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Serum immunoglobulin G, M and IgG:IgM
ratio as predictors for outcome of childhood
nephrotic syndrome
Ranjit Ranjan Roy, Eliza Roy, Mohammed Habibur Rahman,
Mohammed Moazzam Hossain
Dhaka, Bangladesh
Author Affiliations: Department of Pediatrics, Nephrology Unit, Bangabandhu Sheikh Mujib Medical University (BSMMU), Dhaka, Bangladesh (Roy RR, Rahman MH, Hossain MM); International Centre for Diarrhoeal Disease Research, Bangladesh (ICDDR,B), Dhaka, Bangladesh (Roy E)
Corresponding Author: Ranjit Ranjan Roy, MBBS, FCPS MD, Flat # 6/C Sheltech Sierra, 236 New Elephant Road, Dhaka 1205, Bangladesh (Tel: 880 2 01715004079; 880 2 9673374; Email: dder@bangla.net; eliza@icddrb.org)
doi:10.1007/s12519-009-0025-2
Background: Nephrotic syndrome is an immune mediated disorder of the kidney associated with T cell dysfunction and secondary disturbance of B cell with changes in levels of immunoglobulin and IgG:IgM ratio. These changes in immunoglobulin levels can be used as a proxy marker to understand the clinical variety and prognosis of nephrotic syndrome.
Methods: We studied 43 children with nephrotic syndrome during January 2003 to January 2005 in the Pediatric Nephrology Unit, Department of Pediatrics, Bangabandhu Sheikh Mujib Medical University, Dhaka, Bangladesh. Blood samples were collected from the 43 patients, and serum levels of IgG, IgM and IgG:IgM were measured by liquid phase immunoprecipitation assay. Another 20 healthy children attending the laboratory for blood grouping and hepatitis B screening test were enrolled as controls.
Results: In the 43 children with nephrotic syndrome, 24 had steroid sensitive nephrotic syndrome (SSNS) and 19 steroid resistant nephrotic syndrome (SRNS). Compared with healthy children, the IgG level was low, IgM level was high, and IgG:IgM ratio was low (P<0.05). The serum IgG level and IgG:IgM ratio were significantly lower in children with SRNS and in children with frequent relapse (FRNS) combined with steroid dependent nephrotic syndrome (SDNS) than in those with infrequent relapse nephrotic syndrome (IFRNS) (P<0.05, respectively).
Conclusions: Management of different nephrotic syndromes is based on the levels of immunoglobulins along with clinical and biochemical parameters. The decrease of IgG level as a predictive marker for unfavorable prognosis of nephrotic syndrome in children needs further evaluation in larger scale studies.
Key words: immunoglobulins; nephrotic syndrome; prognosis
World J Pediatr 2009;5(2):127-131
Introduction
Childhood nephrotic syndrome is an immune mediated kidney disease associated with T cell dysfunction and secondary disturbance of B cell that leads to changes in levels of immunoglobulins. Researchers have hypothesized that this systemic disorder of T cell function results in the production of humoral factors or lymphokines responsible for the increase of glomerular basement membrane permeability.[1,2] Estimate on the annual incidence of nephrotic syndrome is 2-7 per 100 000 children, and the prevalence is 12-16 per 100 000. There is epidemiological evidence of a higher incidence of nephrotic syndrome in children from south Asia and Africa.[3-6]
The disease is characterized by massive proteinuria (urinary total protein >1 g/m2 per day or urinary spot protein creatinine ratio of >200 mg/mmol), hypoalbuminemia (serum albumin ¡Ü2.5 g/dL), edema, and hypercholesterolemia (serum cholesterol ¡Ý200 mg/dL).[7] The clinical outcome of the disease depends upon the age at presentation, histological changes, absence of hematuria, hypertension, impaired renal function, and responsiveness to steroid therapy.[6] Although recurrence is common in nephrotic syndrome, 90%-95% of children with minimal change nephrotic syndrome (MCNS) are responsive to steroid therapy with complete clinical and biochemical remission and have excellent long-term prognosis.[6,8-10] Primary or idiopathic nephrotic syndrome is commonly seen in 95% of patients,[8] 80% of whom show histological features of MCNS and have good prognosis.[9,11]
Nephrotic syndrome after the first diagnosis is treated with a standard steroid regimen.[12] Eighty to ninety percent of patients respond to this therapy and 10%-20% are steroid resistant.[12] Giangiocomo et al[13] correlated serum immunoglobulin with steroid treatment outcome in various types of nephrotic syndrome. They reported T cell defect in the conversion from IgM-secreting T cell to IgG-secreting T cell (switching defect), leading to a high level of IgM and a low level of IgG.[13] Therefore the estimation of IgG and IgM levels and their ratio as well as correlation of these values with clinical responsiveness to steroid therapy, relapse, and dependency is important to monitor management strategies and to know the outcome.
The objectives of this study were to compare immunoglobulin levels in children with nephrotic syndrome and healthy children, to understand changes in diseased state, and to assess differences in immunoglobulin levels among the steroid resistant (SRNS), frequent relapse and steroid dependent (FRNS+SDNS), and infrequent relapse (IFRNS) groups. Changes in IgG:IgM ratio were compared in SSNS, SRNS, FRNS+SDNS, IFRNS and healthy children.
Methods
Patients
The prospective study was carried out in the Pediatric Nephrology Unit of Bangabandhu Sheikh Mujib Medical University (BSMMU) from January 2003 to January 2005. The hospital is a tertiary referral hospital with diagnostic and treatment facilities.
A total of 480 children diagnosed with primary nephrotic syndrome were admitted in BSMMU during the study period. Forty-three children were randomly selected who were aged 1-15 years. Among them, 19 had steroid resistant nephrotic syndrome (SRNS, group B) and 24 steroid sensitive nephrotic syndrome (SSNS, group C). In group C, 11 children had FRNS+SDNS (group C1) and 13 infrequent relapsing nephrotic syndrome (IFRNS, group C2). Meanwhile, 20 healthy children attending the outpatient department for blood grouping and hepatitis B virus screening were enrolled as controls (group A). Among the 19 children with SRNS, the histological reports on biopsy were mesangial proliferative glomerulonephritis (9 children), MCNS (3), focal segmental glomerulosclerosis (3), membranoproliferative glomerulonephritis (2), and membranous glomerulonephritis (2).
Excluded were children below one year or above 15 years, and those with congenital nephrotic syndrome, nephrotic syndrome secondary to systemic disease like systemic lupus erythematosus, hepatitis B, Henoch-Schönlein purpura, falciparum malaria, lymphoma, or amyloidosis. Those with severe protein energy malnutrition or Down's syndrome were also excluded from the study.
Parents and guardians of the enrolled children were informed about the purpose of data collection and the procedures of the study, and consent was obtained at the enrollment. They were given the choice to withdraw from the study at any time during the course of the study. The study was approved by the Ethical Review Committee of BSMMU.
Laboratory and clinical investigations
Urine samples were collected on admission, and routine microscopic and physical examinations included culture sensitivity (C/S) with colony count (C/C). Spot urinary protein creatinine ratio or urinary total protein was measured by an autoanalyzer (RA 50 chemistry analyzer). 5 ml of venous blood sample was collected for estimation of serum albumin, total protein, cholesterol, creatinine, and blood urea. Serum immunoglobulin (IgG, IgM) levels were measured by liquid phase immunoprecipitation assay in all groups. Reference values of IgG and IgM were 7-14 g/L and 0.4-2.4 g/L, respectively. Cut-off value for low IgG was <7 g/L, high IgM >2.4 g/L, and IgG:IgM >3.
Mantoux test (MT) and Bacillus Calmette-Guerin (BCG) acceleration tests were performed when indicated. Antinuclear antibody (ANA) and anti-DNA double stranded antibody (anti dsDNA) were used for enzyme-linked immunosorbent assay (ELISA) in the children when indicated to rule out systemic disease. HBsAg was tested by screening and ELISA.
Chest X-ray and ultrasonography of the kidneys, ureter, and bladder were performed for all the patients. Renal biopsy was done for SRNS patients.
Study definition
SSNS was defined as responding to steroid therapy within 4 weeks after initiation of the therapy.[3,6] IFRNS was defined as less than 4 relapses within one year or less than 2 relapses within six months after initial responsive episode, and FRNS was defined as more than 4 relapses in one year and more than 2 relapses within six months after initial responsive episode. Remission was defined as protein-free urine for 3 consecutive days, and relapse was defined a proteinuria (urine albumin 3+ or more) for 3 consecutive days after initial responsive episode.[3,6] The occurrence of 2 consecutive relapses during alternate day prednisolone therapy or within 2 weeks of its discontinuation was defined as SDNS.[3,6] No remission after 4 weeks of standard prednisolone therapy at 60 mg/m2 per day was defined as SRNS.[3,6]
Treatment regimens
All children with first attack and infrequent relapse were given prednisolone 60 mg/m2 per day at divided doses for 6 weeks, followed by 40 mg/m2 on alternate days at a single dose for another 6 weeks provided they responded by 4 weeks.[3,12]
IFRNS was treated with prednisolone 60 mg/m2 per day at divided doses until urine was albumin free for 3 consecutive days and then 40 mg/m2 on alternate day for 4 weeks.[3,6]
FRNS was treated with prednisolone at a single morning dose of 0.5 mg/kg on alternate days for 12 months.[3,6] In case of steroid toxicity, a 12-week course of cyclophosphamide (2.5 mg/kg per day) or levamisole (2.5 mg/kg) on alternate days for one year was given after remission with prednisolone.[3,6] Initial prednisolone was given on alternate days at 1 mg/kg for a few weeks, then it was discontinued.[3,6]
SDNS was treated with a minimum threshold dose of prednisolone, and it was 0.25 mg/kg on alternate days, which was continued for 12 months provided there were no major side effects. The patients who developed steroid toxicity were treated with levamisole or cyclophosphamide.[3,6]
SRNS was treated with intravenous methyl prednisolone at 30 mg/kg on alternate days for 6 doses, followed by tapering doses of oral prednisolone on alternate days starting at 1.5 mg/kg for 12 months.[3] Supportive measures were also taken, including control of edema, infection, salt restriction, treatment of hypertension, supplementation of protein rich diet, calcium and micronutrient, and albumin infusion.[3,12]
Statistical analysis
Statistical analyses were performed using computer-based software, Statistical Package for Social Science (SPSS). ANOVA was used to compare differences in mean immunoglobulin levels between groups. The Chi-square test and Odd's ratio were compared between the groups. A P value <0.05 was considered statistically significant.
Results
Age distribution
Of the 63 children enrolled in the study, 41 were male and 22 female. There was no significant difference in sex distribution among groups A, B, C1, and C2 (P>0.50). The mean (¡ÀSD) ages of children in groups A, B, and C were 7.70¡À4.00, 8.70¡À4.81, and 8.43¡À3.92 years, respectively (P>0.50).
Comparisons of IgG, IgM and IgG:IgM ratio
The IgG level was lower, IgM level was higher, and IgG:IgM ratio was lower in the patient groups than in healthy controls (P<0.05) (Table 1).
The mean (¡ÀSD) IgG levels in the patient groups are shown in Table 2. The mean (¡ÀSD) IgG level was normal (11.60¡À5.24 g/L) in the healthy controls (group A). The IgG level decreased in FRNS+SDNS group (group C1) and IFRNS group (group C2), and was the lowest in SRNS group (group B). The difference in the mean IgG levels between groups B and C2 was significantly significant (P<0.001), but no statistical difference was found between groups B and C1. There was similar difference in the mean IgG (¡ÀSD) level between groups C1 and C2 (P<0.05).
The mean (¡ÀSD) IgM levels in the patient groups are shown in Table 2. The mean (¡ÀSD) IgM level was normal (1.62¡À0.76 g/L) in the healthy controls. It was higher in group B than in group C, though the difference was not statistically significant. The median values of IgM level in groups A, B, C1 and C2 were 1.50, 3.60, 2.11 and 2.90 g/L, respectively.
IgG:IgM ratio was significantly lower (P<0.05) in groups B and C1 than in group C2, but the ratio did not differ between groups B and C1. The median values of IgG:IgM ratio in groups A, B, C1 and C2 were 8.5, 0.70, 1.50 and 1.88, respectively.
Table 1. IgG, IgM levels and IgG:IgM ratio in the patients and controls
|
Parameters |
Controls
n (%) |
Patients
n (%) |
Odd's
ratio |
95% CI |
P |
|
IgG (g/L) |
|
|
|
|
|
|
<7 (low) |
4 (20.0) |
38 (88.4) |
0.03 |
(0.01, 0.16) |
<0.05 |
|
7-14 (normal) |
16 (80.0) |
5 (11.6) |
|
IgM (g/L) |
|
|
|
|
|
|
0.4-2.4 (normal) |
7 (85.0) |
18 (41.9)
|
7.8 |
(1.7, 39.9) |
<0.05 |
|
>2.4 (high) |
3 (15.0) |
25 (58.1) |
|
IgG:IgM |
|
|
|
|
|
|
<3 (low) |
3 (15.0) |
35 (81.4) |
0.05 |
(0.01, 0.22) |
<0.05 |
|
>3 (high) |
17 (85.0) |
9 (20.9) |
Table 2. Comparison of IgG, IgM and IgG:IgM ratio between different types of nephrotic syndrome
|
Parameters |
Mean ¡À SD |
Median |
Range |
95% CI |
|
IgG (g/L) |
|
|
|
|
|
SRNS (B) |
2.67¡À1.65 |
2.30 |
0.60-7.50 |
(1.88, 3.47) |
|
FRNS + SDNS (C1) |
3.34¡À1.44 |
3.50 |
0.50-5.50 |
(2.37, 4.31) |
|
IFRNS (C2) |
5.84¡À3.37* |
4.60 |
1.00-12.50 |
(3.80, 4.87) |
|
IgM (g/L) |
|
|
|
|
|
SRNS (B) |
3.17¡À1.54 |
3.60 |
0.75-5.10 |
(2.42, 3.91) |
|
FRNS + SDNS (C1) |
2.27¡À0.87 |
2.11 |
1.25-3.69 |
(1.69, 2.85) |
|
IFRNS (C2) |
2.92¡À1.63 |
2.90 |
0.37-5.70 |
(1.93, 3.90) |
|
IgG:IgM |
|
|
|
|
|
SRNS (B) |
1.27¡À1.25 |
0.70 |
0.14-4.55 |
(0.67, 1.88) |
|
FRNS + SDNS (C1) |
1.74¡À1.10 |
1.50 |
0.28-3.52 |
(1.01, 2.48) |
|
IFRNS (C2) |
3.51¡À3.78† |
1.88 |
0.20-12.16 |
(1.22, 5.79) |
*: P<0.05, compared with groups B and C2, respectively; †: P<0.05, compared with groups B and C1, respectively.
Discussion
The children with nephrotic syndrome had low levels of IgG and high levels of IgM compared with the controls in this study, which is consistent with a previous study by Giangiocomo et al[13] where low IgG and IgA levels and high IgM level in idiopathic and secondary nephrotic syndrome have been reported. They concluded that T cell dysfunction is responsible for failure to convert surface IgM-bearing B lymphocyte (plasma cell) into subsequent IgG and IgA secreting plasma cell apart from urinary loss of immunoglobulin as was suggested previously by Peterson et al.[14] This hypothesis was further supported by Shakib et al[15] who have shown asymmetric depression of IgG subclasses (I to IV) in serum of patients with nephrotic syndrome. Subsequent works supporting similar view of T cell defect were made by Warshaw and Check,[16] Sobel et al,[17] Ingelfinger et al,[18] and Rashid et al.[19] Chen et al[20] reported that enhanced suppressor T cell activity resulted in increased IgM and decreased IgG production in children with nephrotic syndrome. Dall'Aglio et al[21] observed significantly increased IgG-bearing (sIgG-C) B cells. Vascular permeability factor produced by T lymphocytes had been observed.[22-24]
The IgG levels were lower in the SRNS, FRNS+SDNS groups compared to the IFRNS group in our study. Similar low levels of IgG were found in a study by Andal et al[24] who observed frequent relapses had lower IgG than infrequent relapsers, but there was no difference in IgM level between the two groups. In another study, Das et al[25] noticed very low IgG level in SRNS patients. Mishra et al,[26] however, did not find any significant difference between IFRNS and FRNS patients, but observed decreased IgG and IgA levels and increased IgM level and circulating immune complex in the serum of patients with active nephrotic syndrome. Mishra et al[26] showed significantly higher circulating IgG complexes in relapse than in remission or controlled children. Kemper et al[27] found no difference in relapse and remission children; in both situations they observed low IgG and high IgM levels.
The IgM level was elevated significantly in the patient group compared with the healthy controls. Similar findings of low IgG and high IgM levels in the patient group of idiopathic nephrotic syndrome are consistent with previous reports.[13,17,19,26,28] Low IgG and high IgM levels are seen in hyper IgM syndrome, a condition in which hypogamma globulinemia occurs with increased IgM and decreased IgG levels in the absence of features of nephrotic syndrome.[29] Therefore, decreased IgG and increased IgM levels associated with other features of nephrotic syndrome may be of diagnostic value.
In this study, IgG:IgM ratio was found to be significantly lower in the patient group than in the healthy controls. Similarly, a study in Taiwan showed IgG:IgM ratio of more than 3.0 in most patients with SSNS and the ratio of IgG:IgM more than 1.0 in those of SRNS or FRNS.[30] The finding indicates that the lower the ratio the worse the outcome.
In conclusion, IgG level is decreased and IgM level is increased in all patients with nephrotic syndrome compared with healthy children. Immunoglobulin levels can be used as an important serological marker to predict responsiveness to treatment in different nephrotic syndromes. Serological makers for quick diagnosis are extremely important in management of the disease.
Funding: No funding.
Ethical approval: This study was approved by the BSMMU.
Competing interest: None declared.
Contributors: Roy RR conducted the study, Roy E and Rahman MH provided help, and Hossain MM supervised the study.
References
1 Sahali D, Lang P, Guellaen G, Bensman A. New insights about immunopathology of lipoid nephrosis. Bull Acad Natl Med 2002;186:683-690.
2 Bagga A, Mantan M. Nephrotic syndrome in children. Indian J Med Res 2005;122:13-28.
3 Abdurrahman MB, Aikhionbare HA, Babaoye FA, Sathiakumar N, Narayana PT. Clinicopathological features of childhood nephrotic syndrome in northern Nigeria. Q J Med 1990;75:563-576.
4 Eddy AA, Symons JM. Nephrotic syndrome in childhood. Lancet 2003;362:629-639.
5 McKinney PA, Feltbower RG, Brocklebank JT, Fitzpatrick MM. Time trends and ethnic patterns of childhood nephrotic syndrome in Yorkshire, UK. Pediatr Nephrol 2001;16:1040-1044.
6 Srivastava RN, Bagga A. Nephrotic syndrome. In: Srivastava RN, Bagga A, eds. Pediatric Nephrology, 4th ed. New Delhi: Jaypee Brothers, Medical Publishers (P) Ltd., 2005: 161-197.
7 ISKDC (International Study of Kidney Diseases in Children). Nephrotic syndrome in children: prediction of histopathology from clinical and laboratory characteristics at time of diagnosis. Kidney Int 1978;13:159-165.
8 Churg J, Habib R, White RH. Pathology of the nephrotic syndrome in children. A report for the International Study of Kidney Disease in Children. Lancet 1970;1:1299-1302.
9 Salcedo JR, Thabet MA, Latta K, Chan JC. Nephrosis in childhood. Nephron 1995;71:373-385.
10 ISKDC (International Study of Kidney Diseases in Children). The primary nephrotic syndrome in children. Identification of patients with minimal change nephrotic syndrome from initial response to prednisone. A report of the International Study of Kidney Disease in Children. J Pediatr 1981;98:561-564.
11 Behrman RE, Kliegman RM, Jenson HB. Nephrotic syndrome. In: Nelson Textbook of Pediatrics, 17th ed. Philadelphia: WB Saunders Company, 2004: 1753-1757.
12 Niaudet P. Steroid sensitive idiopathic nephrotic syndrome in children. In: Avner ED, Harmoh WE, Niaudet P, eds. Pediatric Nephrology, 5th ed. Philadelphia: Lippincott Williams and Wilkins, 2004: 543-553.
13 Giangiacomo J, Cleary TG, Cole BR, Hoffsten P, Robson AM. Serum immunoglobulins in the nephrotic syndrome. A possible cause of minimal-change nephrotic syndrome. N Engl J Med 1975;293:8-12.
14 Peterson PA, Berggard I. Urinary immunoglobulin components in normal, tubular, and glomerular proteinuria: quantities and characteristics of free light chains, IgG, igA, and Fc-gamma fragment. Eur J Clin Invest 1971;1:255-264.
15 Shakib F, Hardwicke J, Stanworth DR, White RH. Asymmetric depression in the serum level of IgG subclasses in patients with nephrotic syndrome. Clin Exp Immunol 1977;28:506-511.
16 Warshaw BL, Check IJ. IgG subclasses in children with nephrotic syndrome. Am J Clin Pathol 1989;92:68-72.
17 Sobel AT, Intrator L, Lagrue G. Serum immunoglobulins in idiopathic minimal change nephrotic syndrome. N Engl J Med 1976;294:250.
18 Ingelfenger JR, Link DA, Davies AE, Grupe WE. Serum immunoglobulin in idiopathic minimal change nephrotic syndrome [letter]. N Engl J Med 1976;294:1.
19 Rashid H, Skillen AW, Morley AR, Kerr DN. Serum immunoglobulins in minimal change nephrotic syndrome: a possible defect in T cell function. Bangladesh Med Res Coun Bull 1982;8:15-20.
20 Chen CH, Hsieh KH, Lee PP. Enhanced suppressor T cell activity resulting in increased IgM and decreased IgG productions in children with minimal change nephrotic syndrome. Int J Pediatr Nephrol 1987;8:75-80.
21 Dall'Aglio P, Meroni PL, Barcellini W, Brigati C, Chizzolini C, De Bartolo G, et al. Altered expression of B lymphocyte surface immunoglobulins in minimal change nephrotic syndrome and focal glomerulosclerosis. Nephron 1984;37:224-228.
22 Lagrue G, Xheneumont S, Branellec A, Weil B. Letter: Lymphokines and nephrotic syndrome. Lancet 1975;1:271-272.
23 Kondo S, Yoshizawa N, Kusumi Y, Takeuchi A, Torikata C. Studies of glomerular permeability factor (GPF) in focal segmental glomerular sclerosis and the relationship between GPF and vascular permeability factor (VPF). Clin Nephrol 1999;52:278-284.
24 Andal A, Chellani H, Anand NK, Chandra M. Low serum immunoglobulin G ¨C a predictor of frequent relapses in idiopathic nephrotic syndrome. Indian Pediatr 1990;27:1045-1049.
25 Das BK, Kumar S, Sen MR, Mishra OP. Letters to editor. J Trop Pediatr 1994;49:189-190.
26 Mishra OP, Garg R, Usha, Ali Z, Das BK. Immunoglobulins and circulating immune complexes in nephrotic syndrome. J Trop Pediatr 1997;43:93-97.
27 Kemper MJ, Altrogge H, Ganschow R, M¨¹ller-Wiefel DE. Serum levels of IgG and IgG subclasses in steroid sensitive nephrotic syndrome. Pediatr Nephrol 2002;17:413-417.
28 Momma K. Immunochemical semiquantitative estimation of M and A immunoglobulins in healthy and diseased children. 2. Immunoglobulin levels in nephrotic syndrome, exudative enteropathy, acute leukemia, and malignant tumors. Acta Paediatr Jpn 1965;7:13-22.
29 Cotran RS, Kumar V, Collins T. Diseases of immunity. In: Cotran RS, Kumar V, Collins T, eds. Robbins Pathologic Basis of Disease, 6th ed. Philadelphia: WB Saunders Company, 1999: 188-259.
30 Wang HH, Fu LW, Yang LY, Chen WP, Tasai SJ, Lin CY. A study of the relationship between IgG subclass/IgM and idiopathic nephrotic syndrome. Zhonghua Min Guo Xiao Er Ke Yi Xue Hui Za Xhi 1997;38:21-27.
Received December 20, 2007 Accepted after revision August 13, 2008
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