G U I D E L I N E S F O R P R A C T I C E
Management of Steroid Sensitive INTRODUCTION Nephrotic Syndrome:
Nephrotic syndrome is an important chronic disease
Revised Guidelines
in children. About 80% children with idiopathicnephrotic syndrome show remission of proteinuriafollowing treatment with corticosteroids, and are
INDIAN PEDIATRIC NEPHROLOGY GROUP,
classified as ‘steroid sensitive’. Most patients have
INDIAN ACADEMY OF PEDIATRICS
multiple relapses, placing them at risk for steroidtoxicity, systemic infections and other complica-tions. A small proportion of patients who are not
ABSTRACT
steroid sensitive (steroid resistant) are also at risk forsimilar complications and renal insufficiency. Justification: In 2001, the Indian Pediatric Nephrology Group formulated guidelines for management of patients
Most pediatricians would encounter few patients
with steroid sensitive nephrotic syndrome. In view of
with nephrotic syndrome in their practice. They
emerging scientific evidence, it was felt necessary to
should be familiar with management of these
review the existing recommendations. Process:
patients and be aware of situations in which referral
Following a preliminary meeting in March 2007, a draft
to a pediatric nephrologist is required. Long-term
statement was prepared and circulated among pediatric
management of these patients should thereafter be a
nephrologists in the country to arrive at a consensus on
joint effort between the pediatrician and the pediatric
the evaluation and management of these patients. Objectives: To revise and formulate recommendations for management of steroid sensitive nephrotic syndrome.OBJECTIVES Recommendations: The need for adequate cortico- steroid therapy at the initial episode is emphasized.
Guidelines on the management of children with
Guidelines regarding the initial evaluation, indications
nephrotic syndrome were first formulated by the
for renal biopsy and referral to a pediatric nephrologist
Indian Pediatric Nephrology Group in 2001(1). are updated. It is proposed that patients with frequently
Since a number of studies on management of these
relapsing nephrotic syndrome should, at the first
patients have been published during the last 7 years,
instance, be treated with long-term, alternate-dayprednisolone. The indications for use of alternative
it was felt desirable to review the existing
immunosuppressive agents, including levamisole,
recommendations. Therefore, following a prelimi-
cyclophosphamide, mycophenolate mofetil and
nary meeting in New Delhi (7 March 2007), a draft
cyclosporin are outlined. The principles of dietary
statement was prepared, circulated and reviewed
therapy, management of edema, and prevention and
by pediatric nephrologists across the country
management of complications related to nephrotic
(Annexure I). The present document reflects the
syndrome are described. These guidelines, formulated on
current opinion on management of patients with
basis of current best practice, are aimed to familiarize
steroid sensitive nephrotic syndrome. physicians regarding management of children withsteroid sensitive nephrotic syndrome.RECOMMENDATIONS Key words: Nephrotic syndrome, Practice guidelines,
Important revisions in this document are listed in Table I. Correspondence to: Dr. Arvind Bagga, Department ofDefinitions Pediatrics, All India Institute of Medical Sciences, AnsariNagar, New Delhi 110 029, India.
Nephrotic syndrome is characterized by heavy
proteinuria, hypoalbuminemia (serum albumin
TABLE I IMPORTANT REVISIONS IN THIS DOCUMENT
Investigations necessary at initial and subsequent evaluation are described.
While updating the literature, the Group endorses the existing guidelines on therapy for the initial episode of nephroticsyndrome.
The role of alternative medications, including mycophenolate mofetil, cyclosporin and tacrolimus in patients withfrequent relapses and steroid dependence is discussed and therapeutic choices further clarified.
Details on dose and duration of therapy with corticosteroids, when co-administered with other agents are included.
Guidelines on immunization, isoniazid prophylaxis and hypertension updated in conformity with recommendations ofthe Indian Academy of Pediatrics.
Management of complications updated.
<2.5 g/dL), hyperlipidemia (serum cholesterol >200
creatinine. Estimation of blood levels of anti-
mg/dL) and edema(1,2). Nephrotic range proteinuria
streptolysin O and C3 is required in patients
is present if early morning urine protein is 3+/4+ (on
with gross or persistent microscopic hematuria.
dipstick or boiling test), spot protein/creatinine ratio
Appropriate tests are performed, if necessary, for
>2 mg/mg, or urine albumin excretion >40 mg/m2
associated conditions (e.g., chest X-ray and tuber-
per hr (on a timed-sample). Precise quantitative
culin test, hepatitis B surface antigen, antinuclear
assessment of proteinuria, including 24-hr urine
antibodies). Urine culture is not necessary unless the
protein measurement is seldom necessary.
patient has clinical features suggestive of a urinary
Definitions for clarifying the course of nephrotic
syndrome are shown in Table II. Treatment of the Initial Episode Initial Evaluation
Adequate treatment of the initial episode, both in
A detailed evaluation is necessary before starting
terms of dose and duration of corticosteroids, is
treatment with corticosteroids. The height, weight
important. Evidence from multiple studies suggests
and blood pressure should be recorded. Regular
that appropriate therapy at the first episode of
weight record helps monitor the decrease or increase
nephrotic syndrome is an important determinant of
of edema. Physical examination is done to detect
the long-term course of the disease(3).
infections and underlying systemic disorder, e.g.,systemic lupus erythematosus, Henoch Schonlein
Medication: The standard medication for treatment
purpura, etc. Infections should be treated before
is prednisolone or prednisone. The medication is
starting therapy with corticosteroids.
administered after meals to reduce its gastro-intestinal side effects. The use of methyl-
Investigations recommended at the initial
prednisolone, dexamethasone, betamethasone, tri-
episode include: (i) urinalysis; (ii) complete blood
amcinolone or hydrocortisone is not recommended.
count, blood levels of albumin, cholesterol, urea and
There is also limited evidence on the efficacy or
TABLE II DEFINITIONS RELATED TO NEPHROTIC SYNDROME
Urine albumin nil or trace (or proteinuria <4 mg/m2/h) for 3 consecutive early morning specimens.
Urine albumin 3+ or 4+ (or proteinuria >40 mg/m2/h) for 3 consecutive early morning specimens,having been in remission previously.
Two or more relapses in initial six months or more than three relapses in any twelve months.
Two consecutive relapses when on alternate day steroids or within 14 days of its discontinuation.
Absence of remission despite therapy with daily prednisolone at a dose of 2 mg/kg per day for 4 weeks.
benefits of therapy with deflazocort for nephrotic
rarely result in spontaneous remission, thereby
avoiding the need for treatment with corticosteroids. Treatment regimen:Various treatment regimens
Prednisolone is administered at a dose of
have been used for the treatment of the initial episode
2 mg/kg/day (single or divided doses) until urine
of nephrotic syndrome. The International Study
protein is trace or nil for three consecutive days.
for Kidney Diseases in Children had originally
Subsequently, prednisolone is given in a single
recommended a regimen comprising of four-weeks
morning dose of 1.5 mg/kg on alternate days for
each of daily and alternate day steroid therapy(4),
4 weeks, and then discontinued(1,5). The usual
which was used for almost three decades. Controlled
duration of treatment for a relapse is thus 5-6 weeks.
studies later suggested that prolongation of initial
Prolongation of therapy is not necessary for patients
steroid therapy for 12 weeks or longer is associated
with infrequent relapses (see below).
with significantly reduced risk for subsequentrelapses. However, prolonged treatment with
In case the patient is not in remission despite two
steroids is associated with a higher frequency of
weeks treatment with daily prednisolone, the
treatment is extended for 2 more weeks. Patientsshowing no remission despite 4 weeks’ treatment
The Cochrane Renal Group(3), on systematic
with daily prednisolone should be referred for
analysis of the literature, recommends that the
duration of initial prednisolone therapy should be fora minimum of 12 weeks. It further suggests that the
Infrequent Relapsers
benefits of sustained remission and reduction in
Patients who have three or less relapses a year and
relapse rates are superior if alternate-day treatment is
respond promptly to prednisolone are managed
not stopped abruptly at 12 weeks, but tapered over
using the aforementioned regimen for each relapse.
the next 2-4 months. It is emphasized that none of the
Such children are at a low risk for developing steroid
studies included in this analysis was placebo-
controlled, most lacked allocation concealment andwere not powered to evaluate side effects of
Frequent Relapsers and Steroid Dependence
prolonged treatment(3). The debate regarding
Patients with frequent relapses or steroid
appropriate dose and duration of steroid treatment is
dependence should be managed in consultation with
not resolved. Other regimens are being examined
that reduce the risk of relapse without increased sideeffects.
It is usually not necessary to perform a renal
biopsy in these cases. Following treatment of a
Based on current evidence and opinion, the
relapse, prednisolone is gradually tapered to
Group recommends that the initial episode of
maintain the patient in remission on alternate day
nephrotic syndrome be treated with prednisolone at a
dose of 0.5-0.7 mg/kg, which is administered for 9-
dose of 2 mg/kg per day (maximum 60 mg in single
18 months. A close monitoring of growth and blood
or divided doses) for 6 weeks, followed by 1.5 mg/kg
pressure, and evaluation for features of steroid
(maximum 40 mg) as a single morning dose on
toxicity is essential. If the prednisolone threshold,
alternate days for the next 6 weeks; therapy is then
to maintain remission, is higher or if features of
discontinued. The benefits and safety of prolonged
corticosteroid toxicity are seen, additional use of the
initial steroid therapy, beyond 12 weeks, require
following immuno-modulators is suggested. Treatment of Relapse Levamisole is administered at a dose of2-2.5 mg/kg on alternate days for 12-24
The patient should be examined for infections,
months(7-9). Co-treatment with prednisolone
which should be treated before initiating steroid
at a dose of 1.5 mg/kg on alternate days is given
therapy. Appropriate therapy of an infection might
for 2-4 weeks; its dose is gradually reduced
by 0.15-0.25 mg/kg every 4 weeks to a mainte-
nephrotoxicity (increase in serum creatinine by
nance dose of 0.25-0.5 mg/kg that is continued
30% or more from the baseline)(12). Trough
for six or more months. Occasionally, it might
(12-hr) CsA levels should be kept between 80-
be possible to discontinue treatment with
120 ng/mL(12). Side effects of CsA therapy
corticosteroids. The chief side effect of
levamisole is leukopenia; flu-like symptoms,
liver toxicity, convulsions and skin rash are
toxicity; hypercholesterolemia and elevated
rare. The leukocyte count should be monitored
transaminases may occur. Estimation of blood
levels of creatinine is required every 2-3months and a lipid profile annually. A repeat
Cyclophosphamide is administered at a
kidney biopsy, to examine for histological
dose of 2-2.5 mg/kg/day for 12 weeks(10).
evidence of nephrotoxicity, should be done if
Prednisolone is co-administered at a dose of
therapy with calcineurin inhibitors is extended
followed by 1 mg/kg for the next 8 weeks;steroid therapy is tapered and stopped over the
Tacrolimus is an alternative agent, adminis-
tered at a dose of 0.1-0.2 mg/kg daily for 12-24
months. Side effects include hyperglycemia,
diarrhea and rarely neurotoxicity (headache,seizures). The use of tacrolimus is preferred
Total leukocyte counts are monitored every
especially in adolescents, because of lack of
2 weeks; treatment with cyclophosphamide is
cosmetic side effects(13). Blood levels of
temporarily discontinued if the count falls
creatinine and glucose should be estimated
Mycophenolate mofetil (MMF) is given at a
complication of hemorrhagic cystitis; other
dose of 800-1200 mg/m2 along with tapering
side effects are alopecia, nausea and vomiting.
doses of prednisolone for 12-24 months(7,14).
The risk of gonadal toxicity is limited with
The principal side effects include gastro-
intestinal discomfort, diarrhea and leukopenia.
phosphamide(7,10,11). The use of more than
Leukocyte counts should be monitored every
one course of this agent should preferably be
1-2 months; treatment is withheld if count falls
Choice of agent: The advantages of using these
chlorambucil, unless under close supervision,
drugs should be balanced against their potential
toxicity. There are few studies comparing one agent
Calcineurin inhibitors: Cyclosporin (CsA) is
with another, but evidence for efficacy is strongest
given at a dose of 4-5 mg/kg daily for 12-24
for cyclophosphamide and CsA. Levamisole has a
months. Prednisolone is co-administered at a
modest steroid sparing effect and is a satisfactory
dose of 1.5 mg/kg on alternate days for 2-4
initial choice for patients with frequent relapses or
weeks; its dose is gradually reduced by 0.15-
steroid dependence. Treatment with cyclophospha-
0.25 mg/kg every 4 weeks to a maintenance
mide is preferred in patients showing: (i) significant
dose of 0.25-0.5 mg/kg that is continued for six
steroid toxicity, (ii) severe relapses with episodes
or more months. Occasionally, treatment with
of hypovolemia or thrombosis, and (iii) poor
corticosteroids may be discontinued.
compliance or difficult follow up, where 12 weekstherapy might be possible to ensure than long-term
Estimation of trough blood levels of CsA is
required in patients with suspected non-compliance, unsatisfactory response or
recommended for patients who continue to show
corticosteroids stimulates appetite, parents should be
steroid dependence or frequent relapses despite
advised regarding ensuring physical activity and
treatment with the above medications(12). Either of
these agents is effective in maintaining remission in
Edema: Control of edema is an integral part of
most patients with steroid sensitive nephrotic
supportive care. Since treatment with corticosteroids
syndrome. The chief concern with their use is
usually leads to diuresis within 5-10 days, diuretics
nephrotoxicity, but with careful assessment of renal
are avoided unless edema is significant. Diuretics
function, minimizing the maintenance dose and
should also not be given to patients with diarrhea,
utilizing renal biopsies in those receiving prolonged
therapy, this risk can be minimized. Recent caseseries(14) and a controlled trial(15) support the use
Patients with persistent edema and weight gain of
of MMF as a steroid sparing agent. The lack of renal,
7-10% are treated with oral frusemide (1-3 mg/kg
hemodynamic and metabolic toxicity with this agent
daily). Additional treatment with potassium sparing
makes it an attractive alternative to calcineurin
diuretics is not required if frusemide is used at this
dose for less than one week. Patients requiringhigher doses and prolonged duration of treatment
with frusemide should receive potassium sparing
levamisole, MMF and calcineurin inhibitors,
diuretics, e.g., spironolactone (2-4 mg/kg daily).
treatment with prednisolone might be tapered and
Blood pressure should be monitored frequently. A
discontinued after 6-12 months. Some patients who
gradual reduction of edema, over one week, is
respond to therapy with levamisole, MMF and
calcineurin inhibitors may relapse once thesemedications are discontinued. Relapses during or
Edema not responding to the above therapy
following therapy with these agents are treated with
should be managed in a hospital. A combination of a
loop and thiazide diuretic, and/or a potassiumsparing agent is occasionally necessary. For patients
Failure of alternative medication: If a patient has
with refractory edema, a combination of diuretics
two or more relapses over 6 months while on
and albumin infusion is used. Albumin (20%) is
treatment with any of the above agents, its
given as an infusion at a dose of 0.5-1 g/kg over 2-4
replacement with an alternative medication should
hr, followed by administration of frusemide (1-2 mg/
be considered. A protocol summarizing the
kg intravenously). While infusion of albumin results
management of patients with steroid sensitive
in increased urine output, the effect is not sustained
nephrotic syndrome is shown in Fig. 1.
and repeated administration might be necessary. Supportive Care
Albumin should be administered very cautiously inpatients with renal failure, pneumonia or pulmonary
This forms an important aspect of managing children
edema due to its potential to increase the plasma
volume. Patients receiving albumin should beobserved for respiratory distress, hypertension
Diet: A balanced diet, adequate in protein (1.5-2 g/
and congestive heart failure. Refractory ascites
kg) and calories is recommended. Patients with
interfering with respiration or associated with breaks
persistent proteinuria should receive 2-2.5 g/kg of
in the skin may be removed by cautious paracentesis.
protein daily(16). Not more than 30% calories
A protocol for treatment of edema is shown in Fig. 2.
should be derived from fat and saturated fatsavoided. While salt restriction is not necessary in
Patient and parent education: Long-term outcome of
most patients with steroid sensitive nephrotic
children with steroid sensitive nephrotic syndrome is
syndrome, reduction of salt intake (1-2 g per day) is
satisfactory, with the majority in sustained remission
advised for those with persistent edema. Salt should
and with normal renal functions by adolescence. A
not be added to salads and fruits, and snacks
proportion of patients, especially those (i) with early
containing high salt avoided. Since treatment with
onset of nephrotic syndrome, (ii) with a frequently
Absence of hypertension, hematuria, azotemia
Prednisolone 2 mg/kg daily for 6 weeks, followed by 1.5 mg/kg on alternate days for 6 weeks
Threshold <0.5-0.7 mg/kg on alternate days
FIG. 1. Management of patients with steroid sensitive nephrotic syndrome.
relapsing course, and (iii) requiring treatment with
expected course and risk of complications. The
alkylating agents or CsA may continue to show
relapses beyond adolescence(18). Parents should be
Urine examination for protein at home using
reassured that despite a relapsing course, progression
dipstick, sulfosalicylic acid or boiling test. The
to end stage renal failure necessitating dialysis or
during a relapse, during intercurrent infections
Parental motivation and involvement is essential
or if there is even mild periorbital puffiness.
in the long-term management of these children. They
should be provided information about the disease, its
remission. The importance of detecting relapse
before development of significant edema is
Maintain a diary showing results of urine
protein examination, medications received and
Ensure normal activity and school attendance;
the child should continue to participate in all
Since infections are an important cause ofmorbidity, patients should receive appropriate
Other medications: The use of antacids or histamine receptor antagonists (e.g., ranitidine) is not
necessary, unless there are symptoms of upper
gastrointestinal discomfort. Long-term calciumsupplementation (calcium carbonate, 250-500 mg) is
necessary if the patient receives more than 3 months
treatment with prednisolone(19). Patients withsteroid sensitive nephrotic syndrome do not usually
require medications for hyperlipidemia, since lipids
Immunization:Parents should be advised regarding
the need for completing the primary immunization. Administration of some vaccines, e.g., hepatitis B,measles-mumps-rubella or meningococcal vaccines
Patients receiving prednisolone at a dose of 2 mg/
kg/day or greater, or total 20 mg/day or greater (for
patients weighing >10 kg) for more than 14 days areconsidered immunocompromised(20). Such patients
FIG. 2. Management of edema in patients with nephrotic
should not receive live attenuated vaccines;
syndrome. Patients requiring high-dose frusemide or
inactivated or killed vaccines are safe(20). Live
addition of other diuretics should be under closesupervision, preferably in a hospital. Monitoring of
vaccines are administered once the child is off
serum electrolytes is necessary in all patients
immunosuppressive medications for at least 4
receiving diuretics. Patients showing hypokalemia
weeks. If there is a pressing need, these vaccines may
require potassium supplements or co-administration
be given to patients receiving alternate day
of spironolactone. The medications are reduced
prednisolone at a dose less than 0.5 mg/kg.
* Management of hypovolemia consists of rapid infusion of
All children with nephrotic syndrome should
normal saline at a dose of 15-20 mL/kg over 20-30 minutes;
receive immunization against pneumococcal
this may be repeated if clinical features of hypovolemia
infections(21). It is important to note that not all
persist. Infusion of 5% albumin (10-15 mL/kg) or 20%
pneumococcal serotypes are included in the vaccines
albumin (0.5-1 g/kg) may be used in subjects who do notrespond despite two boluses of saline.
and that antibody levels may decline during a
relapse. Previously vaccinated children may, there-
TABLE III INDICATIONS FOR KIDNEY BIOPSY
fore, develop pneumococcal peritonitis and sepsis.
The Expert Group endorses the recommendations ofthe Immunization Committee of the Indian Academy
of Pediatrics(22). The Committee recommends 2-4
• Gross hematuria, persistent microscopic hematuria or
doses of the heptavalent conjugate pneumococcal
vaccine for children below 2 yr of age. For
previously unimmunized children between 2-5 yr
• Renal failure not attributable to hypovolemia.
old, a priming dose of the conjugate vaccine should
• Suspected secondary causes of nephrotic syndrome.
be followed 8 weeks later, by a dose of the 23-valent
polysaccharide vaccine. Children older than 5 yr
• Proteinuria persisting despite 4-weeks of daily
require only a single dose of the polysaccharide
vaccine. The vaccine should be given during
• Before treatment with cyclosporin A or tacrolimus.
remission, preferably when the child is not receivingdaily prednisolone. Revaccination after 5 yr isconsidered for children (<10-yr-old) with active
Complications
Patients with steroid sensitive nephrotic syndrome
suppressive therapy should receive the varicella
are at risk for certain complications, early detection
vaccine. One dose is recommended for children
between 12 months and 12 yr of age, and 2 doses
Infections:Children with nephrotic syndrome are
separated by an interval of at least 4 weeks for
susceptible to severe infections, which need prompt
treatment. Common infections include peritonitis,
Kidney Biopsy
cellulitis and pneumonia. Viral and bacterial infec-tions may occasionally precipitate relapses in
Children with idiopathic nephrotic syndrome not
patients previously in remission. The clinical
having hematuria, hypertension or impaired renal
features and management of common serious
function are treated with corticosteroids without
infections are summarized in Table V.
requiring a kidney biopsy. A biopsy is usually not
Varicella may be a severe illness in patients with
necessary in patients with frequent relapses or
nephrotic syndrome receiving corticosteroids or
steroid dependence before starting treatment with
other immunosuppressive drugs. Susceptible
levamisole, cyclophosphamide or MMF, but should
patients (those unimmunized or with no history of
be performed before therapy with calcineurin
varicella) who are exposed to a case of chickenpox
inhibitors. A biopsy is required to identify the underlying renal disease in certain cases (Table III). TABLE IV INDICATIONS FOR REFERRAL TO A PEDIATRIC
Kidney biopsies must be performed by experts
with experience in the procedure. Centers that
Onset below 1-year of age; family history of nephrotic
perform kidney biopsies should have facilities for
evaluation of the specimens by light and immuno-
Nephrotic syndrome with hypertension, gross/persistent
microscopic hematuria, impaired renal function, orextrarenal features (e.g., arthritis, serositis, rash). Referral to Pediatric Nephrologist
Complications: refractory edema, thrombosis, severeinfections, steroid toxicity.
Indications for referral of patients are given in Table IV. The care of these patients should be a joint
collaboration between the pediatrician and pediatric
Frequently relapsing or steroid dependent nephrotic
should therefore receive a single dose of varicella
immobilization, indwelling vascular catheters,
zoster immunoglobulin, within 96 hr of exposure to
aggressive diuretic use and puncture of deep vessels
prevent or lessen the severity of the disease(17).
predispose to thrombus formation. Renal vein
Since, this preparation is expensive and not easily
thrombosis is suspected in a patient with oligoanuria,
available, a single dose of intravenous immuno-
hematuria or flank pain, especially following an
globulin (400 mg/kg) may be used instead(23).
episode of dehydration. Femoral and mesenteric
However, no clinical data showing the effectiveness
arterial thrombosis may occasionally occur. Deep
of the latter strategy are available.
vein thrombosis of calf veins is less common inchildren but may lead to pulmonary embolism.
Patients who develop varicella should receive
Saggital sinus and cortical venous thrombosis may
intravenous acyclovir (1500 mg/m2/day in 3 doses)
follow episodes of diarrhea and present with
or oral acyclovir (80 mg/kg/day in 4 doses) for
convulsions, vomiting, altered sensorium and
7-10 days(23). The dose of prednisolone should be
neurological deficits. Ultrasonography, Doppler
tapered to 0.5 mg/kg/day or lower during the
studies and cranial MRI are useful in confirming the
Patients with thrombotic complications require
urgent treatment. The treatment includes correction
tuberculosis should receive prophylaxis with INH
of dehydration and other complications, and
for six months(24). Those showing evidence of
use of heparin (IV) or low-molecular-weight
active tuberculosis should receive standard therapy
heparin (subcutaneously) initially, followed by oral
anti-coagulants on the long-term(16,17). There
Thrombosis: Children with nephrotic syndrome
is no role for prophylactic treatment with
are at risk for venous and, rarely, arterial
anticoagulants in patients with hypoalbuminemia
thrombosis(16,17). Reduced intravascular volume,
TABLE V CLINICAL FEATURES AND MANAGEMENT OF INFECTIONS* Parenteral: ampicillin andaminoglycoside; orcefotaxime/ceftriaxonefor 7-10 days
Systemic: Amphotericinfor 14-21 days
*Supplemental stress doses of hydrocortisone or prednisolone are usually necessaryHypertension: This may be detected at the onset of
and revised based on systematic reviews, published
nephrotic syndrome or later due to steroid toxicity.
studies and expert opinion of the members of the
Therapy is initiated with ACE inhibitors, calcium
channel blockers or adrenergic antagonists,
guidelines are intended to familiarize physicians
keeping the blood pressure at less than the 90th
with principles of management of children with
steroid sensitive nephrotic syndrome. Therapy needsto be individualized for each patient and optimal care
Hypovolemic shock:This complication can occur
will be achieved by combined inputs of the primary
due to unsupervised use of diuretics especially if
pediatrician and pediatric nephrologist. Further
accompanied by septicemia, diarrhea or vomiting.
revisions of these guidelines, indicating best current
The diagnosis is suggested by moderate to severe
practice, shall be periodically necessary.
abdominal pain, hypotension, tachycardia, coldextremities and poor capillary refill; hematocrit and
Annexure I
blood levels of urea and uric acid are elevated. Management consists of rapid infusion of normal
Members of the Review Committee
saline at a dose of 15-20 mL/kg over 20-30 minutes;this is repeated if clinical features of hypovolemia
Kamran Afzal, Jawaharlal Nehru Medical College,
persist. Infusion of 5% albumin (10-15 mL/kg) or
Aligarh; Indira Agarwal, Christian Medical College
20% albumin (0.5-1 g/kg) may be used in subjects
Hospital, Vellore; Vinay Agarwal, Max Hospital,
who do not respond despite two boluses of saline.
New Delhi; Uma Ali, Bai Jerbai Wadia Hospital forChildren, Mumbai; Sanjeev Bagai, Rockland
Corticosteroid side effects: Prolonged steroid
Hospital, New Delhi; Arvind Bagga, All India
therapy may be associated with significant side ef-
fects. Patients (if they can understand) and the par-
(Convenor); Sushmita Banerjee, Calcutta Medical
ents should be explained about the side effects of the
Research Institute, Kolkata; Ashima Gulati, All India
medications, including increased appetite, impaired
Institute of Medical Sciences, Delhi; Sanjeev Gulati,
growth, behavioral changes, risk of infections, salt
Fortis Hospital, New Delhi; Pankaj Hari, All India
and water retention, hypertension and bone deminer-
alization. All patients should be monitored for
(Secretary); Arpana Iyengar, St. John’s Medical
cushingoid features and blood pressure; six-monthly
College, Bangalore; OP Jaiswal, Sunder Lal Jain
record of height and weight, and yearly evaluation
Hospital, New Delhi; Rupesh Jain, Ekta Hospital for
for cataract should be done. Patients on prolonged
Children, Raipur; M Kanitkar, Armed Forces
(>3 months) treatment with steroids should receive
Medical College, Poona; Mukta Mantan, Maulana
daily supplements of oral calcium (250-500 mg
Azad Medical College, New Delhi; Kamini Mehta,
daily) and vitamin D (125-250 IU)(19).
Lilavati Hospital & Research Center, Mumbai;
Steroids during stress: Patients who have received Kumud Mehta, Jaslok Hospital & Research Center &
high-dose steroids for more than 2 weeks in the past
Bai Jerbai Wadia Hospital for Children, Mumbai; BR
year are at risk of suppression of the hypothalamo-
Nammalwar, Kanchi Kamakoti CHILDS Trust
pituitary-adrenal axis. These children require
Hospital, Chennai; Amitava Pahari, Apollo
supplementation of steroids during surgery,
Hospital, Kolkata; Saroj K Patnaik, No.12 Air Force
anesthesia or serious infections(26). Corticosteroids
Hospital, Gorakhpur; KD Phadke, St. John’s
are supplemented, as parenteral hydrocortisone
Medical College, Bangalore; PK Pruthi, Sir
at a dose of 2-4 mg/kg/day, followed by oral
Gangaram Hospital, New Delhi; Abhijeet Saha,
prednisolone at 0.3-1 mg/kg/day. This is given for the
Government Medical College, Chandigarh; VK
duration of stress and then tapered rapidly. Sairam, Sri Ramchandra Medical College, Chennai;Jayati Sengupta, AMRI Hospital, Kolkata; PrabhaCONCLUSIONS Senguttuvan, Institute of Child Health, Chennai
Recommendations on management of nephrotic
(Chairperson); Sidharth K Sethi, All India Institute of
syndrome, proposed in 2001, have been reexamined
Medical Sciences, New Delhi; Mehul Shah, Apollo
Hospital, Hyderabad; Jyoti Sharma, Bharti
Davin JC, Merkus MP. Levamisole in steroid-
Vidyapeeth Medical College, Poona; RN Srivastava,
sensitive nephrotic syndrome of childhood: the lost
Indraprastha Apollo Hospital, New Delhi; AS
paradise? Pediatr Nephrol 2005; 20: 10-14. Vasudev, Indraprastha Apollo Hospital, New Delhi;
Latta K, von Schnakenburg C, Ehrich JHH. A meta-
Anil Vasudevan, St. John’s Medical College,
analysis of cytotoxic treatment for frequently
Bangalore; and M Vijayakumar, Mehta Children’s
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