenciaunclassified

“…Las infecciones son consideradas causa importante de morbilidad y mortalidad en pacientes con (5) LES, reportándose dentro de las primeras dos causas de muerte más comunes en estos pacientes . Las (6) infecciones en LES son responsables del 40-50% de la morbilidad y mortalidad .…”

Section: Introductionunclassified

Causes of fever in adults patients of systemic lupus erythematosus

Saucedo

Taboada

Montiel

2017

Rev. virtual Soc. Parag. Med. Int

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RESUMENIntroducción: la fiebre que se presenta en un paciente con lupus eritematoso sistémico (LES) es muchas veces un desafío etiológico para el Internista, por lo que resulta trascendental establecer un correcto diagnóstico, ya que las conductas terapéuticas a adoptar son claramente diferentes. Objetivos: describir las causas de fiebre en pacientes con LES del Hospital Nacional y determinar la frecuencia de actividad lúpica según la escala MEX-SLEDAI. Metodología: estudio observacional, prospectivo, realizado en pacientes de ambos sexos mayores de edad, portadores con LES que acudieron por fiebre al Hospital Nacional (Itauguá, Paraguay) entre abril y noviembre de 2016. Resultados: se incluyeron 37 pacientes con edad media 30±11 años, con predomino del sexo femenino (89%). El tiempo medio de duración de la fiebre fue 8±5 días y las causas de la misma fueron: infecciones (43%), reactivación (35%) y ambas causas (22%). Los focos principales de infección fueron pulmonar, piel y partes blandas. La media de puntajes de la escala MEX-SLEDAI fue 8±5 puntos. Los pacientes con esta escala en valores altos se caracterizaron por ANA elevado y complementos disminuidos. Conclusiones: la causa de fiebre más frecuente en pacientes con LES fue la infección. La media de puntajes de la escala MEX-SLEDAI fue 8±5 puntos.Palabras claves: lupus eritematoso sistémico, fiebre, infección ABSTRACT Introduction: Fever seen in patients with systemic lupus erythematosus (SLE) is often an etiologic challenge for the internist. It is fundamental to make a correct diagnosis because the therapeutic choices are clearly different. Objectives: To describe the causes of fever in patients with SLE of the National Hospital and determine the frequency of the lupus activity according to the MEX-SLEDAI. Rev. virtual Soc. Parag. Med. Int. marzo 2017; 4 (1):35-45 Doi:10.18004/rvspmi/ 2017 4 (1):35-45 Doi:10.18004/rvspmi/ .04(01)35-045 2312 Methodology: This was an observational prospective study carried out in male and female adult patients with SLE that attended the National Hospital (Itauguá, Paraguay) for fever between April and November, 2016. Results: Thirty seven patients were included, they had a mean age of 30±11 years and there was a predominance of women (89%). The mean time of fever duration was 8±5 days and the causes were: infections (43%), reactivation (35%) and both causes (22%). The main infection foci were lung, skin and soft tissues. The mean score of MEX-SLEDAI was 8±5 points. The patients who had high values in this scale were characterized by high ANA and decreased complements. Conclusions:The most frequent cause of fever in patients with SLE was infection. The mean score in MEX-SLEDAI was 8±5 points.

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Distinguishing infectionsvsflares in patients with systemic lupus erythematosus: Table 1

Cited by 58 publications

References 89 publications

The CD38/NAD/SIRTUIN1/EZH2 Axis Mitigates Cytotoxic CD8 T Cell Function and Identifies Patients with SLE Prone to Infections

The CD38/NAD/SIRTUIN1/EZH2 Axis Mitigates Cytotoxic CD8 T Cell Function and Identifies Patients with SLE Prone to Infections

Differential Parameters between Activity Flare and Acute Infection in Pediatric Patients with Systemic Lupus Erythematosus

Causes of fever in adults patients of systemic lupus erythematosus

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