Transcript Slide 1

Drugs and Renal
Disease
Sue Ayers
Advanced Pharmacist Palliative
Medicine and Chronic Pain
April 2006
Overview
 Effects
of renal failure on ADME
 Renal Physiology
 Estimating Renal Function
 Dose Adjustment in Renal Impairment
 Principles of dialysis
 Drug dosing in dialysis
Effects of renal failure on ADME
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Adsorption –
If increased nausea and vomiting ? reduced adsorption
Metabolism
Liver metabolism not affected.
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Metabolism only significant in conversion of cholecalciferol to 1,25dihydroxycholecalciferol (25-OH group added in kidney )– use 1
alpha – hydroxycholecalciferol to supplement Vitamin D.
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Insulin metabolised in kidney so requirement may be lower.
Effects of renal failure on ADME
(continued)
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Distribution –
fluid changes - ascites or oedema - increases volume of
distribution, dehydration reduced volume of distribution. Only
clinically significant if Vd small (less than 50litres)
e.g. aminoglycosides or lithium
Reduction of plasma protein binding - (uraemia and other
accumulated waste products) or protein loss . Significance of
increased free drug once new Css reached?. (Diazepam, morphine,
phenytoin, levothyroxine and warfarin affected).
Digoxin displaced from skeletal muscle tissue binding sites by toxic
waste products – increased drug in plasma = decreased Vd and
hence lower loading dose needed (Loading dose = target
concentration x Vd)
Effects of renal failure on ADME
(continued)
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Elimination – most important factor in dose decisions
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Non-renal and renal clearance should be considered
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Fall in renal drug clearance = fall in functioning nephrons(50%
reduction ion GFR suggests a 50% decline in renal clearance)
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Need to reduce doses in renal impairment depends on renal
clearance, clearance of metabolites and potential toxic side effects,
or narrow therapeutic index
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General considerations – uraemic patients are often more
susceptible to adverse drug effects (GI bleeding on anticoagulants
or NSAIDs or increase Blood Brain Barrier permeability to hypnotics
http://www.nottingham.ac.uk/healthquest/sonet/rlos/bioproc/kidneydrug/index.html
The Nephron
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The major organ for the excretion of drugs is the KIDNEY. The functional unit of the
kidney is the nephron in which there are three major processes to consider:-
Glomerular filtration
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molecules of low molecular weight are filtered out of the blood,
unless they are tightly bound to large molecules such as plasma
protein or have been incorporated into red blood cells.
Clearance by filtration  fu x GFR
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The glomerular filtration rate normal range is 110 to 130 ml/min.
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About 10% of the blood which enters the glomerular is filtered.
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Inulin is readily filtered in the glomerular, and is not subject to tubular
secretion or re-absorption. Thus inulin clearance is equal to the
glomerular filtration rate.
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Although most drugs are filtered from blood in the glomerular the
overall renal excretion is controlled by what happens in the tubules.
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More than 90% of the filtrate is reabsorbed. 120 ml/min is 173 L/day.
Normal urine output is about 1 to 2 liter per day.
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Tubular secretion
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In the proximal tubule there is re-absorption of water and
active secretion of some weak electrolytes but especially
weak acids such as penicillins.
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There may be competitive inhibition of the secretion of
one compound by another. (e.g. inhibition of penicillin
excretion by competition with probenecid)
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Drugs or compounds which are extensively secreted,
such as p-aminohippuric acid (PAH), may have
clearance values approaching the renal plasma flow rate
of 425 to 650 ml/min, and are used clinically to measure
this physiological parameter
Tubular re-absorption
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In the distal tubule there is passive excretion and re-absorption of
lipid soluble drugs (non-ionized or in the unionized form).
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Many drugs are either weak bases or acids and therefore the pH of
the filtrate can greatly influence the extent of tubular re-absorption
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When urine is acidic- weak acid drugs tend to be reabsorbed.
Alternatively when urine is more alkaline, weak bases are more
extensively reabsorbed. Urine pH can vary from 4.5 to 8.0
depending on the diet
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In the case of a drug overdose it is possible to increase the
excretion of some drugs by suitable adjustment of urine pH e.g.
pentobarbital ( a weak acid) overdose it may be possible to increase
drug excretion by making the urine more alkaline with sodium
bicarbonate injection.
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Effective if the drug is extensively excreted as the unchanged drug .
If the drug is extensively metabolized then alteration of kidney
excretion will not alter the overall drug metabolism all that much.
Renal clearance
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Renal clearance can be used to investigate the mechanism of drug
excretion.
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If the drug is filtered but not secreted or reabsorbed the renal clearance will
be about 120 ml/min in normal subjects.
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If the renal clearance is less than 120 ml/min then we can assume that at
least two processes are in operation, glomerular filtration and passive
tubular re-absorption (total renal clearance < fu x GFR,)
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If the renal clearance is greater than 120 ml/min then active tubular
secretion must be contributing to the elimination process (total renal
clearance > fu x GFR)
It is also possible that all three processes are occurring simultaneously.
Renal clearance is then:-
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Estimating renal function - GFR
•Approximately 125mls/min in normal adult
•Cockcroft and Gault Equation:
Cl Cr (male) = 1.23 x (140 – age) x IBW
Serum creatinine (micromol/litre)
Cl Cr (female) = 1.04 x (140 – age) x IBW
Serum creatinine (micromol/litre)
• Accuracy poor if GFR< 20ml/min
• SeCr doubling is equivalent to halving of CrCl ( eg a rise
from 60 to 120 micromol/litre is potentially equal to the
loss of one kidney
•Smallchanges in low Se Cr are as significant as large
changes in already high Se Cr
Calculating Ideal Body Weight
IBW (male) = 50 + (2.3 x height in inches over 5 feet) kg
= (Height (cm) -154) x 0.9 +50
kg
IBW (female) = 45.5 + (2.3 x height in inches over 5 feet) kg
= (Height (cm) -154) x 0.9 +50
kg
GFRs (ml/min/kg) for various species:
 Cow
1.8
 Horse 1.7
 Human 1.8
 Sheep 2.0
 Goat
2.2
 Dog
4.0
 Rat
10.0
4vMDRD
(modification of diet in renal disease)
( eGFR )
• Best fit calculation required 6 variables, one of which was urinary urea
• needed an equation that required only serum measurements and easy
calculation,
• Used an equation which has 4 variables (with only a small loss of
accuracy)
4-variable MDRD =
186 x [Pcr X0.011312]-1. 154 x [Age]-0.203 x [0.742 female] x [1.212 black
race]
Dose Adjustments in Renal
Impairment
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Alter dose or dose interval or both
DRrf = DRn x ((1-Feu) + (Feu x RF))
where DRrf = dosing rate in renal failure
DRn = normal dosing rate
RF = extent of renal failure
= patient’s creatinine clearance (ml/min)
Ideal creatinine clearance (120ml/min)
Feu = fraction of drug normally excreted unchanged in the
urine
Dose Adjustments in Renal
Impairment (continued)
 Use
the most appropriate resource
(e.g. SPC or Renal Drug Handbook)
Ideal Drug in Renal Failure
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Less than 25% excreted unchanged in the urine
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No active (or toxic) metabolites
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Disposition unaffected by fluid balance changes
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Disposition unaffected by altered protein binding
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Response unaffected by altered tissue sensitivity
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Wide therapeutic range
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Not nephrotoxic
Dialysis (Renal Replacement Therapy)
 Remove
Toxins
 Remove
Excess Fluids
 Correct
acid/base balance
 Correct
electrolyte disturbance
General principles of dialysis
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Semi-permeable membrane
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Blood one side / dialysis fluid the other
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Method of delivering blood to membrane (pump)
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Method of delivering dialysis fluid/removing
excess water and waste products (pump or PD
catheter
Passage through the semipermeable membrane (SPM)
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Diffusion – Passage of SOLUTE from a high
concentration to a low concentration through a SPM (ie
in haemodialysis waste out Ca and HCO3 in)
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Ultrafiltration – passage of FLUID under pressure (+ve
or –ve ) across a SPM
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In Haemodialysis/haemofiltration pressure is hydrostatic
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In Peritoneal Dialysis pressure is osmotic
Haemodialysis
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Blood is drawn through the artificial kidney
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Dialysis fluid is perfused around the SPM filaments in the artificial
kidney – never coming into contact with blood directly
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Solutes are cleared by diffusion
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Calcium and Bicarbonate may be replaced in ECF across the
diffusion gradient
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Excess fluid is removed by ultrafiltration under control of dialysis
machine
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Can be intermittent or continuous
Peritoneal Dialysis
 PD
fluid is introduced into peritoneal cavity
and “dwelled” for a specific time, drained
and replaced
 Diffusion and ultrafiltration takes place
across the SPM
 Ultrfiltration is controlled by concentration
of glucose in PD fluid
 Intermittent (Acute) or Continuous
Haemofiltration
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Blood is drawn through artificial kidney and ECF
is removed by ultrafiltration.
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ECF is replaced with haemofiltration fluid –rate
controlled to lead to overall fluid removal
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Solute clearance is achieved by convection
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Can be intermittent (mainly to remove fluid if
overloaded) or continuous in sicker patients
Haemodiafiltration
 Combined
techniques of dialysis by
diffusion and filtration which removes
solutes by convection.
 Dialysate is haemofiltration or peritoneal
dailysis solution and transmembrane
pressure is ajusted to remove solutes or
water
Approximate clearance of dialysis
systems
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Intermittent Haemodialysis
 Intermittent Haemofiltration
 Acute Intermittent PD
 CAPD
 Continuous haemofiltration
 Continuous Haemodiafiltration
150 – 200ml/min
100 - 150ml/min
10 - 20ml/min
5 - 8ml/min
5 - 15ml/min
15 - 25ml/min
Factors Affecting Drug removal
during dialysis
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molecular size, steric hindrance
protein binding,
volume of distribution,
water solubility,
plasma clearance.
technical aspects of dialysis procedure (Surface
area of membrane,Blood flow rate,Dialysate flow
rate,dialysis time (HD),Dialysate volume (PD) )
Molecular Weight
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Dialytic membrane pore size - synthetic membrane or
natural (CAPD)
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Size vs pore size
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Pore size of the peritoneal membrane is assumed to be
larger than that of a HD membrane.
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MW > 1,000 daltons “seived” ,< 1,000 “diffuse”
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Heamodiafiltration removes 10% more middle molecules
(500 – 5,000 daltons) than heamodialysis and 24%
more > 5,000 daltons
Protein Binding and dialysis
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Concentration gradient of unbound (free) drug across the dialysis
membrane is important
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High degree of protein binding = low plasma conc. of unbound drug
available for dialysis.
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Uremia may decrease protein binding
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If significant, increased dialyzability of free drug may occur.
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In peritonitis Increased protein concentrations often occur in
peritoneal effluent
Volume of distribution and dialysis
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A drug with a large Vd is distributed widely throughout
tissues and has relatively small amounts in the blood.
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Factors that contribute to a large Vd include high lipid
solubility and low plasma protein binding.
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Drugs with a large volume of distribution are likely to be
dialyzed minimally.
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Conversely, highly water soluble drugs are likely to be
more easily dialysable
Plasma Clearance
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The inherent metabolic clearance = sum of renal and
non-renal clearance ( "plasma clearance“)
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In dialysis patients, renal clearance is largely replaced by
dialysis clearance.
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If non-renal clearance is large vs renal clearance,
contribution of dialysis to total drug removal is low.
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If renal (and hence dialysis) clearance is >30% more,
dialysis clearance is considered to be clinically
Important.
Digoxin
 Molecular
weight 750
 Protein binding 20%
 Water soluble
 ? Is it well dialysed
 No – Vd is 7litres/kg – total body clearance
low as most of drug not available to be
dialysed
Dose Adjustment for Renal
Replacement Therapy
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Only required for drugs that already need dose
adjustment in renal failure
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Supplementation rarely needed, even if removed - give
after intermittent techniques
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Dose drugs requiring TDM by blood levels rather than
computer models and nomograms
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Use recognised resources
Dose Adjustment for Renal
Replacement Therapy (continued)
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Always aim to give drugs at the end of any
session of intermittent dialysis or filtration
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For continuous RRT dose according to the SPC
recommendations for the estimated CrCl of the
dialysis system
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Never give more than doses recommended in
patients with normal renal function
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Discuss doses with an experienced colleague