Malnutrition Clinical Trial
Official title:
Thalidomide for the Treatment of Malnutrition Inflammation Syndrome in Peritoneal Dialysis Patients: A Randomized Control Trial
Hypothesis In peritoneal dialysis (PD) patients, malnutrition, inflammation and
atherosclerotic cardiovascular disease commonly coexist. The triad has been coined the "MIA
syndrome". Proinflammatory cytokines, such as tumor necrosis factor-alpha (TNF-alpha), plays
a central role in the pathogenesis of the MIA syndrome. Thalidomide selectively inhibits the
production of TNF-alpha and represents a valuable anti-cytokine therapy.
Specific Aim To study the effect of thalidomide in attenuating or reversing malnutrition and
systemic inflammation in PD patients.
Research Plan
Design: Double-blinded randomised prospective placebo control trial. Setting: Renal unit of
a university teaching hospital. Subjects: Sixty prevalent PD patients with evidence of
malnutrition. Interventions: Patients will be randomised to receive either oral thalidomide
100 mg nocte or placebo.
Main outcome measures: Patients will be followed for 1 year. Nutritional parameters
including serum albumin, subjective global assessment, malnutrition-inflammation score,
normalised protein nitrogen appearance, fat-free edema-free body mass and anthropometry
measurements will be monitored. Systemic inflammatory markers such as serum C-reactive
protein and IL-6 will be assayed. Hospitalisation, cardiovascular events, and overall
patient survival will also be compared during study period.
Expected Outcome
Nutritional parameters and markers of systemic inflammation are expected to improve with
thalidomide therapy. The magnitude of improvement in nutrition, as well as patient
morbidity, will be compared with placebo.
In Hong Kong, 80% of end-stage renal failure patients are treated with PD. Malnutrition,
cardiovascular disease and systemic inflammatory response are all common in our clinical
practice. They are major causes of patient morbidity and mortality. As a readily available
anti-cytokine therapy, thalidomide may represent a valuable treatment of the MIA syndrome.
The proposed study will provide important insight on the clinical benefit of thalidomide
treatment in malnourished PD patients, which accounts for about one-third of our dialysis
population.
Overall study design
This is a single-center randomized placebo control study on 60 prevalent PD patients.
Recruitment phase will take up to 12 months, and the study phase will be 1 year. Study code
will only be revealed at the end of the study period or if patients develop serious adverse
reactions.
Patient selection
A randomized prospective study will be performed in 60 stable PD patients. Recruitment
criteria are:
A. clinically stable adult patients (18 to 80 years old) on PD; and
B. evidence of malnutrition:
1. overall subjective global assessment score < 5; or
2. malnutrition inflammation score > 9; or
3. serum albumin < 35 g/L C. written patient informed consent
Exclusion criteria are:
Patients who are planned to have elective living donor transplant within 6 months
Patients who are planned to transfer to other renal center within 6 months High
likelihood of early withdrawal from the study (e.g. myocardial infarction, severe or
unstable coronary disease, stroke, severe liver disease within 3 months) Active
infection or systemic inflammatory disease. Current malignant disease Pregnancy or
breast-feeding Women of childbearing potential with unreliable birth control methods
Known hypersensitivity to thalidomide
Baseline data including age, sex, underlying renal disease, presence of diabetes,
hepatitis B status, requirement of helper for dialysis procedure, PD regimen and
duration on dialysis are recorded.
Interventions
After initial evaluation in a screening visit at -4 week, patients will be randomly
assigned to receive either oral thalidomide 100 mg nocte or placebo. Thalidomide will
be obtained from Penn Pharmaceuticals Ltd (Gwent, UK) as 100 mg tablets, and prescribed
in accordance with the published guidelines for the clinical use and dispensing of
thalidomide [34]. There will be 30 patients on each arm of randomization. Dialysis
prescription will be changed only if there is clinical evidence of underdialysis. Both
patients and investigators will be blinded from the therapy during follow up
assessment. Side effects will be recorded and the drug will be discontinued when
clinically necessary.
Clinical follow up
Patients will be followed at at -4 (screening), 0, 4, 8, 12, 18, 24, 30, 36, 44 and 52
weeks. The following clinical data will be documented during each visit:
Body height and body weight Blood pressure Compliance to thalidomide by pill count
Compliance to dialysis exchange by direct questioning Skin itchiness score from 0 to
3+, as described previously [31]
Body-mass index and body surface area will be computed. The majority of patients will
be on three or four 2-liter exchanges per day. Blood pressure or edema are controlled
with standard anti-hypertensive agents and/or hypertonic dialysate.
Laboratory parameters
A full panel of biochemical parameters will be monitored:
Hemoglobin, plasma sodium, potassium, urea, creatinine, albumin, calcium, phosphate,
alkaline phosphatase, and alanine transaminase at -4, 0, 4, 8, 12, 18, 24, 30, 36, 44
and 52 weeks Fasting serum glucose, lipid and iron profile at 0, 24 and 52 weeks Serum
parathyroid hormone at 0 and 52 weeks Serum inflammatory markers at 0, 12, 24, 36 and
52 weeks
Inflammatory markers include serum C-reactive protein (CRP), interleukin-6 (IL-6),
leptin, adiponectin, tumor necrosis factor alpha (TNF-alpha) and fibrinogen levels, as
suggested by other groups [35-38].
Nutritional assessment
Nutritional status will assessed by subjective global assessment (SGA), comprehensive
malnutrition-inflammation score (MIS), normalized protein nitrogen appearance (NPNA),
serum albumin level, anthropometric lean body mass (LBM), and fat-free edema-free body
mass (FEBM).
SGA will be performed at -4, 0, 12, 24, 36 and 52 weeks by a single observer. The
4-item 7-point scoring system proposed by Enia et al [39] will be used. MIS will be
performed at -4, 0, 12, 24, 36 and 52 weeks. The calculation of MIS has been described
previously [40]. Briefly, MIS consists of 4 main parts and 10 components, all scored
from 0 (normal) to 3 (very severe). The total score ranges from 0 to 30.
FEBM and PNA will be measured by creatinine kinetics at 0, 24 and 52 weeks. A 24-hour
dialysate and urine collections will be performed. Total and peritoneal Kt/V are
determined by standard methods. Residual GFR is calculated as average of 24-hour
urinary urea and creatinine clearance. FEBM is calculated according to the formula of
Forbes and Brunining [41]. PNA is derived from the Randerson's formula [42]. It is
further normalized to standard body weight.
Anthropometric measurements will be performed at 0, 12, 24, 36 and 52 weeks by a single
observer. This include bicep, tricep, subscapular and supra-iliac skin fold thickness,
and midarm muscle circumference. Derived variables by anthropometric measurements,
including lean body mass (LBM) and percentage of body fat, will be computed by standard
formula [43].
Pulse wave velocity
Pulse wave velocity (PWV), an index of aortic stiffness, is measured using an automatic
computerized recorder at 0, 24 and 52 weeks. The results will be analyzed by the
Complior SP program (Artech Medical, France). Briefly, pressure-sensitive transducers
are placed over the neck (carotid artery), wrist (radial artery) and groin (femoral
artery) with the patient in the supine position on day of haemodialysis treatment
before putting patient to the dialysis machine. PWV of the carotid-femoral and
carotid-radial territory is calculated by dividing the distance between the sensors by
the time corresponding to the period separating the start of the rising phase of the
carotid pulse wave and that of the femoral and also the radial pulse waves. The
procedure takes 10 to15 seconds to complete. The test will be performed by the same
observer to eliminate effect of intra-observer variation.
Health-related quality of life
Patient acceptance and satisfaction will be assessed by the Chinese translation of
"Kidney Disease Quality of Life Short Form (KDQOL-SFTM), version 1.3", at 0 and 52
weeks.
Outcome
The major outcome measure is nutritional status, as detailed above. The schedule of
various tests is summarized in Appendix 2. Secondary outcomes include the followings:
Change in arterial pulse wave velocity Total number of days of hospital admission
during study period Composite cardiovascular end point: cardiovascular death, non-fatal
myocardial infarction or stroke, hospital admission for unstable angina, coronary
intervention, transient ischemic attack, or lower limb ischemia Number of episode of
peritonitis during study period All cause mortality
Transplantation, conversion to hemodialysis, recovery of renal function, and transfer
out of the unit will also be recorded.
4. Potential Outcomes
In Hong Kong, 80% of end-stage renal failure patients are treated with peritoneal dialysis
(PD). In 2004, there were over 3000 PD patients in Hong Kong. Malnutrition, cardiovascular
disease and systemic inflammatory state are all common in our clinical practice. They are
major causes of patient morbidity and mortality. The financial implication is considerable.
As a readily available anti-cytokine therapy, thalidomide may represent a valuable treatment
of the MIA syndrome. The proposed study will provide important insight on the clinical
benefit of thalidomide treatment in malnourished PD patients, which accounts for about
one-third of our dialysis population.
Data Analysis
Statistical analysis will be performed by SPSS for Windows software version 11.5 (SPSS Inc.,
Chicago, IL). All data will be expressed in mean +/- standard deviation unless otherwise
specified. Serial changes of nutritional parameters, dialysis adequacy, and inflammatory
markers will be compared to the baseline values by analysis of variance for multiple
measures (MANOVA). Serial change in residual GFR is examined by Wilcoxon's rank sum test
with Bonferroni's correction for multiple comparison because of skewed data. Nutritional
status and systemic inflammatory markers after one year will be compared between the 2
groups by Student's t-test for parametric data. Hospitalization and peritonitis rate between
the groups are compared by Kruskal-Wallis test because the data will be highly skewed.
Actuarial patient survival will be compared by logrank test with Kaplan-Meier survival
curves and treatment group as stratifying variable.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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