Michail Tzanakakis scite author profile

The treatment of lupus nephritis has seen significant advances during the past decade mainly due to the publication of well-designed randomized clinical trials (RCTs). The choice of treatment is guided by the histopathologic classification but is also influenced by demographic, clinical, and laboratory characteristics that allow for the identification of patients at risk for more aggressive disease. For the induction arm, low-dose cyclophosphamide regimens and mycophenolate mofetil have been validated as alternatives to the established National Institutes of Health regimen of high-dose cyclophosphamide; for the maintenance phase, azathioprine and mycophenolate compete for treatment of first choice. Rituximab is efficacious in real-life clinical practice but ineffective in clinical trials. The role of recently approved belimumab in lupus nephritis eagerly awaits further documentation. Aggressive management of comorbid conditions, such as hypertension and dyslipidemia, is of utmost importance. Here, we review the latest advances in lupus nephritis therapy with a focus on recent RCTs as well as new biologic agents under development. Furthermore, we propose a therapeutic algorithm in an effort to facilitate clinical decision-making in this gradually changing landscape. Upcoming European and American recommendations should provide further clarification.

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Recent progress in the treatment of lupus nephritis

Fanouriakis

¹

,

Krasoudaki

²

,

Tzanakakis

³

et al. 2012

Modern Rheumatology

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The treatment of lupus nephritis has seen significant advances during the past decade mainly due to the publication of well-designed randomized clinical trials (RCTs). The choice of treatment is guided by the histopathologic classification but is also influenced by demographic, clinical, and laboratory characteristics that allow for the identification of patients at risk for more aggressive disease. For the induction arm, low-dose cyclophosphamide regimens and mycophenolate mofetil have been validated as alternatives to the established National Institutes of Health regimen of high-dose cyclophosphamide; for the maintenance phase, azathioprine and mycophenolate compete for treatment of first choice. Rituximab is efficacious in real-life clinical practice but ineffective in clinical trials. The role of recently approved belimumab in lupus nephritis eagerly awaits further documentation. Aggressive management of comorbid conditions, such as hypertension and dyslipidemia, is of utmost importance. Here, we review the latest advances in lupus nephritis therapy with a focus on recent RCTs as well as new biologic agents under development. Furthermore, we propose a therapeutic algorithm in an effort to facilitate clinical decision-making in this gradually changing landscape. Upcoming European and American recommendations should provide further clarification.

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What’s new in clinical trials in lupus?

Ntali¹,

Tzanakakis²,

Βertsias³

et al. 2009

International Journal of Clinical Rheumatology

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Mo1034phosphate Equivalent (Peq) Education System: An Efficient Self-Adjustment Phosphate Binder Dosage Tool in Dialysis Patients

Xydakis

¹

,

Antonaki

²

,

Papadaki

³

et al. 2021

0

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Background and Aims Hyperphosphatemia is common in end-stage renal disease (ESRD) because of impaired renal phosphate excretion and is treated by dietary measures, dialysis techniques and the use of phosphate binder medication. It is one of the most important cardiovascular risk factors for dialysis patients. Our goal was to involve dialysis patients in the achievement of phosphate targets by self-adjusting the dose of Phosphate Binders (PB) on a meal-to-meal basis, according to the individual dietary P intake Method We conducted an interventional prospective single-arm study with a pre-post design. The inclusion criteria were patients with ESRD who had been receiving dialysis for more than three months, with dialysis schedule for four hours per session, three times per week, and who were older than 18 years of age. The primary endpoints of the study were the number of patients who reached the goal of serum phosphate before and after the training program and the weekly mean serum phosphate levels evaluated after the intervention period and compare them with the pre-intervention baseline levels. The secondary end-point was the burden of PB daily. All patients were trained in a self-administer PB program. A self-adjusted PB dose card was developed based on the phosphate food content list published by the National Technical University of Athens. The aim was to allow patients to immediately calculate the iP content of any food they consume easily. Phosphate Equivalent (PEQ) was defined as the weight of phosphorus having the same phosphate impact as a given weight of food. One PEQ corresponded in 100 mg of inorganic phosphorous and to one tablet of PB (one tablet of 800 mg of sevelamer). After 4 weeks (weeks 1-4) of washout from previous phosphate binders, eligible patients with serum phosphorus concentrations ≥ 6 mg/dl were included in the study. All patients received standard dietary phosphate counseling and a fixed dosing regimen of sevelamer PB was prescribed according to KDIGO and dialysis unit protocols for eight weeks (weeks 5-12 – pre-intervention period) In the 13th week, patients were asked to practice the self-administer PB program for eight more weeks. Results A total of 97 patients were screened for the study. 21 patients were excluded. 74 patients completed the study. The percentage of patients with uncontrolled phosphate levels reduced from 56.76% (42 out of 74) to 36.48 % (27 out of 74) in the post-intervention period. Of 9 patients who initially had a serum phosphorus level ≥9 mg/dl, 8 were reverted to phosphorus levels < 6 mg/dl at the end of the PEQ intervention period. There was a significant reduction of phosphate levels (prePEQ 7.42 ± 1.43 mg/dl vs. postPEQ 5.59 ± 1.82 mg/dL, p=0.036) and Ca × P levels (prePEQ: 67.1 ± 11.5 mg2/dL2; postPEQ: 51.9 ± 13.4 mg2/dL2, p=0.021) after patient education. There was a non-significant increase on serum calcium (pre PEQ: 8.13 ± 1.18 mg/dL; post PEQ: 8.56 ± 0.83mg/dL, p=0.515) and iPTH (prePEQ: 411 ± 376 pg/mL; postPEQ: 381 ± 321 pg/mL,p=0.13) Conclusion Our work shows that providing the patients with a relatively simple tool about the use of phosphate binders as PEQ is, we had a positive effect on the dialysis patients’ knowledge about the use of PB, phosphate content of their meals, and increase their sense of the necessity of the treatment and it was proved more effective than the standard fixed dose method. Using the PEQ education system was rewarding in an additional 20% of the patients with previous uncontrolled hyperphosphatemia. The PEQ education system is an efficient self-adjustment phosphate binder dosage tool in dialysis patients in reducing the serum phosphate level in our hemodialysis patients.

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Mp112urinary Ngal and Risk for Progression in Iga Nephropathy Patients

Xidakis¹,

Antonaki²,

Tzanakakis³

et al. 2016

0

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Introduction and Aims: IgA Nephropathy is the most common glomerulonephritis throughout the world and one of the most common causes of renal failure through a slowly progressive renal injury process. Τubulointerstitial injury at kidney biopsy is a strong predictor of progression of IgA nephropathy. NGAL, a tubular biomarker is upregulated in the distal nephron following tubular damage and both serum and urine NGAL excretion is increased. The aim of this study is to investigate any association between serum and urinary levels of NGAL at the time of kidney biopsy for the prediction of renal progression in patients with IgAN. Methods: We included in our study 103 patients with biopsy-proven IgA glomerulonephritis and a median follow up period of 6.4±3.2 years. In all subjects, serum and urine samples at the time of kidney biopsy were preserved by freezing and serum and urine NGAL levels were measured at 69 patients-included in our study, using an enzyme-linked immunosorbent assay kit. The end-points were doubling in baseline serum creatinine and/or initiation of dialysis. Results: At baseline, M/F 42/27, age was 43.5±11.5 years, creatinine 1.17±0.64 mg/dl, proteinuria was 1128±1092 mg/24H, 78% of the patients had a baseline creatinine of ≤ 1.3 mg/dl, 57% had a proteinuria of <1000mg/24H. During follow up time, 8 patients (11%) have doubled serum creatinine and 5 of them (7%) started dialysis in a period of 5.1±4.2 years. pNGAL was associated with with age (r=0.413, p=0.0001), with eGFR (r=-0,311, p<0.001), 24H proteinuria (r=0.337, p<0.001). In a multivariate Cox proportional hazard analysis, 24H proteinuria > 1 gr (HR 5.196 ; 95% confidence interval) , hypertension (HR 6.744 ;95%CI) were independent predictors of adverse outcome. Serum NGAL, showed a 4-fold hazard to reach the outcome (HR=4.06, p=0.04) after adjusting for age, sex, presence of hypertension. Conclusions: Classical risk factors for progression of IgA nephropathy also apply to our own population. Additionally, serum NGAL appears to be associated with a worse outcome. Our data suggest that serum NGAL could play a role as an early biomarker in IgA nephropathy.

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