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‫الرحيم‬ ‫الرحمن‬ ‫هللا‬ ‫بسم‬
Water treatment for HD Unit
DR Samir Sally, MD
Consultant Internal Medicine & Nephrology,
MUNC, Mansoura University, Egypt
•
1940 1960 today
THE UNDENIABLE TECHNOLOGICAL PROGRESS IN DIALYSIS
Mission
Vision
Goals
Our Mission
• To serve our community at all levels by
providing health care services through a
multidisciplinary team approach at highest
international standards covering all aspects of
Hemodialysis
Our Vision
• To be one of the best recognized Health Care
providers not only at local or national level but
internationally too
Our Core Values
• Focus on patient safety
• Focus on Staff safety
• More and more education for the patients
• More and more education for the staff
• Confidentiality & Respect to patients and staff
alike
Manual of Hemodialysis
Policies and Procedures
Purpose
Policy Statement
Definition
Procedure
Forms/Attachments/Flowcharts
Material/Equipment
Review History
Reference
Approval
Manual of HD
• Policies and procedures (patient related)
1-Dialysis request and patient specific care
2-Assessment of medical status of patient
3-Iniating & discontinuing dialysis treatment
4-Nursing care during dialysis
5-Fluid management of dialysis
6-Intravenous drug administration
7-Anticoagulant regimens
Manual of HD
8-Diagnostic testing including frequency
9-Managing vascular access
10-Adequacy of dialysis
11-Code blue arrest protocols
12-Management of complications ( CPG)
13-Dialyzer selection and priming
14-Water treatment & monitoring of quality
15-preperation and monitoring of Dialyzate
Manual of HD
• Infection Control
1-immunization guidelines
2-Infection prevention:
A- Cleaning procedures
B-Hand Washing
C-Handling of infectious waste
D- Handling of infected/contagious patient
Manual of HD
• Equipment
1-Operating and service manual
2-Record of repair
Dress code in the treatment area
Manual of HD
• Safety
1-General safety
2-Infection Control
3-Storing & handling of hazardous wast
4-Electrical safety
5-Fire safety
6-Needle injury with contaminated item
7- Staff immuization
Manual of HD
• House keeping: Daily, weekly and monthly
1- Standard precautions
2-Transport of soiled materials
3-Soap/detergent/antiseptic use and dispensing
Regular investigations and action plan
• Monthly
Creatinine,BUN,URR,Na,K,Ca,Po4,ALT,Albumin,
Glucose,CBC
• Every 3 months
Iron pannel
Viral screening
• Every 6 months
Lipid profile
PTH
Towards better quality of HD
Better quality of HD
We suggest that machines should be replaced
after between seven and ten years’ service or
after completing between 25,000 and 40,000
hours of use for haemodialysis, depending
upon an assessment of machine condition.
(2C)
Multidisciplinary Team
Pt. and Family Educator
1-Awarness about kidney failure
2-Choice of RRT ( HD,PD,TX)
3-Compliance with dietary and fluid instructions
and restrictions
4-Compliance with medication instruction and
dialysis treatment prescription and schedule
5- Significance of Lab test results
Pt. and Family Educator
6-Importance of caring vascular access
7-Importance of good hygiene and infection
control
8-Awarness, prevention and management of
HTN,renal bone disease, sexual and
Psychological effects of RF on patients and their
families
Social Worker
1-Discuss medical condition of the patient with
doctors and nurses
2-Provide emotional and psychological support
for new patients and families
3-Evaluate home situation
Renal Dietitian
1-Nutritional assessment and reassessment
2-Current malnutrition related to renal failure
3-Diet history and eating habits
4-Explain relation of lab values to the food
5-Review food and fluid intake
6-Educate medical staff on renal nutrition
7-Food drug interaction
Bio Med
1-Disinfection of water treatment unit and
portable
RO
2-Daily TDS, conductivity and PH
3-Checking all machines maintenance and
contact
with the manufacturing companies
4-Awarness of all AAMI standards
5-Check free chlorine or chloramine test
Pharmacists
1-Chart review
2-Drug related problems
3-Contribute to resolution of drug related
problems
4-Educate pt as needed
5-Review blood work
Vascular access
Vascular access
65% of all patients commencing haemodialysis
should commence with an AV fistula
85% of all prevalent patients on HD should
receive dialysis via a functioning AVF
Vascular access planning should commence on
CKD stage 4. (2C)
Vascular access
AVF should be placed as a minimum at three
months prior to the commencement of
haemodialysis and probably not more than
one year from the expected date of dialysis.
In individuals in whom an AV graft is deemed
to be the appropriate access, placement can
be delayed until a time closer to the expected
date of dialysis.
Vascular access
Tunneled catheters should be preferred in all
patients..
We recommend that venous catheters should be
removed in all seriously ill haemodialysis
patients with catheter related bacteraemia
unless no alternative vascular access can be
achieved. (1B)
Vascular access
Catheter related bacteraemia episodes are
relatively common – the incidence is reported at
between 1-10/1000 patient days
Higher rates of mortality and morbidity related
to an increased incidence of metastatic infection
(e.g. discitis, endocarditis).
Introduction
• Survival of HD patients is steadily improving
• Water treatment for preparation of dialysate is
probably the most neglected area of RRT with
dialysis
• Quality of water contributes very significantly in
acute and long term morbidity and prognosis
Introduction
• Dialysis staff should have a fundamental understanding of
water pre-treatment for haemodialysis
• Written policies, practices and procedures shall be in place
for the safe operation of dialysis water pre-treatment systems
• All servicing, maintenance, interventions and changes to the
water pre-treatment plant, as a minimum, shall be recorded
in an on-site log book
Introduction
The worst way to hurt patients is through the
water system, so it is expected that you know
what is going on.
Exposure to Water and Contaminants
Average Population
• Drinks approximately 14
L/week (2L/day)
• Able to excrete toxic
substances in urine
• Contaminants
selectively absorbed in
GI tract, indirectly
exposed to blood
Hemodialysis Patient
• Exposed to
approximately 360 Lw
• Kidneys unable to
excrete toxic substances
• Contaminants directly
exposed to blood via
dialyzer membrane
Weekly Water Exposure
Water supply
There are 2 sources of municipal water:
• Surface water is generally more contaminated
with organisms and microbes, industrial
wastes, fertilizers, and sewage.
• Ground water is generally lower in organic
materials but contains higher inorganic ions
such as iron, ca, mg and sulfate
Toxic effects of water contaminants in HD
Contaminant Possible effects
Aluminum Dialysis encephalopathy, renal bone disease
Calcium, Magnesium Hard water syndrome, hypertension,
hypotension
Chloramine Hemolysis, anemia, methameglobinemia
Copper Nausea, headache, liver damage, fatal hemolysis
Fluoride Osteomalacia, osteoporosis
Sodium Hypertension, pulmonary edema, confusion,
headache, seizures, coma
Microbial Pyrexia reactions, chills, fever, shock
Nitrate Methmeglobinemia, hypotension, nausea
High iron Hemosiderosis
Sulfate Nausea, vomiting, metabolic acidosis
Zinc Anemia, vomiting, fever
Aromatic hydrocarbons Potential chemical carcinogens
Progressive Dialysis Encephalopathy from Dialysate
Aluminium
Arch Intern Med V138, 1978
• 8 cases of fatal dialysis encephalopathy
observed in 22 months (38% of all patients)
• Coincided with addition of Al SO4 and Na
aluminate to city water resulting in dialysis
fluid Al concentration of 200-1000 ug/l
• The outbreak ended after installation of
deionizer that reduced dialysis fluid Al to < 1
ug/l
• “Philadelphia Incident” of 1987. Initially, a nurse in the facility noticed an
unusually large number of hematocrit values that were lower than normal.
• Forty-four patients out of 107 required transfusions, and 10 were sent to
the emergency department for additional treatment.
• Upon further investigation, The staff person monitoring the system
recorded the chloramine levels accurately as they climbed to toxic levels
(AAMI maximum level is 0.1 mg/L), but the staff member was not aware
that this was a dangerous situation and did not report it to a supervisor.
• Further, no written policy was in place regarding the testing of total
chlorine levelsThis incident illustrates the need for staff education
Arnow PM et al. An outbreak of fatal fluoride intoxication in a
long-term hemodialysis unit. Ann Intern Med 1994;121:339-
344.
• On 16 July 1993, 12 patients treated at a long-term HD unit in
Chicago became ill during or soon after HD.
• The patients experienced symptoms of severe pruritus,
headache, nausea, and chest or back pain.
• Three patients arrested and died due to ventricular fibrillation
after completion of dialysis that day.
• Subsequent investigations found that fluoride was released
from the deionization system after the ion exchange resin
inside was exhausted.
• The investigator concluded that the incident was caused by
errors in maintenance of the deionization system
• In February 1996, Caruaru,Brazil, 116 (89%) of 131
patients experienced visual disturbances, nausea,
vomiting, and muscle weakness, following routine HD
treatment. Subsequently, 100 patients developed acute
liver failure. As of December 1996, 52 deaths occurred.
• Two groups of hepatotoxic cyanotoxins were idnetified:
microcystins, specifically microcystin-YR, -LR and -AR.
• The outbreak occurred in one of two HD units using same
water source
Water treatment system
1.Feed Water Components: (Back-flow preventer, Temperature
blending valve, booster pump and raw water tank, ±acid feed
pump )
2.Pre-treatment section: (filters, activated carbon and softner).
3.Treatment section: (reverse osmosis).
4.Post-treatment section: (microbial and UV filters or/and
deionization)
5.the distribution system: piping, valves, pumps, ±storage tanks
• An indication of mineral deposits forming on the membrane will be high readings
of total dissolved solids (TDS), percent rejection and conductivity (or low
resistivity).
• In feed water classified as being very hard, damage to the RO membrane may
occur extremely rapidly, even within hours, with irreversible membrane damage
• So the softener is placed before the reverse osmosis (RO) unit to protect the RO
membrane.
• Analysis of the level of calcium carbonate (CaCO3) in the feed water is important
for determining the size of the softener.
Schematic diagram example of a water
treatment system for hemodialysis
Back flow preventer: inhibits flow
back of treated water into
municipal water
Temperature blending valve:
brings water to a standard
temperature of 25 oC for
proper function of RO system
Booster pump: maintains adequate
flow and pressure of water
so the system operates
successfully.
Acid feed pump
• By increasing the pH of the city water supply using
lime softening agents or Ca CO3 prevent leaching of
lead, copper from the piping system
• For proper function of RO and carbon tanks,
incoming water pH should be between 5-8.5
• A pH higher than 8.5 with chloramines present will
cause the carbon to be less adsorptive and the RO
membrane performance to degrade, resulting in
poor water quality.
Purification Processes
Process Contaminant
Carbon Adsorption Chloramine, organics
Softener Calcium, Mg
Reverse osmosis Inoic contaminants, bacteria,
endotoxin
Deionization Ionic contaminants
Ultrafiltration Bacteria, endotoxin
Multimedia depth filter
• Large particulates of >10
microns such as dirt, are
removed by a multimedia
depth filter.
• Floculants can clog the carbon
and softener tanks, destroy the
RO pump, and foul the RO
membrane
• Contain multiple layers of
various sized rocks that trap the
large particles as the water
filtered downward
Carbon Tank
• Removes chlorine and
chloramine
• These are high level
oxidative chemicals.
They are added to
municipal water
systems to kill bacteria,
but they also cause
hemolysis
Carbon filter
•As the input water flows down through the granular activated
carbon (GAC), solutes diffuse from the water into the pores of the
carbon and become attached to the structure.
•A 10-minute exposure time of the water through the carbon
tanks to reduce chlorine to at least 0.5 mg/L and the chloramine
to be adsorbed to at least 0.1 mg/L.
A wide variety of naturally occurring and synthetic organic
compounds, such as herbicides, pesticides, and industrial
solvents, will be adsorbed as well
Water Softener
• Water containing Ca and Mg
form deposits on RO
membrane
• Softeners work on ion
exchange basis. The resin
beads within the tank have a
high affinity for the cations Ca
and Mg (divalents) present in
the source water and release
2 sodium ions (monovalent)
for one Ca or Mg captured
Hardness of water
• Calcium carbonate Classification
• 0–60 mg/L Soft
• 61–120 mg/L Moderately hard
• 121–180 mg/L Hard
• Greater than 180 mg/L Very hard
Water Softener
• The softener needs regenerating on a routine
basis with concentrated NaCl solution (brine)
before the resin capacity is used up
• The resin is backwashed to loosen the media
and clean any particulates from the tank. After
the backwashing step, the brine solution is
drawn into the tank
Reverse Osmosis system
• RO overcomes natural osmosis by forcing feed
water under pressure thru a semi-permeable
membrane leaving contaminants behind (ions,
organics)
Reverse osmosis
•Reverse osmosis (RO) uses high pressure to force water across a
semipermeable membrane, thereby rejecting
90 to 99 percent of ionic compounds and
>95 percent of nonionic contaminants,
also it is an effective barrier against microbiological contaminants,
including bacteria, viruses, and endotoxin.
Ion exchange deionizers (DI)
DI use a two-stage process to remove virtually all ionic material
remaining in pretreated water.
Two types of synthetic resins are used; one to remove positively
charged ions (cations) and another to remove negatively charged
ions (anions).
•Although deionizers produce water of very high purity with
respect to ionic contaminants, they do not remove
microbiological contaminants.
•Therefore, it is necessary to incorporate bacterial control
equipment after the application of a deionizer.
Ultraviolet filter
The mechanism of microorganism destruction is currently
believed to be that ultraviolet causes molecular rearrangements
in DNA and RNA, which in turn blocks replication.
•As the UV kills the bacteria, it may increase the level of
endotoxinas a result of the destruction of the gram-negative
bacteria (endotoxin producing) cell wall
Bacterial filters
Distribution system
• RO distribution systems: direct feed and
indirect feed
• Direct feed: directly delivers the product water
from the RO unit to the loop for distribution
• Indirect feed: involves a storage tank that
accumulates the product water and delivers to
the distribution loop
• Unused portions are recirculated back into the
storage tank
Microbiological aspects of fluid system
design
• use of a recirculation-type system,
• avoidance of dead ends and dead space areas,
• use of materials compatible with the planned methods of
disinfection
• avoidance of storage tanks. If a storage tank is necessary it
should be cleaned and disinfected.
• The disinfection program could prevent the formation of
biofilm, which can become difficult to eradicate.
Ultrapure dialysis solution
• Decreases CRP and IL-6
• Improves response to EPO
• Promotes better nutrition
• Reduces plasma levels of ß-2-microglobulin
• Slows loss of residual renal function
• Lowers cardiovascular morbidity
• Bacteria level below 0.1 cfu/ml and
endotoxin level below 0.03 EU/ml
Susantitaphong P et al. Effect of ultrapure dialysate on markers of inflammation, oxidative stress,
nutrition and anemia parameters: a meta-analysis. NDT (2013) 28: 438-446
Water treatment unit
TDS, and conductivity daily
Microbiological culture and endotoxin assay.
Monthly
Chemical assay every 6 months
Water treatment unit
• There is no limit for RO product TDS/conductivity.
• Values that are acceptable in one location may not be
acceptable in another location.
• TDS in some areas of 50 ppm is acceptable and other areas
where 10 ppm is NOT acceptable. It all depends on your raw
water.
• A slight change in the amount of Fluoride injected into the
water can cause the RO product water to go less than a 1 ppm
TDS increase.
Bacteriological Monitoring:
• The maximum level of bacteria in water used
to prepare dialysis fluid must not exceed the
AAMI standard of 100 CFU. The AAMI action
level is 50 CFU
• An action level is defined as a point when
measures must be taken to correct the
potential source to remain in compliance with
AAMI standards
Endotoxin standard
• The maximum level of endotoxin in water
used to prepare dialysis fluid must not exceed
the AAMI standard of 0.25 Endotoxin Units/
ml (EU/ml)
• The action level of endotoxin is 0.125 EU/ml
Contaminant Maximum
Concentration mg/L
Test Methodology
Calcium 2 (0.1 mEq/L) EDTA or Atomic Absorption
Magnesium 4 (0.3 mEq/L) Atomic Absorption
Potassium 8 (0.2 mEq/L) Atomic Absorption, or Flame Photometri
Sodium 70 (3.0 mEq/L) Atomic Absorption or Flame Photometric
Antimony 0.006 Atomic Absorption (platform)
Arsenic 0.005 Atomic Absorption (gaseous hydride)
Barium 0.10 Atomic Absorption (electrothermal)
Beryllium 0.0004 Atomic Absorption (platform)
Cadmium 0.001 Atomic Absorption (electrothermal)
Chromium 0.014 Atomic Absorption (electrothermal)
Lead 0.005 Atomic Absorption (electrothermal)
Mercury 0.0002 Flameless Cold Vapor (Atomic
Absorption)
Contaminant Maximum Concentration
mg/L
Test Methodology
Selenium 0.09 Atomic Absorption (gaseous, or
electrothermal)
Silver 0.005 Atomic Absorption (electrothermal)
Aluminum 0.01 Atomic Absorption (electrothermal)
Chloramines 0.10 DPD Ferrous Titrimetric Method
Total chlorine 0.50 DPD Ferrous Titrimetric Method
Copper 0.10 Atomic Absorption (direct aspiration)
Fluoride 0.20 Ion Selective Electrode Method
Nitrate (as N) 2.00 Cadmium Reduction Method
Sulfate 100.00 Turbidimetric Method
Thallium 0.002 Atomic Absorption (platform)
Zinc 0.10 Atomic Absorption (direct aspiration)
Association for the Advancement of Medical Instrumentation. Dialysate for hemodialysis
(ANSI/AAMI RD52:2004).Arlington (VA). American National Standard. 2004
Water treatment unit
A programme of improvement should begin
immediately if routine monitoring
demonstrates that concentrations of chemical
contaminants exceed the maximum allowable
limits of AAMI. (1B)
Disinfection
General
• Disinfection schedules should be designed to prevent
bacterial proliferation, rather than being designed to
eliminate bacteria once they have proliferated to an
unacceptable level (i.e. above the action level).
• A proper disinfection strategy is to be preventive and
this should be applied from the start of operation.
Disinfection
• Disinfection of the distribution piping systems.
• 1- Chemical disinfection
• 2- Hot water disinfection When used to control bacterial
proliferation (minimum distribution loop temp 60 oC).
• Heat disinfection will not remove established biofilms, but is
convenient, requires little rinse time and can thus be used
more often to prevent biofilm formation. An occasional
chemical disinfection might still be necessary.
Testing of samples
• Testing of water samples shall be carried out by
trained and accredited persons or accredited
laboratories.
• The dialysis unit shall maintain records of persons
who have been trained and accredited and full
details of accredited laboratories.
• The records shall be maintained within the dialysis
unit.
Sample collection
• Water sample sites
• Samples are to be taken at outlets of the water distribution system.
• Prior to sampling, the inside of the outlet can be disinfected, especially if no hemodialysis
machine is attached. The reason for such disinfection is that, over time, residual water in an
outlet will support microbial growth. The disinfection can be made by flushing the inside of
the outlet with 70 % ethanol or iso-propanol. A sterile cotton swab wetted with alcohol can
also be used. Exposure time is to be >15 s.
• It is sufficient to let out enough water to rinse off the alcohol (200 ml to 500 ml) prior to
sampling.
• Alternatively, hoses can be disconnected from the tap and the taps opened and allowed to
flush for 2 min to 3 min before aseptically collecting a sample.
• Sample for cultivation and endotoxin analysis: Sample volume 5 ml to 1,000 ml or volume as
specified by the laboratory..
Sample collection
• Dialysis fluid samples
• Dialysis fluid samples should be collected from a sampling port prior to the
dialyzer. The sample port should be designed to minimize the likelihood of
contaminating the sample and should be capable of being effectively disinfected.
• Many dialysis machines are equipped with dialysis fluid sample ports that can be
accessed using a syringe. These sample ports may be disinfected with 70 %
ethanol or iso-propanol and allowed to air dry.
• A sterile syringe (20 ml or larger) should then be used to aspirate dialysis fluid out
of and into the port before filling the syringe. The filled syringe should then be
discarded and a fresh sample of dialysis fluid collected using a new sterile syringe.
• Sample for cultivation and endotoxin analysis: Sample volume 5 ml to 1,000 ml or
a volume as specified by the laboratory. Containers for samples to be cultured
should be sterile and containers for samples to be tested for endotoxins should be
sterile and endotoxin-free.
Storage of samples
• Heterotrophic plate count
• Storage of samples
• Microbial analysis of water and dialysis fluid samples should be conducted
as soon as possible after collection to avoid unpredictable changes in the
microbial population. If samples cannot be analyzed within 4 h of
collection, follow the laboratory's instructions for shipping. Samples
intended for colony counts should not be frozen.
• Storage of samples for endotoxin analysis may be different from what is
given above, provided the complete procedure follows the
manufacturer's instructions for use of the LAL assay.
Conclusion
• Water treatment is a generally neglected area of dialysis
therapy
• Quality of water contributes very significantly in acute and
long term morbidity and prognosis
• Due to increased survival of dialysis patients, increased use of
bicarbonate dialysate and high flux membranes, water
treatment has become essential
• It is worthwhile achieving the goal of sterile, pyrogen free and
chemically pure water for dialysis
Conclusion
• Written policies, practices and procedures shall be in place
• AAMI standards are the accepted minimum standards for
water pre-treatment for haemodialysis.
Each unit should have standard operating procedures in place
for sampling, monitoring and recording of feed and product
water quality
• All servicing, maintenance, interventions and changes to the
water pre-treatment plant shall be recorded.
.
Conclusion
• Medical directors who learn, know, and embrace the
requirements for providing high-quality dialysis
water will be most successful in this task.
• Medical, nursing and technical staff working in
dialysis units share responsibility for the safe
operation of the water pre-treatment plant and shall
participate together in regular multidisciplinary
committee meetings to review the safe operation of
the water pre-treatment plant and RO water plant.
Water treatment

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Water treatment

  • 2. Water treatment for HD Unit DR Samir Sally, MD Consultant Internal Medicine & Nephrology, MUNC, Mansoura University, Egypt
  • 3. • 1940 1960 today THE UNDENIABLE TECHNOLOGICAL PROGRESS IN DIALYSIS
  • 5. Our Mission • To serve our community at all levels by providing health care services through a multidisciplinary team approach at highest international standards covering all aspects of Hemodialysis
  • 6. Our Vision • To be one of the best recognized Health Care providers not only at local or national level but internationally too
  • 7. Our Core Values • Focus on patient safety • Focus on Staff safety • More and more education for the patients • More and more education for the staff • Confidentiality & Respect to patients and staff alike
  • 9. Policies and Procedures Purpose Policy Statement Definition Procedure Forms/Attachments/Flowcharts Material/Equipment Review History Reference Approval
  • 10. Manual of HD • Policies and procedures (patient related) 1-Dialysis request and patient specific care 2-Assessment of medical status of patient 3-Iniating & discontinuing dialysis treatment 4-Nursing care during dialysis 5-Fluid management of dialysis 6-Intravenous drug administration 7-Anticoagulant regimens
  • 11. Manual of HD 8-Diagnostic testing including frequency 9-Managing vascular access 10-Adequacy of dialysis 11-Code blue arrest protocols 12-Management of complications ( CPG) 13-Dialyzer selection and priming 14-Water treatment & monitoring of quality 15-preperation and monitoring of Dialyzate
  • 12. Manual of HD • Infection Control 1-immunization guidelines 2-Infection prevention: A- Cleaning procedures B-Hand Washing C-Handling of infectious waste D- Handling of infected/contagious patient
  • 13. Manual of HD • Equipment 1-Operating and service manual 2-Record of repair Dress code in the treatment area
  • 14. Manual of HD • Safety 1-General safety 2-Infection Control 3-Storing & handling of hazardous wast 4-Electrical safety 5-Fire safety 6-Needle injury with contaminated item 7- Staff immuization
  • 15. Manual of HD • House keeping: Daily, weekly and monthly 1- Standard precautions 2-Transport of soiled materials 3-Soap/detergent/antiseptic use and dispensing
  • 16. Regular investigations and action plan • Monthly Creatinine,BUN,URR,Na,K,Ca,Po4,ALT,Albumin, Glucose,CBC • Every 3 months Iron pannel Viral screening • Every 6 months Lipid profile PTH
  • 18. Better quality of HD We suggest that machines should be replaced after between seven and ten years’ service or after completing between 25,000 and 40,000 hours of use for haemodialysis, depending upon an assessment of machine condition. (2C)
  • 20. Pt. and Family Educator 1-Awarness about kidney failure 2-Choice of RRT ( HD,PD,TX) 3-Compliance with dietary and fluid instructions and restrictions 4-Compliance with medication instruction and dialysis treatment prescription and schedule 5- Significance of Lab test results
  • 21. Pt. and Family Educator 6-Importance of caring vascular access 7-Importance of good hygiene and infection control 8-Awarness, prevention and management of HTN,renal bone disease, sexual and Psychological effects of RF on patients and their families
  • 22. Social Worker 1-Discuss medical condition of the patient with doctors and nurses 2-Provide emotional and psychological support for new patients and families 3-Evaluate home situation
  • 23. Renal Dietitian 1-Nutritional assessment and reassessment 2-Current malnutrition related to renal failure 3-Diet history and eating habits 4-Explain relation of lab values to the food 5-Review food and fluid intake 6-Educate medical staff on renal nutrition 7-Food drug interaction
  • 24. Bio Med 1-Disinfection of water treatment unit and portable RO 2-Daily TDS, conductivity and PH 3-Checking all machines maintenance and contact with the manufacturing companies 4-Awarness of all AAMI standards 5-Check free chlorine or chloramine test
  • 25. Pharmacists 1-Chart review 2-Drug related problems 3-Contribute to resolution of drug related problems 4-Educate pt as needed 5-Review blood work
  • 27. Vascular access 65% of all patients commencing haemodialysis should commence with an AV fistula 85% of all prevalent patients on HD should receive dialysis via a functioning AVF Vascular access planning should commence on CKD stage 4. (2C)
  • 28. Vascular access AVF should be placed as a minimum at three months prior to the commencement of haemodialysis and probably not more than one year from the expected date of dialysis. In individuals in whom an AV graft is deemed to be the appropriate access, placement can be delayed until a time closer to the expected date of dialysis.
  • 29. Vascular access Tunneled catheters should be preferred in all patients.. We recommend that venous catheters should be removed in all seriously ill haemodialysis patients with catheter related bacteraemia unless no alternative vascular access can be achieved. (1B)
  • 30. Vascular access Catheter related bacteraemia episodes are relatively common – the incidence is reported at between 1-10/1000 patient days Higher rates of mortality and morbidity related to an increased incidence of metastatic infection (e.g. discitis, endocarditis).
  • 31. Introduction • Survival of HD patients is steadily improving • Water treatment for preparation of dialysate is probably the most neglected area of RRT with dialysis • Quality of water contributes very significantly in acute and long term morbidity and prognosis
  • 32. Introduction • Dialysis staff should have a fundamental understanding of water pre-treatment for haemodialysis • Written policies, practices and procedures shall be in place for the safe operation of dialysis water pre-treatment systems • All servicing, maintenance, interventions and changes to the water pre-treatment plant, as a minimum, shall be recorded in an on-site log book
  • 33. Introduction The worst way to hurt patients is through the water system, so it is expected that you know what is going on.
  • 34. Exposure to Water and Contaminants Average Population • Drinks approximately 14 L/week (2L/day) • Able to excrete toxic substances in urine • Contaminants selectively absorbed in GI tract, indirectly exposed to blood Hemodialysis Patient • Exposed to approximately 360 Lw • Kidneys unable to excrete toxic substances • Contaminants directly exposed to blood via dialyzer membrane
  • 36. Water supply There are 2 sources of municipal water: • Surface water is generally more contaminated with organisms and microbes, industrial wastes, fertilizers, and sewage. • Ground water is generally lower in organic materials but contains higher inorganic ions such as iron, ca, mg and sulfate
  • 37. Toxic effects of water contaminants in HD Contaminant Possible effects Aluminum Dialysis encephalopathy, renal bone disease Calcium, Magnesium Hard water syndrome, hypertension, hypotension Chloramine Hemolysis, anemia, methameglobinemia Copper Nausea, headache, liver damage, fatal hemolysis Fluoride Osteomalacia, osteoporosis Sodium Hypertension, pulmonary edema, confusion, headache, seizures, coma Microbial Pyrexia reactions, chills, fever, shock Nitrate Methmeglobinemia, hypotension, nausea High iron Hemosiderosis Sulfate Nausea, vomiting, metabolic acidosis Zinc Anemia, vomiting, fever Aromatic hydrocarbons Potential chemical carcinogens
  • 38. Progressive Dialysis Encephalopathy from Dialysate Aluminium Arch Intern Med V138, 1978 • 8 cases of fatal dialysis encephalopathy observed in 22 months (38% of all patients) • Coincided with addition of Al SO4 and Na aluminate to city water resulting in dialysis fluid Al concentration of 200-1000 ug/l • The outbreak ended after installation of deionizer that reduced dialysis fluid Al to < 1 ug/l
  • 39. • “Philadelphia Incident” of 1987. Initially, a nurse in the facility noticed an unusually large number of hematocrit values that were lower than normal. • Forty-four patients out of 107 required transfusions, and 10 were sent to the emergency department for additional treatment. • Upon further investigation, The staff person monitoring the system recorded the chloramine levels accurately as they climbed to toxic levels (AAMI maximum level is 0.1 mg/L), but the staff member was not aware that this was a dangerous situation and did not report it to a supervisor. • Further, no written policy was in place regarding the testing of total chlorine levelsThis incident illustrates the need for staff education
  • 40. Arnow PM et al. An outbreak of fatal fluoride intoxication in a long-term hemodialysis unit. Ann Intern Med 1994;121:339- 344. • On 16 July 1993, 12 patients treated at a long-term HD unit in Chicago became ill during or soon after HD. • The patients experienced symptoms of severe pruritus, headache, nausea, and chest or back pain. • Three patients arrested and died due to ventricular fibrillation after completion of dialysis that day. • Subsequent investigations found that fluoride was released from the deionization system after the ion exchange resin inside was exhausted. • The investigator concluded that the incident was caused by errors in maintenance of the deionization system
  • 41. • In February 1996, Caruaru,Brazil, 116 (89%) of 131 patients experienced visual disturbances, nausea, vomiting, and muscle weakness, following routine HD treatment. Subsequently, 100 patients developed acute liver failure. As of December 1996, 52 deaths occurred. • Two groups of hepatotoxic cyanotoxins were idnetified: microcystins, specifically microcystin-YR, -LR and -AR. • The outbreak occurred in one of two HD units using same water source
  • 42. Water treatment system 1.Feed Water Components: (Back-flow preventer, Temperature blending valve, booster pump and raw water tank, ±acid feed pump ) 2.Pre-treatment section: (filters, activated carbon and softner). 3.Treatment section: (reverse osmosis). 4.Post-treatment section: (microbial and UV filters or/and deionization) 5.the distribution system: piping, valves, pumps, ±storage tanks
  • 43.
  • 44. • An indication of mineral deposits forming on the membrane will be high readings of total dissolved solids (TDS), percent rejection and conductivity (or low resistivity). • In feed water classified as being very hard, damage to the RO membrane may occur extremely rapidly, even within hours, with irreversible membrane damage • So the softener is placed before the reverse osmosis (RO) unit to protect the RO membrane. • Analysis of the level of calcium carbonate (CaCO3) in the feed water is important for determining the size of the softener.
  • 45. Schematic diagram example of a water treatment system for hemodialysis
  • 46. Back flow preventer: inhibits flow back of treated water into municipal water Temperature blending valve: brings water to a standard temperature of 25 oC for proper function of RO system Booster pump: maintains adequate flow and pressure of water so the system operates successfully.
  • 47. Acid feed pump • By increasing the pH of the city water supply using lime softening agents or Ca CO3 prevent leaching of lead, copper from the piping system • For proper function of RO and carbon tanks, incoming water pH should be between 5-8.5 • A pH higher than 8.5 with chloramines present will cause the carbon to be less adsorptive and the RO membrane performance to degrade, resulting in poor water quality.
  • 48. Purification Processes Process Contaminant Carbon Adsorption Chloramine, organics Softener Calcium, Mg Reverse osmosis Inoic contaminants, bacteria, endotoxin Deionization Ionic contaminants Ultrafiltration Bacteria, endotoxin
  • 49. Multimedia depth filter • Large particulates of >10 microns such as dirt, are removed by a multimedia depth filter. • Floculants can clog the carbon and softener tanks, destroy the RO pump, and foul the RO membrane • Contain multiple layers of various sized rocks that trap the large particles as the water filtered downward
  • 50. Carbon Tank • Removes chlorine and chloramine • These are high level oxidative chemicals. They are added to municipal water systems to kill bacteria, but they also cause hemolysis
  • 51.
  • 52. Carbon filter •As the input water flows down through the granular activated carbon (GAC), solutes diffuse from the water into the pores of the carbon and become attached to the structure. •A 10-minute exposure time of the water through the carbon tanks to reduce chlorine to at least 0.5 mg/L and the chloramine to be adsorbed to at least 0.1 mg/L. A wide variety of naturally occurring and synthetic organic compounds, such as herbicides, pesticides, and industrial solvents, will be adsorbed as well
  • 53. Water Softener • Water containing Ca and Mg form deposits on RO membrane • Softeners work on ion exchange basis. The resin beads within the tank have a high affinity for the cations Ca and Mg (divalents) present in the source water and release 2 sodium ions (monovalent) for one Ca or Mg captured
  • 54. Hardness of water • Calcium carbonate Classification • 0–60 mg/L Soft • 61–120 mg/L Moderately hard • 121–180 mg/L Hard • Greater than 180 mg/L Very hard
  • 55. Water Softener • The softener needs regenerating on a routine basis with concentrated NaCl solution (brine) before the resin capacity is used up • The resin is backwashed to loosen the media and clean any particulates from the tank. After the backwashing step, the brine solution is drawn into the tank
  • 56.
  • 57. Reverse Osmosis system • RO overcomes natural osmosis by forcing feed water under pressure thru a semi-permeable membrane leaving contaminants behind (ions, organics)
  • 58. Reverse osmosis •Reverse osmosis (RO) uses high pressure to force water across a semipermeable membrane, thereby rejecting 90 to 99 percent of ionic compounds and >95 percent of nonionic contaminants, also it is an effective barrier against microbiological contaminants, including bacteria, viruses, and endotoxin.
  • 59.
  • 60. Ion exchange deionizers (DI) DI use a two-stage process to remove virtually all ionic material remaining in pretreated water. Two types of synthetic resins are used; one to remove positively charged ions (cations) and another to remove negatively charged ions (anions). •Although deionizers produce water of very high purity with respect to ionic contaminants, they do not remove microbiological contaminants. •Therefore, it is necessary to incorporate bacterial control equipment after the application of a deionizer.
  • 61. Ultraviolet filter The mechanism of microorganism destruction is currently believed to be that ultraviolet causes molecular rearrangements in DNA and RNA, which in turn blocks replication. •As the UV kills the bacteria, it may increase the level of endotoxinas a result of the destruction of the gram-negative bacteria (endotoxin producing) cell wall
  • 63. Distribution system • RO distribution systems: direct feed and indirect feed • Direct feed: directly delivers the product water from the RO unit to the loop for distribution • Indirect feed: involves a storage tank that accumulates the product water and delivers to the distribution loop • Unused portions are recirculated back into the storage tank
  • 64. Microbiological aspects of fluid system design • use of a recirculation-type system, • avoidance of dead ends and dead space areas, • use of materials compatible with the planned methods of disinfection • avoidance of storage tanks. If a storage tank is necessary it should be cleaned and disinfected. • The disinfection program could prevent the formation of biofilm, which can become difficult to eradicate.
  • 65. Ultrapure dialysis solution • Decreases CRP and IL-6 • Improves response to EPO • Promotes better nutrition • Reduces plasma levels of ß-2-microglobulin • Slows loss of residual renal function • Lowers cardiovascular morbidity • Bacteria level below 0.1 cfu/ml and endotoxin level below 0.03 EU/ml Susantitaphong P et al. Effect of ultrapure dialysate on markers of inflammation, oxidative stress, nutrition and anemia parameters: a meta-analysis. NDT (2013) 28: 438-446
  • 66. Water treatment unit TDS, and conductivity daily Microbiological culture and endotoxin assay. Monthly Chemical assay every 6 months
  • 67. Water treatment unit • There is no limit for RO product TDS/conductivity. • Values that are acceptable in one location may not be acceptable in another location. • TDS in some areas of 50 ppm is acceptable and other areas where 10 ppm is NOT acceptable. It all depends on your raw water. • A slight change in the amount of Fluoride injected into the water can cause the RO product water to go less than a 1 ppm TDS increase.
  • 68. Bacteriological Monitoring: • The maximum level of bacteria in water used to prepare dialysis fluid must not exceed the AAMI standard of 100 CFU. The AAMI action level is 50 CFU • An action level is defined as a point when measures must be taken to correct the potential source to remain in compliance with AAMI standards
  • 69. Endotoxin standard • The maximum level of endotoxin in water used to prepare dialysis fluid must not exceed the AAMI standard of 0.25 Endotoxin Units/ ml (EU/ml) • The action level of endotoxin is 0.125 EU/ml
  • 70.
  • 71.
  • 72. Contaminant Maximum Concentration mg/L Test Methodology Calcium 2 (0.1 mEq/L) EDTA or Atomic Absorption Magnesium 4 (0.3 mEq/L) Atomic Absorption Potassium 8 (0.2 mEq/L) Atomic Absorption, or Flame Photometri Sodium 70 (3.0 mEq/L) Atomic Absorption or Flame Photometric Antimony 0.006 Atomic Absorption (platform) Arsenic 0.005 Atomic Absorption (gaseous hydride) Barium 0.10 Atomic Absorption (electrothermal) Beryllium 0.0004 Atomic Absorption (platform) Cadmium 0.001 Atomic Absorption (electrothermal) Chromium 0.014 Atomic Absorption (electrothermal) Lead 0.005 Atomic Absorption (electrothermal) Mercury 0.0002 Flameless Cold Vapor (Atomic Absorption)
  • 73. Contaminant Maximum Concentration mg/L Test Methodology Selenium 0.09 Atomic Absorption (gaseous, or electrothermal) Silver 0.005 Atomic Absorption (electrothermal) Aluminum 0.01 Atomic Absorption (electrothermal) Chloramines 0.10 DPD Ferrous Titrimetric Method Total chlorine 0.50 DPD Ferrous Titrimetric Method Copper 0.10 Atomic Absorption (direct aspiration) Fluoride 0.20 Ion Selective Electrode Method Nitrate (as N) 2.00 Cadmium Reduction Method Sulfate 100.00 Turbidimetric Method Thallium 0.002 Atomic Absorption (platform) Zinc 0.10 Atomic Absorption (direct aspiration) Association for the Advancement of Medical Instrumentation. Dialysate for hemodialysis (ANSI/AAMI RD52:2004).Arlington (VA). American National Standard. 2004
  • 74. Water treatment unit A programme of improvement should begin immediately if routine monitoring demonstrates that concentrations of chemical contaminants exceed the maximum allowable limits of AAMI. (1B)
  • 75. Disinfection General • Disinfection schedules should be designed to prevent bacterial proliferation, rather than being designed to eliminate bacteria once they have proliferated to an unacceptable level (i.e. above the action level). • A proper disinfection strategy is to be preventive and this should be applied from the start of operation.
  • 76. Disinfection • Disinfection of the distribution piping systems. • 1- Chemical disinfection • 2- Hot water disinfection When used to control bacterial proliferation (minimum distribution loop temp 60 oC). • Heat disinfection will not remove established biofilms, but is convenient, requires little rinse time and can thus be used more often to prevent biofilm formation. An occasional chemical disinfection might still be necessary.
  • 77. Testing of samples • Testing of water samples shall be carried out by trained and accredited persons or accredited laboratories. • The dialysis unit shall maintain records of persons who have been trained and accredited and full details of accredited laboratories. • The records shall be maintained within the dialysis unit.
  • 78. Sample collection • Water sample sites • Samples are to be taken at outlets of the water distribution system. • Prior to sampling, the inside of the outlet can be disinfected, especially if no hemodialysis machine is attached. The reason for such disinfection is that, over time, residual water in an outlet will support microbial growth. The disinfection can be made by flushing the inside of the outlet with 70 % ethanol or iso-propanol. A sterile cotton swab wetted with alcohol can also be used. Exposure time is to be >15 s. • It is sufficient to let out enough water to rinse off the alcohol (200 ml to 500 ml) prior to sampling. • Alternatively, hoses can be disconnected from the tap and the taps opened and allowed to flush for 2 min to 3 min before aseptically collecting a sample. • Sample for cultivation and endotoxin analysis: Sample volume 5 ml to 1,000 ml or volume as specified by the laboratory..
  • 79. Sample collection • Dialysis fluid samples • Dialysis fluid samples should be collected from a sampling port prior to the dialyzer. The sample port should be designed to minimize the likelihood of contaminating the sample and should be capable of being effectively disinfected. • Many dialysis machines are equipped with dialysis fluid sample ports that can be accessed using a syringe. These sample ports may be disinfected with 70 % ethanol or iso-propanol and allowed to air dry. • A sterile syringe (20 ml or larger) should then be used to aspirate dialysis fluid out of and into the port before filling the syringe. The filled syringe should then be discarded and a fresh sample of dialysis fluid collected using a new sterile syringe. • Sample for cultivation and endotoxin analysis: Sample volume 5 ml to 1,000 ml or a volume as specified by the laboratory. Containers for samples to be cultured should be sterile and containers for samples to be tested for endotoxins should be sterile and endotoxin-free.
  • 80. Storage of samples • Heterotrophic plate count • Storage of samples • Microbial analysis of water and dialysis fluid samples should be conducted as soon as possible after collection to avoid unpredictable changes in the microbial population. If samples cannot be analyzed within 4 h of collection, follow the laboratory's instructions for shipping. Samples intended for colony counts should not be frozen. • Storage of samples for endotoxin analysis may be different from what is given above, provided the complete procedure follows the manufacturer's instructions for use of the LAL assay.
  • 81. Conclusion • Water treatment is a generally neglected area of dialysis therapy • Quality of water contributes very significantly in acute and long term morbidity and prognosis • Due to increased survival of dialysis patients, increased use of bicarbonate dialysate and high flux membranes, water treatment has become essential • It is worthwhile achieving the goal of sterile, pyrogen free and chemically pure water for dialysis
  • 82. Conclusion • Written policies, practices and procedures shall be in place • AAMI standards are the accepted minimum standards for water pre-treatment for haemodialysis. Each unit should have standard operating procedures in place for sampling, monitoring and recording of feed and product water quality • All servicing, maintenance, interventions and changes to the water pre-treatment plant shall be recorded. .
  • 83. Conclusion • Medical directors who learn, know, and embrace the requirements for providing high-quality dialysis water will be most successful in this task. • Medical, nursing and technical staff working in dialysis units share responsibility for the safe operation of the water pre-treatment plant and shall participate together in regular multidisciplinary committee meetings to review the safe operation of the water pre-treatment plant and RO water plant.