Original Article

Idiopathic Nephrotic Syndrome in Childhood: A Retrospective Analysis of Two Hundred and Eighty Nine Patients

10.4274/haseki.46855

  • Kenan Yılmaz
  • Ruhan Düşünsel
  • İsmail Dursun
  • Sibel Yel
  • Zübeyde Gündüz
  • Hakan Poyrazoğlu

Received Date: 15.04.2017 Accepted Date: 09.11.2017 Med Bull Haseki 2017;55(4):280-285

Aim

In this study, we aimed to evaluate the demographic and histopathological characteristics and response to medications in children with idiopathic nephrotic syndrome in Turkey.

Methods

We reviewed medical records of patients older than one year, who were newly diagnosed with nephrotic syndrome and had been followed for at least one year in our department between November 1994 and March, 2013.

Results

A total of 289 children (169 boys) were included in the study. Fifty theree patients (18.4%) were with steroid-resistant nephrotic syndrome, 33 (11.4%) with frequently relapsing nephrotic syndrome and 53 (18.4%) were with steroid-dependent nephrotic syndrome. Cyclosporine A (CsA), cyclophosphamide, mycophenolate mofetil, levamisole, azathioprine, and rituximab were used as steroid-sparing agents in some patients. The number of patients who were responder to steroid and to CsA was similar. Majority of patients with steroid-resistant nephrotic syndrome were also resistant to mycophenolate mofetil and CsA.

Conclusion

There was a high prevalence of minimal change disease based on kidney biopsy especially in boys younger than six years of age and response to steroid and CsA was almost similar.

Keywords: Children,idiopathic nephrotic syndrome,steroid resistance,steroid dependent,relapse

Introduction

Nephrotic syndrome (NS) is characterized by massive proteinuria, generalized edema, hypoalbuminemia and hyperlipidemia. Idiopathic NS (INS) is the most common form of NS (>90%) with annual incidence of 1 to 3:100.000 in children below 16 years of age (1).

Although majority of children with INS are well responder for steroids, 20% of them are steroid-resistant. Therapeutic response to medications and long-term outcome of the disease may be different between the geographic regions (2). However, there are few studies on this topic. Thus, in this study, our aim was to evaluate the demographic and histopathological characteristics, and response to medications in children with INS in our center.


Methods

We reviewed medical records of children diagnosed with INS in the pediatric nephrology department at Erciyes University, between November 1994 and March 2013. Our study was conducted in accordance with the principles of the Helsinki Declaration. Ethics Committee of Erciyes University Medical Faculty approved the study (approval no: 2014/582). Inclusion criteria were; 1) At least one year of follow-up after diagnosis, and 2) ≥1 year of age at the time of diagnosis. Children with secondary NS were excluded. Patient`s charts were retrospectively reviewed in terms of demographic, histopathologic and clinical findings, and response to immunosuppressive treatment.

NS was defined as edema, proteinuria (≥40 mg/m2/hour) and hypoalbuminemia (serum albumin level <2.5 g/dL). The classifications of the patients based on steroid response were as follows (2):

  1. Complete remission: Urine protein creatinine ratio (uPCR) <200 mg/g or <1+ protein on a urine dipstick measurement for three consecutive days.
  2. Partial remission: Fifty percent or more decrease in proteinuria and uPCR between 200 and 2000 mg/g.
  3. No remission: Failure to reduce urine protein excretion by 50% from baseline or persistent excretion uPCR>2000 mg/g.
  4. Steroid-resistant NS (SRNS): Failure to achieve complete remission after eight weeks of corticosteroid therapy.
  5. Relapse: uPCR ≥2000 mg/g, or ≥300 mg/dL or 3+ protein on urine dipstick.
  6. Frequently relapsing NS (FRNS): Two or more relapses within six months of initial response, or four or more relapses in any 12-month period.
  7. Steroid-dependent NS (SDNS): Two consecutive relapses during corticosteroid therapy, or within 14 days of ceasing therapy.
  8. Early nonresponder: Failure to achieve complete remission after eight weeks of corticosteroid therapy.
  9. Late nonresponder: Persistent proteinuria during four or more weeks of corticosteroids following one or more remission.

Renal biopsy was routinely performed in patients with gross hematuria, persistent microscopic hematuria, increased serum creatinine, resistance to steroid, low serum complement and age at onset <1 y or >8 y. The biopsy specimens were examined by light and immunofluorescence microscopy. Steroid therapy was initiated at a dose of 60 mg/m2/day over four weeks, which then titrated to 60 mg/m2 on alternate days over an additional four weeks. The dose was then tapered over the next two-three months and discontinued. Alternative agents used in patients with SDNS, SRNS and FRNS were: cyclosporine A (CsA) 3-5 mg/kg/day, oral cyclophosphamide (CYC) 2 mg/kg/day (maximum cumulative dose: 168 mg/kg, 8-12 weeks), intravenous CYC500 mg/m2/month (3-6 months), mycophenolate mofetil (MMF) 600 mg/m2/dose (twice daily), pulse methylprednisolone 30 mg/kg (maximum: 1000 mg), levamisole 2-3 mg/kg/day, azathioprine 1-3 mg/kg/day, and rituximab 375 mg/m2.

CsA and MMF resistance were defined as failure to achieve partial or complete remission after six months of CsA and MMF treatment (2).


Statistical Analysis

Data were analyzed by using IBM SPSS version 21 software. The Shapiro-Wilk test was used to assess normality in numeric variables. The Mann-Whitney U test was used for comparison between groups with skewed distribution while the Kruskal-Wallis test was used for comparison among groups. Chi-square test was used for comparisons between categorical variables. A p value of less than 0.05 was considered statistically significant.


Results

A total of 289 children were included in the study. Of these, 169 (58.5%) were boys and 120 (41.5%) were girls. The mean age at the time of diagnosis was 40 months (range: 12-180 months). The mean follow-up time was 76 months (range: 12-204 months). On the first admission, there was oliguria in 134 (46.4%), hypertension in 54 (18.7%), massive edema in 47 (16.3%), microscopic hematuria in 39 (13.5%) and gross hematuria in two (0.7%) patients.

The number and mean age of the patients without relapse were 58 (20.1%) and 48 months (minimum-maximum: 165 months), respectively. 46.6% of them were girls. The boys less than 6 of age were more steroid resistant (51% in SRNS group). Only 29 patients (10%) had a glomerular filtration rate of <90 mL/min/1.73m2 at presentation. Of the patients 53 (18.4%) were with SRNS, 33 (11.4%) with FRNS and 53 (18.4%) were with SDNS. Kidney biopsy was performed in 72 patients; initial renal histology showed minimal change disease (MCD) in 43 patients (59.7%), focal segmental glomerulosclerosis (FSGS) in 12 (16.7%), mesangioproliferative glomerulonephritis in 8 (11.1%), membranoproliferative glomerulonephritis in 6 (8.3%) and membranous glomerulonephritis in 3 patients (4.2%). Ninety five patients (32.9%) required albumin replacement for effective intravascular volume. 37.2% of patients with MCD at the initial biopsy were steroid-resistant (Table 1). Similarly, majority of them were also resistant to MMF and CsA. The response rate to CYC in this group was approximately 50% (Table 2). The response rate to MMF and CYC in SRNS group was 36% and 54%, respectively. Majority of the children who were responder to steroid were also responder to CsA (86.6%) (p<0.01).

Rituximab therapy was given in two patients. Of them, one was steroid-dependent and the other one was steroid-resistant.

Eleven patients were treated with levamisole. Of them, only one responded to the therapy (Table 3).

The most common complications related to disease and medication were osteoporosis and hypertrichosis (Table 4). Of the patients with osteoporosis, 29 patients (54.7%) were in SRNS group, 16 patients (30.2%) in SDNS group and eight patients (15.1%) in FRSN group. Hypertension was detected in eight (61.5 %) patients with SRNS. Five of them had MCD based on kidney biopsy. All the patients were alive in the course of the study.

The distribution of the patients with hypertension according to steroid response was as follows: eight patients (61.5%) with SRNS, two patient (15.4%) with SDNS and three patients (23.1%) with FRNS. Based on the biopsy results, there was MCD in five patients (38.5%), FSGS in four patients (30.8%) and mesangial proliferative glomerulonephritis in two patients (15.4%).

Four patients progressed to end-stage renal disease (ESRD) at the end of the follow-up.


Discussion

The present study demonstrates that boys younger than six years of age show a higher incidence of steroid resistance and that the rate of response to steroid and CsA is similar. In addition, hypertension and osteoporosis are common complications in patients with SRNS as expected.

INS is more common in boys than in girls with a ratio of 4:1 for new cases of NS. The peak age for the onset of NS is 2-3 years (3,4). In the previous studies in our country, male predominance was shown and average age of onset was 3-6 years (5-7). In our cohort, 58.5% of patients were boys and they experienced more steroid resistance.

One of the cardinal findings of INS in children is good response to steroid (8). Initially, response rate to steroid has been reported to be between 77.6% and 88% in different studies and the outcome was found to be better in patients who responded to steroid when compared to those who were resistant to steroid (9,10). The rate of steroid resistance has been reported to be approximately 20% in the literature (1). In the current study, the rate of response to steroid was found to be 81.7%. Resistance to steroid was detected in 18.3% of children with INS which was similar with that in a previous study performed in our country (5).

In 1978, the International Study of Kidney Disease in Children reported that 77% and 7% of childhood INS consisted of MCD and FSGS, respectively (11). In our study, MCD was the most common histopathological finding in children under the age of six. It was followed by FSGS. Recently, many studies have revealed that the frequency of the diagnosis of FSGS has been increased year by year (12-15). In our study, FSGS was detected in 16.6% of patients who underwent kidney biopsy and 75% of them had steroid resistance. Our findings were compatible with that of the study by Boyer et al. (16) which showed increased steroid resistance over the past two decades. FSGS is a histopathological finding of poor prognosis leading to the development of ESRD in patients with NS (17). In our study, we showed that 1.4% of our patients progressed to ESRD and all of them were diagnosed with FSGS.

In this study, an interesting finding was the presence of steroid resistance in 37.2% of patients who had MCD based on kidney biopsy findings. 81% of them were boys and the mean age at the diagnosis was 27 months (12-43 months). Thus, we think that younger boys were at risk for steroid resistance even in biopsy-proven MCD.

The remission rate for CsA has been reported to be between 60% and 90% (18-20). In our study, this rate was found to be 66.6% and the patients showed similar response to steroid and CsA. In a recent study performed in our country, full and partial remissions were observed with a rate of 85% with the use of Cs (5). Recently, MMF has been a commonly used steroid-sparing agent in childhood NS. In patients with SRNS, MMF gave rise to complete remission in 23-62% of patients and partial remission in 25-37% of patients (21-23). In our study, we used MMF with a mean duration of 26 months (10-44 months) and complete remission was achieved in 50% of patients. It failed in the remaining 50%.

CYC has been used to reduce relapse frequency and to induce long-term remission. In a meta-analysis including 102 children from three trials performed in children with relapsing steroid-sensitive NS, CYC significantly reduced the relapse risk at 6-12 months compared to prednisone alone (24). The response rate to CYC was 72.5% in our cohort. In addition, majority of patients who achieved remission with CYC were sensitive to steroid (79.3%). Only half of the patients with SRNS were responder to CYC.

Isolated case reports have shown a beneficial effect of rituximab in pediatric patients with primary FSGS (25). We used rituximab in two patients with SRNS who received steroids, CsA, CYC and MMF previously. Both patients were diagnosed with FSGS. One of them did not benefit from rituximab and progressed to ESRD; renal transplantation was performed ultimately in this patient. The second achieved complete remission and was clinically doing well at the last follow-up visit.

Levamisole is an antihelminthic agent and also used as a steroid-sparing agent in children with SDNS and/or FRNS. Al-Saran et al. (26) studied the effect of levamisole on FRNS/SDNS. They showed that 20 patients (62.5%) were relapse-free during the follow-up in levamisole group while no patient was relapse-free in control group. In our study, levamisole was given to 11 patients including five patients in SRNS group and six patients in SSNS group. None of the patients in SRNS group responded to levamisole. Only one child (16.6 %) in SSNS group was responder to levamizole.

It is well-known that complications may be observed due to disease itself or medications used in NS (27,28). In our study, the most common complication was osteoporosis, followed by hypertrichosis, alopecia, hypertension, peritonitis, cataract, hypothyroidism, and thromboembolism (Table 4).

Our study has several limitations associated with the retrospective design of the study. For example, the number of patients who underwent kidney biopsy and the number of patients who were given MMF and rituximab are limited. In addition, it was a single center study and etiology of INS was not uniform.


Conclusion

In conclusion, there is a high prevalence of MCD based on kidney biopsy especially in boys younger than six years of age and response to steroid and CsA is almost similar. We assume that prospective clinical studies with large number of patients should be done to evaluate the effect of the new steroid-sparing agents on outcome in children with INS.

Ethics

Ethics Committee Approval: Ethics Committee of Erciyes University Medical Faculty approved the study. (approval no: 2014/582).

Informed Consent: It was taken.

Peer-review: Externally and internally peer-reviewed.

Authorship Contributions

Surgical and Medical Practices: K.Y., İ.D. Concept: R.D., Z.G. Design: H.P., R.D. Data Collection or Processing: K.Y., S.Y. Analysis or Interpretation: İ.D., Z.G. Literature Search: K.Y., İ.D. Writing: K.Y.

Conflict of Interest: No conflict of interest was declared by the authors.

Financial Disclosure: The authors declared that this study received no financial support.


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