SlideShare a Scribd company logo

Quality control

SKYFALL
SKYFALL

Quality control (QC) is a procedure or set of procedures intended to ensure that a manufactured product or performed service adheres to a defined set of quality criteria or meets the requirements of the client or customer. QC is similar to, but not identical with, quality assurance (QA). QC IN clinical biochemistry labs and hospitals

Science
1 of 33
Download to read offline
QUALITY CONTROL Amal George SBS MGU george.oa.jr@gmail.com
Quality Control - QC refers to the measures that must be included during each assay run to verify that the test is working properly. Quality Assurance - QA is defined as the overall program that ensures that the final results reported by the laboratory are correct. “The aim of quality control is simply to ensure that the results generated by the test are correct. However, quality assurance is concerned with much more: that the right test is carried out on the right specimen, and that the right result and right interpretation is delivered to the right person at the right time” DEFINITIONS
Quality The Degree to which a set of inherent characters fulfils the requirements. IMPORTANT TERMINOLOGIES
Precision Precision is the reproducibility of an analytical method Accuracy Accuracy defines how close the measured value is to the actual value.
Sensitivity Sensitivity of an assay in a measure of how little of the analyte the method can detect. Specificity Specificity of a assay related to how good the assay is at discriminating between the requested analyte and potentially interfering substances.
Standard This is a substance of constant composition of sufficient purity to be used for comparison purposes or standardisation Control This is a sample, which is chemically and Physically similar to unknown specimen A solution , lyophilised preparation or pool of collected human or animal specimen or artificially derived material intend for use in the QC process.
Calibrator: A material or solution of known concentration (or activity / intensity) used to calibrate or adjust a measurement procedure. It is also used to calculate the concentration of an unknown sample (as standard)
Variation in results Biochemical measurements vary for two reasons, namely: analytical variation biological variation. Quality Control
Analytical Measurement Instrument not calibrated correctly Specimens mix – up Incorrect volume of specimen Interfering substances present Instrument precision problem Test reporting Wrong patient ID Transcription error Report not legible Report delayed ANALYTICAL ERRORS
POST ANALYTICAL ERRORS Test interpretation Interfering substance not recognized Specificity of the test not understood Precision limitation not recognized Analytical sensitivity not appropriate Previous values not available for comparison
HOW TO CONTROL THESE ERRORS? PRE ANALYTICAL VARIABLES It is very difficult to establish effective methods for monitoring and controlling preanalytical variables because many of the variables are outside the laboratory areas. Requires the coordinated effort of many individuals and hospital departments Patient Identification The highest frequency of errors occurs with the use of handwritten labels and request forms. The use of bar code technology has significantly reduced ID problems. Turn around time Delayed and lost test requisitions, specimens and reports can be major problems for labs. Recording of the actual times of specimen collection, receipt in the lab and reporting of results with use of computers will solve these problems.
Transcription error A substantial risk of transcription error exists from manual entry of data even with the double checking of results, computerization will reduce this type of transcription error. Patient preparation Lab tests are affected by many factors, such as, recent intake of food, alcohol, or drugs smoking exercise stress sleep posture during specimen collection The lab must define the instructions and procedures compliance with these instructions can be monitored directly efforts should be made to correct non compliance
GENERAL PRINCIPLES OF CONTROL CHARTS  Control charts are simple graphical displays in which the observed values are plotted versus the time when the observations are made.  The control limits are calculated from the mean (x) and standard deviations (s)
Internal Quality Control Program for Serological Testing An internal quality control program depend on the use of internal quality control (IQC) specimens, Shewhart Control Charts, and the use of statistical methods for interpretation. Internal Quality Control Specimens IQC specimens comprises either (1) in-house patient sera (single or pooled clinical samples), or (2) international serum standards with values within each clinically significant ranges.
QC Log with Patient Results
Basic statistics to develop an acceptable control range The most fundamental statistics used by the laboratory are the mean [x] and standard deviation [s]. Calculating a Mean [x]: The mean (or average) is the laboratory’s best estimate of the analyte’s true value for a specific level of control. Calculating a Standard Deviation [s]:  Standard deviation is a statistic that quantifies how close numerical values (i.e., QC values) are in relation to each other  Standard deviation is calculated for control products from the same data used to calculate the mean.  It provides the laboratory an estimate of test consistency at specific concentrations.  The repeatability of a test may be consistent (low standard deviation, low imprecision) or inconsistent (high standard deviation, high imprecision).
Mean [x] Standard Deviation [s]
Creating a Levey-Jennings Chart • Standard deviation is commonly used for preparing Levey-Jennings (L-J or LJ) charts. The Levey-Jennings chart is used to graph successive (run-to-run or day-to-day) quality control values. • A chart is created for each test and level of control. • The first step is to calculate decision limits. These limits are ±1s, ±2s and ±3s from the mean. • From the mean and standard deviation value calculated in the previous slide we can now construct the Levy Jennings chart as follows:
The Levey-Jennings chart that was developed can be overlaid onto a bell-shaped curve to illustrate the overall distribution of quality control values
Cont.. • When an analytical process is within control, approximately 68% of all QC values fall within ±1 standard deviation (1s). • Likewise 95.5% of all QC values fall within ±2 standard deviations (2s) of the mean. About 4.5% of all data will be outside the ±2s limits when the analytical process is in control. Approximately 99.7% of all QC values are found to be within ±3 standard deviations (3s) of the mean. • As only 0.3%, or 3 out of 1000 points, will fall outside the ±3s limits, any value outside of ±3s is considered to be associated with a significant error condition and patient results should not be reported.
Systematic Errors Trends: A trend indicates a gradual loss of reliability in the test system. Trends are usually subtle. Causes of trending may include: Systematic error is evidenced by a change in the mean of the control values. The change in the mean may be gradual and demonstrated as a trend in control values or it may be abrupt and demonstrated as a shift in control values.  Deterioration of the instrument light source  Gradual accumulation of debris in sample/reagent tubing  Gradual accumulation of debris on electrode surfaces  Aging of reagents  Gradual deterioration of control materials  Gradual deterioration of incubation chamber  temperature (enzymes only)  Gradual deterioration of light filter integrity  Gradual deterioration of calibration
Shift Abrupt changes in the control mean are defined as shifts. Shifts in QC data represent a sudden and dramatic positive or negative change in test system performance. Shifts may be caused by:  Sudden failure or change in the light source  Change in reagent formulation  Change of reagent lot  Major instrument maintenance  Sudden change in incubation temperature (enzymes only)  Change in room temperature or humidity  Failure in the sampling system  Failure in reagent dispense system  Inaccurate calibration/recalibration
Random Errors  Random error is any deviation away from an expected result.  For QC results, any positive or negative deviation away from the calculated mean is defined as random error.  There is acceptable (or expected) random error as defined and quantified by standard deviation.  There is unacceptable (unexpected) random error that is any data point outside the expected population of data (e.g., a data point outside the ±3s limits).
Westgard Rules There are six basic rules in the Westgard scheme. These rules are used individually or in combination to evaluate the quality of analytical runs. Most of the quality control rules can be expressed as NL where N represents the number of control observations to be evaluated and L represents the statistical limit for evaluating the control observations Thus 13s represents a control rule that is violated when one control observation exceeds the ±3s control limits.
Rule 12s This rule merely warns that random error or systematic error may be present in the test system The relationship between this value and other control results within the current and previous analytical runs must be examined. If no relationship can be found and no source of error can be identified, it must be assumed that a single control value outside the ±2s limits is an acceptable random error. Rule 13s This rule identifies unacceptable random error or possibly the beginning of a large systematic error. Any QC result outside ±3s violates this rule.
Rule 22s This rule identifies systematic error only. The criteria for violation of this rule are: • Two consecutive QC results • Greater than 2s • On the same side of the mean There are two applications to this rule: within-run and across runs. The within-run application affects all control results obtained for the current analytical run. • If a normal (Level I) and abnormal (Level II) control are assayed in this run and both levels of control are greater than 2s on the same side of the mean, this run violates the within-run application for systematic error. If however, Level I is -1s and Level II is +2.5s (a violation of the 12s rule), the Level II result from the previous run must be examined. If Level II in the previous run was at +2.0s or greater, then the across run application for systematic error is violated. Violation of the within-run application indicates that systematic error is present and that it affects potentially the entire analytical curve. Violation of the across run application indicates that only a single portion of the analytical curve is affected by the error.
• This rule identifies random error only, and is applied only within the current run. If there is at least a 4s difference between control values within a single run, the rule is violated for random error. • For example, assume both Level I and Level II have been assayed within the current run. Level I is +2.8s above the mean and Level II is -1.3s below the mean. The total difference between the two control levels is greater than 4s (e.g. [+2.8s – (-1.3s)] = 4.1s). Rule R4s
The criteria which must be met to violate this rule are: • Three consecutive results • Greater than 1s • On the same side of the mean Rule 31s The criteria which must be met to violate this rule are: • Four consecutive results • Greater than 1s • On the same side of the mean Rule 41s There are two applications to the 31s and 41s rule. These are within control material (e.g. all Level I control results) or across control materials (e.g., Level I, II, and III control results in combination). Within control material violations indicate systematic bias in a single area of the method curve while violation of the across control materials application indicates systematic error over a broader concentration
Rules 7X 8X 9X 10X12X These rules are violated when there are: 7 or 8, or 9, or 10, or 12 control results On the same side of the mean regardless of the specific standard deviation in which they are located. Each of these rules also has two applications: within control material (e.g., all Level I control results) or across control materials (e.g. Level I, II, and III control results in combination). Within control material violations indicate systematic bias in a single area of the method curve while violation of the across control materials application indicates systematic bias over a broader concentration
Coefficient of Variation [CV] • The Coefficient of Variation [CV] is the ratio of the standard deviation to the mean and is expressed as a percentage. • CV allows the technologist to make easier comparisons of the overall precision. • Standard deviation typically increases as the concentration of the analyte increases, the CV can be regarded as a statistical equalizer. • Technologist/technician who is comparing precision for two different methods and uses only standard deviation, can be easily misled • For example, a comparison between hexokinase and glucose oxidase (two methods for assaying glucose) is required. The standard deviation for the hexokinase method is 4.8 and it is 4.0 for glucose oxidase. If the comparison only uses standard deviation, it can be incorrectly assumed that the glucose oxidase method is more precise that the hexokinase method. If, however, a CV is calculated, it might show that both methods are equally precise. Assume the mean for the hexokinase method is 120 and the glucose oxidase mean is 100. The CV then, for both methods, is 4%. They are equally precise.
Coefficient of Variation Ratio [CVR] • Accuracy of test results is paramount in the clinical laboratory, precision is just as important • One way a laboratory can determine whether the precision of a specific test is acceptable is to compare its precision to that of another laboratory performing the same test on the same instrument using the same reagents (laboratory peer group) • If the CV for potassium on a particular instrument is 4% and the potassium for all other laboratories using the same instrument is 4.2%, then the coefficient of variation ratio [CVR] is 4/4.2 or 0.95. • Any ratio less than 1.0 indicates that precision is better than the peer group. Any score greater than 1.0 indicates that imprecision is larger • Ratios greater than 1.5 indicate a need to investigate the cause of imprecision and any ratio of 2.0 or greater usually indicates need for troubleshooting and corrective action
Standard Deviation Index [SDI] • The standard deviation index [SDI] is a peer-based estimate of reliability. If the peer group mean is defined as XGroup , the standard deviation is defined as SGroup and the laboratory’s mean is defined as Xlab • The target SDI is 0.0 which indicates a perfect comparison with the peer group. The following guidelines may be used with SDI. A value of: • 1.25 or less is considered acceptable. • 1.25 – 1.49 is considered acceptable to marginal performance. Some investigation of • the test system may be required. • 1.5 – 1.99 is considered marginal performance and investigation of the test system is • recommended. • 2.0 or greater is generally considered to be unacceptable performance and remedial action is usually required.
Thankyou!

Recommended

Quality Control in Laboratory
Quality Control in LaboratoryQuality Control in Laboratory
Quality Control in LaboratoryManal Elsayed CPPS, CPHQ, CLSSBB, FISQua, DTQM
 
Quality control
Quality controlQuality control
Quality controlPavalaveelzi C.M
 
Quality Control In Clinical Laboratory
Quality Control In Clinical LaboratoryQuality Control In Clinical Laboratory
Quality Control In Clinical LaboratoryDr. Rajesh Bendre
 
Internal quality control
Internal quality controlInternal quality control
Internal quality controlSyed Basheer
 
WESTGARD RULES
WESTGARD RULESWESTGARD RULES
WESTGARD RULESDr. K. Selvakumar @ Benny
 
Quality Control in a Medical Testing Laboratory
Quality Control in a Medical Testing LaboratoryQuality Control in a Medical Testing Laboratory
Quality Control in a Medical Testing LaboratoryDr. Bikash Kumar Chaudhury
 
Quality control in the medical laboratory
Quality control in the medical laboratoryQuality control in the medical laboratory
Quality control in the medical laboratoryAdnan Jaran
 
Quality control
Quality controlQuality control
Quality controlAbhra Ghosh
 

More Related Content

What's hot

Laboratory Internal Quality Control presentation master revision, 2014
Laboratory Internal Quality Control presentation master revision, 2014Laboratory Internal Quality Control presentation master revision, 2014
Laboratory Internal Quality Control presentation master revision, 2014Adel Elazab Elged
 
Quality control in clinical laboratory
Quality control in clinical laboratoryQuality control in clinical laboratory
Quality control in clinical laboratorydrgomi basar
 
Internal quality control in clinical laboratories hematology(2)
Internal quality control in clinical laboratories hematology(2)Internal quality control in clinical laboratories hematology(2)
Internal quality control in clinical laboratories hematology(2)NAZAR ABU-DULLA
 
quality control in clinical pathology
quality control in clinical pathologyquality control in clinical pathology
quality control in clinical pathologyIshaque Vadakkethil
 
Automation in the Clinical Lab
Automation in the Clinical LabAutomation in the Clinical Lab
Automation in the Clinical LabAli Raza Ph.D
 
Quality assurance in medical laboratory
Quality assurance in medical laboratoryQuality assurance in medical laboratory
Quality assurance in medical laboratoryFaiz Alkhawlani
 
Internal quality control (IQC) in coagulation lab
Internal quality control (IQC) in coagulation labInternal quality control (IQC) in coagulation lab
Internal quality control (IQC) in coagulation labAnkit Raiyani
 
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...Adel Elazab Elged
 
Quality assurance in the department of clinical biochemistry
Quality assurance in the department of clinical biochemistryQuality assurance in the department of clinical biochemistry
Quality assurance in the department of clinical biochemistryDipesh Tamrakar
 
Total Quality Management (TQM) by Dr Anurag Yadav
Total Quality Management (TQM) by Dr Anurag YadavTotal Quality Management (TQM) by Dr Anurag Yadav
Total Quality Management (TQM) by Dr Anurag YadavDr Anurag Yadav
 
Validation of lab instruments and quantitative test methods
Validation of lab instruments and quantitative test methods Validation of lab instruments and quantitative test methods
Validation of lab instruments and quantitative test methods Mostafa Mahmoud
 
Pre analytic and postanalytic test management
Pre analytic and postanalytic test managementPre analytic and postanalytic test management
Pre analytic and postanalytic test managementVarsha Shahane
 
Quality control in clinical laboratories
Quality control in clinical laboratoriesQuality control in clinical laboratories
Quality control in clinical laboratoriesAshish Jawarkar
 
Laboratory accreditation
Laboratory accreditationLaboratory accreditation
Laboratory accreditationGift Sam
 

What's hot (20)

Troubleshooting IQC / EQAS
Troubleshooting IQC / EQASTroubleshooting IQC / EQAS
Troubleshooting IQC / EQAS
 
Quality Control
Quality ControlQuality Control
Quality Control
 
Laboratory Internal Quality Control presentation master revision, 2014
Laboratory Internal Quality Control presentation master revision, 2014Laboratory Internal Quality Control presentation master revision, 2014
Laboratory Internal Quality Control presentation master revision, 2014
 
Quality control in clinical laboratory
Quality control in clinical laboratoryQuality control in clinical laboratory
Quality control in clinical laboratory
 
Internal quality control in clinical laboratories hematology(2)
Internal quality control in clinical laboratories hematology(2)Internal quality control in clinical laboratories hematology(2)
Internal quality control in clinical laboratories hematology(2)
 
quality control in clinical pathology
quality control in clinical pathologyquality control in clinical pathology
quality control in clinical pathology
 
Automation in the Clinical Lab
Automation in the Clinical LabAutomation in the Clinical Lab
Automation in the Clinical Lab
 
Quality assurance in medical laboratory
Quality assurance in medical laboratoryQuality assurance in medical laboratory
Quality assurance in medical laboratory
 
Internal quality control (IQC) in coagulation lab
Internal quality control (IQC) in coagulation labInternal quality control (IQC) in coagulation lab
Internal quality control (IQC) in coagulation lab
 
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...
External Quality Control Lecture MD General 2014 Course, Clin Path Ain Shams ...
 
Total Quality Management in Medical Laboratories
Total Quality Management in Medical LaboratoriesTotal Quality Management in Medical Laboratories
Total Quality Management in Medical Laboratories
 
Quality assurance in the department of clinical biochemistry
Quality assurance in the department of clinical biochemistryQuality assurance in the department of clinical biochemistry
Quality assurance in the department of clinical biochemistry
 
Automation
AutomationAutomation
Automation
 
Quality assurance in a medical laboratory
Quality assurance in a medical laboratoryQuality assurance in a medical laboratory
Quality assurance in a medical laboratory
 
Total Quality Management (TQM) by Dr Anurag Yadav
Total Quality Management (TQM) by Dr Anurag YadavTotal Quality Management (TQM) by Dr Anurag Yadav
Total Quality Management (TQM) by Dr Anurag Yadav
 
Validation of lab instruments and quantitative test methods
Validation of lab instruments and quantitative test methods Validation of lab instruments and quantitative test methods
Validation of lab instruments and quantitative test methods
 
Westgard rules
Westgard rulesWestgard rules
Westgard rules
 
Pre analytic and postanalytic test management
Pre analytic and postanalytic test managementPre analytic and postanalytic test management
Pre analytic and postanalytic test management
 
Quality control in clinical laboratories
Quality control in clinical laboratoriesQuality control in clinical laboratories
Quality control in clinical laboratories
 
Laboratory accreditation
Laboratory accreditationLaboratory accreditation
Laboratory accreditation
 

Similar to Quality control

Quality management system BY M .REJA
Quality management system BY M .REJAQuality management system BY M .REJA
Quality management system BY M .REJAMamunReja1
 
Laboratory Quality Control .ppt
Laboratory Quality Control .pptLaboratory Quality Control .ppt
Laboratory Quality Control .pptABRARAHMED767665
 
Quality Assurance and Quality Control
Quality Assurance and Quality ControlQuality Assurance and Quality Control
Quality Assurance and Quality ControlECRD IN
 
Quality assurance and quality control
Quality assurance and quality controlQuality assurance and quality control
Quality assurance and quality controlECRD2015
 
Chapter 12
Chapter 12Chapter 12
Chapter 12ECRD IN
 
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...Randox
 
Control of analytical quality using stable control materials postgrad
Control of analytical quality using stable control materials postgradControl of analytical quality using stable control materials postgrad
Control of analytical quality using stable control materials postgradMedhatEldeeb2
 
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)Aamir Ijaz Brig
 
(IQC) - Internal Quality Control.pptx
(IQC) - Internal Quality Control.pptx(IQC) - Internal Quality Control.pptx
(IQC) - Internal Quality Control.pptxDr.Rajeev Ranjan
 
quality control in clinical laboratory
quality control in clinical laboratory quality control in clinical laboratory
quality control in clinical laboratory DrmanarEmam
 
Evaluation of methods in clinical laboratory
Evaluation of methods in clinical laboratoryEvaluation of methods in clinical laboratory
Evaluation of methods in clinical laboratoryDrMAnwar2
 
Basics of laboratory internal quality control, Ola Elgaddar, 2012
Basics of laboratory internal quality control, Ola Elgaddar, 2012Basics of laboratory internal quality control, Ola Elgaddar, 2012
Basics of laboratory internal quality control, Ola Elgaddar, 2012Ola Elgaddar
 
Variability of clinical chemistry laboratory results
Variability of clinical chemistry laboratory resultsVariability of clinical chemistry laboratory results
Variability of clinical chemistry laboratory resultsAdetokunboAjala
 
Internal quality control in blood bank testing
Internal quality control in blood bank testingInternal quality control in blood bank testing
Internal quality control in blood bank testingSanjeew Yadav
 
2. Quality Control Notes
2. Quality Control Notes2. Quality Control Notes
2. Quality Control NotesLeah Molai
 

Similar to Quality control (20)

Quality management system BY M .REJA
Quality management system BY M .REJAQuality management system BY M .REJA
Quality management system BY M .REJA
 
Laboratory Quality Control .ppt
Laboratory Quality Control .pptLaboratory Quality Control .ppt
Laboratory Quality Control .ppt
 
Quality control.pptx
Quality control.pptxQuality control.pptx
Quality control.pptx
 
Clinical lab qc sethu
Clinical lab qc sethuClinical lab qc sethu
Clinical lab qc sethu
 
Qc and qa
Qc and qaQc and qa
Qc and qa
 
Quality Assurance and Quality Control
Quality Assurance and Quality ControlQuality Assurance and Quality Control
Quality Assurance and Quality Control
 
Quality assurance and quality control
Quality assurance and quality controlQuality assurance and quality control
Quality assurance and quality control
 
Chapter 12
Chapter 12Chapter 12
Chapter 12
 
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...
Basic QC Statistics - Improving Laboratory Performance Through Quality Contro...
 
Control of analytical quality using stable control materials postgrad
Control of analytical quality using stable control materials postgradControl of analytical quality using stable control materials postgrad
Control of analytical quality using stable control materials postgrad
 
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)
Quality Control for Quantitative Tests by Prof Aamir Ijaz (Pakistan)
 
(IQC) - Internal Quality Control.pptx
(IQC) - Internal Quality Control.pptx(IQC) - Internal Quality Control.pptx
(IQC) - Internal Quality Control.pptx
 
Quality management
Quality managementQuality management
Quality management
 
quality control in clinical laboratory
quality control in clinical laboratory quality control in clinical laboratory
quality control in clinical laboratory
 
Quality control chemical
Quality control chemicalQuality control chemical
Quality control chemical
 
Evaluation of methods in clinical laboratory
Evaluation of methods in clinical laboratoryEvaluation of methods in clinical laboratory
Evaluation of methods in clinical laboratory
 
Basics of laboratory internal quality control, Ola Elgaddar, 2012
Basics of laboratory internal quality control, Ola Elgaddar, 2012Basics of laboratory internal quality control, Ola Elgaddar, 2012
Basics of laboratory internal quality control, Ola Elgaddar, 2012
 
Variability of clinical chemistry laboratory results
Variability of clinical chemistry laboratory resultsVariability of clinical chemistry laboratory results
Variability of clinical chemistry laboratory results
 
Internal quality control in blood bank testing
Internal quality control in blood bank testingInternal quality control in blood bank testing
Internal quality control in blood bank testing
 
2. Quality Control Notes
2. Quality Control Notes2. Quality Control Notes
2. Quality Control Notes
 

More from SKYFALL

Structure of amino acids
Structure of amino acidsStructure of amino acids
Structure of amino acidsSKYFALL
 
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACID
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACIDALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACID
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACIDSKYFALL
 
Bacteriophages
Bacteriophages Bacteriophages
Bacteriophages SKYFALL
 
Nutrition in pregnancy and lactation
Nutrition in pregnancy and lactation Nutrition in pregnancy and lactation
Nutrition in pregnancy and lactation SKYFALL
 
RIA, IMMUNOFLURESCENCE ASSAY
RIA, IMMUNOFLURESCENCE ASSAYRIA, IMMUNOFLURESCENCE ASSAY
RIA, IMMUNOFLURESCENCE ASSAYSKYFALL
 
Structural aberrations of chromosomes
Structural aberrations of chromosomesStructural aberrations of chromosomes
Structural aberrations of chromosomesSKYFALL
 
The citric acid cycle
The citric acid cycleThe citric acid cycle
The citric acid cycleSKYFALL
 
Trp operon
Trp operonTrp operon
Trp operonSKYFALL
 
Regulation of glycolysis and gluconeogenesis
Regulation of glycolysis and gluconeogenesisRegulation of glycolysis and gluconeogenesis
Regulation of glycolysis and gluconeogenesisSKYFALL
 
Rna pol ii
Rna pol iiRna pol ii
Rna pol iiSKYFALL
 
Complement fixation
Complement fixationComplement fixation
Complement fixationSKYFALL
 
Cerebrospinal fluid
Cerebrospinal fluidCerebrospinal fluid
Cerebrospinal fluidSKYFALL
 
Density gradient centrifugation
Density gradient centrifugationDensity gradient centrifugation
Density gradient centrifugationSKYFALL
 
Thyroid hormone disorders
Thyroid hormone disordersThyroid hormone disorders
Thyroid hormone disordersSKYFALL
 

More from SKYFALL (15)

Structure of amino acids
Structure of amino acidsStructure of amino acids
Structure of amino acids
 
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACID
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACIDALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACID
ALL ABOUT VITAMINS VITAMIN B6, B7, B12 AND FOLIC ACID
 
Bacteriophages
Bacteriophages Bacteriophages
Bacteriophages
 
Nutrition in pregnancy and lactation
Nutrition in pregnancy and lactation Nutrition in pregnancy and lactation
Nutrition in pregnancy and lactation
 
RIA, IMMUNOFLURESCENCE ASSAY
RIA, IMMUNOFLURESCENCE ASSAYRIA, IMMUNOFLURESCENCE ASSAY
RIA, IMMUNOFLURESCENCE ASSAY
 
GLP
GLPGLP
GLP
 
Structural aberrations of chromosomes
Structural aberrations of chromosomesStructural aberrations of chromosomes
Structural aberrations of chromosomes
 
The citric acid cycle
The citric acid cycleThe citric acid cycle
The citric acid cycle
 
Trp operon
Trp operonTrp operon
Trp operon
 
Regulation of glycolysis and gluconeogenesis
Regulation of glycolysis and gluconeogenesisRegulation of glycolysis and gluconeogenesis
Regulation of glycolysis and gluconeogenesis
 
Rna pol ii
Rna pol iiRna pol ii
Rna pol ii
 
Complement fixation
Complement fixationComplement fixation
Complement fixation
 
Cerebrospinal fluid
Cerebrospinal fluidCerebrospinal fluid
Cerebrospinal fluid
 
Density gradient centrifugation
Density gradient centrifugationDensity gradient centrifugation
Density gradient centrifugation
 
Thyroid hormone disorders
Thyroid hormone disordersThyroid hormone disorders
Thyroid hormone disorders
 

Recently uploaded

Loudspeaker- direct radiating type and horn type.pptx
Loudspeaker- direct radiating type and horn type.pptxLoudspeaker- direct radiating type and horn type.pptx
Loudspeaker- direct radiating type and horn type.pptxpriyankatabhane
 
Role of Gibberellins, mode of action and external applications.pptx
Role of Gibberellins, mode of action and external applications.pptxRole of Gibberellins, mode of action and external applications.pptx
Role of Gibberellins, mode of action and external applications.pptxjana861314
 
Abnormal LFTs rate of deco and NAFLD.pptx
Abnormal LFTs rate of deco and NAFLD.pptxAbnormal LFTs rate of deco and NAFLD.pptx
Abnormal LFTs rate of deco and NAFLD.pptxzeus70441
 
DNA isolation molecular biology practical.pptx
DNA isolation molecular biology practical.pptxDNA isolation molecular biology practical.pptx
DNA isolation molecular biology practical.pptxGiDMOh
 
Total Legal: A “Joint” Journey into the Chemistry of Cannabinoids
Total Legal: A “Joint” Journey into the Chemistry of CannabinoidsTotal Legal: A “Joint” Journey into the Chemistry of Cannabinoids
Total Legal: A “Joint” Journey into the Chemistry of CannabinoidsMarkus Roggen
 
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...Speed Breeding in Vegetable Crops- innovative approach for present era of cro...
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...jana861314
 
BACTERIAL SECRETION SYSTEM by Dr. Chayanika Das
BACTERIAL SECRETION SYSTEM by Dr. Chayanika DasBACTERIAL SECRETION SYSTEM by Dr. Chayanika Das
BACTERIAL SECRETION SYSTEM by Dr. Chayanika DasChayanika Das
 
Understanding Nutrition, 16th Edition pdf
Understanding Nutrition, 16th Edition pdfUnderstanding Nutrition, 16th Edition pdf
Understanding Nutrition, 16th Edition pdfHabibouKarbo
 
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...Christina Parmionova
 
Advances in AI-driven Image Recognition for Early Detection of Cancer
Advances in AI-driven Image Recognition for Early Detection of CancerAdvances in AI-driven Image Recognition for Early Detection of Cancer
Advances in AI-driven Image Recognition for Early Detection of CancerLuis Miguel Chong Chong
 
Introduction of Organ-On-A-Chip - Creative Biolabs
Introduction of Organ-On-A-Chip - Creative BiolabsIntroduction of Organ-On-A-Chip - Creative Biolabs
Introduction of Organ-On-A-Chip - Creative BiolabsCreative-Biolabs
 
Production technology of Brinjal -Solanum melongena
Production technology of Brinjal -Solanum melongenaProduction technology of Brinjal -Solanum melongena
Production technology of Brinjal -Solanum melongenajana861314
 
6.2 Pests of Sesame_Identification_Binomics_Dr.UPR
6.2 Pests of Sesame_Identification_Binomics_Dr.UPR6.2 Pests of Sesame_Identification_Binomics_Dr.UPR
6.2 Pests of Sesame_Identification_Binomics_Dr.UPRPirithiRaju
 
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...Chayanika Das
 
Food_safety_Management_pptx.pptx in microbiology
Food_safety_Management_pptx.pptx in microbiologyFood_safety_Management_pptx.pptx in microbiology
Food_safety_Management_pptx.pptx in microbiologyHemantThakare8
 
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learning
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep LearningCombining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learning
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learningvschiavoni
 
Environment modelling and its environmental aspects
Environment modelling and its environmental aspectsEnvironment modelling and its environmental aspects
Environment modelling and its environmental aspectsMansi Rastogi
 

Recently uploaded (20)

Interferons.pptx.
Interferons.pptx.Interferons.pptx.
Interferons.pptx.
 
Loudspeaker- direct radiating type and horn type.pptx
Loudspeaker- direct radiating type and horn type.pptxLoudspeaker- direct radiating type and horn type.pptx
Loudspeaker- direct radiating type and horn type.pptx
 
Introduction Classification Of Alkaloids
Introduction Classification Of AlkaloidsIntroduction Classification Of Alkaloids
Introduction Classification Of Alkaloids
 
Role of Gibberellins, mode of action and external applications.pptx
Role of Gibberellins, mode of action and external applications.pptxRole of Gibberellins, mode of action and external applications.pptx
Role of Gibberellins, mode of action and external applications.pptx
 
Abnormal LFTs rate of deco and NAFLD.pptx
Abnormal LFTs rate of deco and NAFLD.pptxAbnormal LFTs rate of deco and NAFLD.pptx
Abnormal LFTs rate of deco and NAFLD.pptx
 
DNA isolation molecular biology practical.pptx
DNA isolation molecular biology practical.pptxDNA isolation molecular biology practical.pptx
DNA isolation molecular biology practical.pptx
 
PLASMODIUM. PPTX
PLASMODIUM. PPTXPLASMODIUM. PPTX
PLASMODIUM. PPTX
 
Total Legal: A “Joint” Journey into the Chemistry of Cannabinoids
Total Legal: A “Joint” Journey into the Chemistry of CannabinoidsTotal Legal: A “Joint” Journey into the Chemistry of Cannabinoids
Total Legal: A “Joint” Journey into the Chemistry of Cannabinoids
 
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...Speed Breeding in Vegetable Crops- innovative approach for present era of cro...
Speed Breeding in Vegetable Crops- innovative approach for present era of cro...
 
BACTERIAL SECRETION SYSTEM by Dr. Chayanika Das
BACTERIAL SECRETION SYSTEM by Dr. Chayanika DasBACTERIAL SECRETION SYSTEM by Dr. Chayanika Das
BACTERIAL SECRETION SYSTEM by Dr. Chayanika Das
 
Understanding Nutrition, 16th Edition pdf
Understanding Nutrition, 16th Edition pdfUnderstanding Nutrition, 16th Edition pdf
Understanding Nutrition, 16th Edition pdf
 
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...
Charateristics of the Angara-A5 spacecraft launched from the Vostochny Cosmod...
 
Advances in AI-driven Image Recognition for Early Detection of Cancer
Advances in AI-driven Image Recognition for Early Detection of CancerAdvances in AI-driven Image Recognition for Early Detection of Cancer
Advances in AI-driven Image Recognition for Early Detection of Cancer
 
Introduction of Organ-On-A-Chip - Creative Biolabs
Introduction of Organ-On-A-Chip - Creative BiolabsIntroduction of Organ-On-A-Chip - Creative Biolabs
Introduction of Organ-On-A-Chip - Creative Biolabs
 
Production technology of Brinjal -Solanum melongena
Production technology of Brinjal -Solanum melongenaProduction technology of Brinjal -Solanum melongena
Production technology of Brinjal -Solanum melongena
 
6.2 Pests of Sesame_Identification_Binomics_Dr.UPR
6.2 Pests of Sesame_Identification_Binomics_Dr.UPR6.2 Pests of Sesame_Identification_Binomics_Dr.UPR
6.2 Pests of Sesame_Identification_Binomics_Dr.UPR
 
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...
ESSENTIAL FEATURES REQUIRED FOR ESTABLISHING FOUR TYPES OF BIOSAFETY LABORATO...
 
Food_safety_Management_pptx.pptx in microbiology
Food_safety_Management_pptx.pptx in microbiologyFood_safety_Management_pptx.pptx in microbiology
Food_safety_Management_pptx.pptx in microbiology
 
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learning
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep LearningCombining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learning
Combining Asynchronous Task Parallelism and Intel SGX for Secure Deep Learning
 
Environment modelling and its environmental aspects
Environment modelling and its environmental aspectsEnvironment modelling and its environmental aspects
Environment modelling and its environmental aspects
 

Quality control

  • 1. QUALITY CONTROL Amal George SBS MGU george.oa.jr@gmail.com
  • 2. Quality Control - QC refers to the measures that must be included during each assay run to verify that the test is working properly. Quality Assurance - QA is defined as the overall program that ensures that the final results reported by the laboratory are correct. “The aim of quality control is simply to ensure that the results generated by the test are correct. However, quality assurance is concerned with much more: that the right test is carried out on the right specimen, and that the right result and right interpretation is delivered to the right person at the right time” DEFINITIONS
  • 3. Quality The Degree to which a set of inherent characters fulfils the requirements. IMPORTANT TERMINOLOGIES
  • 4. Precision Precision is the reproducibility of an analytical method Accuracy Accuracy defines how close the measured value is to the actual value.
  • 5. Sensitivity Sensitivity of an assay in a measure of how little of the analyte the method can detect. Specificity Specificity of a assay related to how good the assay is at discriminating between the requested analyte and potentially interfering substances.
  • 6. Standard This is a substance of constant composition of sufficient purity to be used for comparison purposes or standardisation Control This is a sample, which is chemically and Physically similar to unknown specimen A solution , lyophilised preparation or pool of collected human or animal specimen or artificially derived material intend for use in the QC process.
  • 7. Calibrator: A material or solution of known concentration (or activity / intensity) used to calibrate or adjust a measurement procedure. It is also used to calculate the concentration of an unknown sample (as standard)
  • 8. Variation in results Biochemical measurements vary for two reasons, namely: analytical variation biological variation. Quality Control
  • 9. Analytical Measurement Instrument not calibrated correctly Specimens mix – up Incorrect volume of specimen Interfering substances present Instrument precision problem Test reporting Wrong patient ID Transcription error Report not legible Report delayed ANALYTICAL ERRORS
  • 10. POST ANALYTICAL ERRORS Test interpretation Interfering substance not recognized Specificity of the test not understood Precision limitation not recognized Analytical sensitivity not appropriate Previous values not available for comparison
  • 11. HOW TO CONTROL THESE ERRORS? PRE ANALYTICAL VARIABLES It is very difficult to establish effective methods for monitoring and controlling preanalytical variables because many of the variables are outside the laboratory areas. Requires the coordinated effort of many individuals and hospital departments Patient Identification The highest frequency of errors occurs with the use of handwritten labels and request forms. The use of bar code technology has significantly reduced ID problems. Turn around time Delayed and lost test requisitions, specimens and reports can be major problems for labs. Recording of the actual times of specimen collection, receipt in the lab and reporting of results with use of computers will solve these problems.
  • 12. Transcription error A substantial risk of transcription error exists from manual entry of data even with the double checking of results, computerization will reduce this type of transcription error. Patient preparation Lab tests are affected by many factors, such as, recent intake of food, alcohol, or drugs smoking exercise stress sleep posture during specimen collection The lab must define the instructions and procedures compliance with these instructions can be monitored directly efforts should be made to correct non compliance
  • 13. GENERAL PRINCIPLES OF CONTROL CHARTS  Control charts are simple graphical displays in which the observed values are plotted versus the time when the observations are made.  The control limits are calculated from the mean (x) and standard deviations (s)
  • 14. Internal Quality Control Program for Serological Testing An internal quality control program depend on the use of internal quality control (IQC) specimens, Shewhart Control Charts, and the use of statistical methods for interpretation. Internal Quality Control Specimens IQC specimens comprises either (1) in-house patient sera (single or pooled clinical samples), or (2) international serum standards with values within each clinically significant ranges.
  • 15. QC Log with Patient Results
  • 16. Basic statistics to develop an acceptable control range The most fundamental statistics used by the laboratory are the mean [x] and standard deviation [s]. Calculating a Mean [x]: The mean (or average) is the laboratory’s best estimate of the analyte’s true value for a specific level of control. Calculating a Standard Deviation [s]:  Standard deviation is a statistic that quantifies how close numerical values (i.e., QC values) are in relation to each other  Standard deviation is calculated for control products from the same data used to calculate the mean.  It provides the laboratory an estimate of test consistency at specific concentrations.  The repeatability of a test may be consistent (low standard deviation, low imprecision) or inconsistent (high standard deviation, high imprecision).
  • 17. Mean [x] Standard Deviation [s]
  • 18. Creating a Levey-Jennings Chart • Standard deviation is commonly used for preparing Levey-Jennings (L-J or LJ) charts. The Levey-Jennings chart is used to graph successive (run-to-run or day-to-day) quality control values. • A chart is created for each test and level of control. • The first step is to calculate decision limits. These limits are ±1s, ±2s and ±3s from the mean. • From the mean and standard deviation value calculated in the previous slide we can now construct the Levy Jennings chart as follows:
  • 19. The Levey-Jennings chart that was developed can be overlaid onto a bell-shaped curve to illustrate the overall distribution of quality control values
  • 20. Cont.. • When an analytical process is within control, approximately 68% of all QC values fall within ±1 standard deviation (1s). • Likewise 95.5% of all QC values fall within ±2 standard deviations (2s) of the mean. About 4.5% of all data will be outside the ±2s limits when the analytical process is in control. Approximately 99.7% of all QC values are found to be within ±3 standard deviations (3s) of the mean. • As only 0.3%, or 3 out of 1000 points, will fall outside the ±3s limits, any value outside of ±3s is considered to be associated with a significant error condition and patient results should not be reported.
  • 21. Systematic Errors Trends: A trend indicates a gradual loss of reliability in the test system. Trends are usually subtle. Causes of trending may include: Systematic error is evidenced by a change in the mean of the control values. The change in the mean may be gradual and demonstrated as a trend in control values or it may be abrupt and demonstrated as a shift in control values.  Deterioration of the instrument light source  Gradual accumulation of debris in sample/reagent tubing  Gradual accumulation of debris on electrode surfaces  Aging of reagents  Gradual deterioration of control materials  Gradual deterioration of incubation chamber  temperature (enzymes only)  Gradual deterioration of light filter integrity  Gradual deterioration of calibration
  • 22. Shift Abrupt changes in the control mean are defined as shifts. Shifts in QC data represent a sudden and dramatic positive or negative change in test system performance. Shifts may be caused by:  Sudden failure or change in the light source  Change in reagent formulation  Change of reagent lot  Major instrument maintenance  Sudden change in incubation temperature (enzymes only)  Change in room temperature or humidity  Failure in the sampling system  Failure in reagent dispense system  Inaccurate calibration/recalibration
  • 23. Random Errors  Random error is any deviation away from an expected result.  For QC results, any positive or negative deviation away from the calculated mean is defined as random error.  There is acceptable (or expected) random error as defined and quantified by standard deviation.  There is unacceptable (unexpected) random error that is any data point outside the expected population of data (e.g., a data point outside the ±3s limits).
  • 24. Westgard Rules There are six basic rules in the Westgard scheme. These rules are used individually or in combination to evaluate the quality of analytical runs. Most of the quality control rules can be expressed as NL where N represents the number of control observations to be evaluated and L represents the statistical limit for evaluating the control observations Thus 13s represents a control rule that is violated when one control observation exceeds the ±3s control limits.
  • 25. Rule 12s This rule merely warns that random error or systematic error may be present in the test system The relationship between this value and other control results within the current and previous analytical runs must be examined. If no relationship can be found and no source of error can be identified, it must be assumed that a single control value outside the ±2s limits is an acceptable random error. Rule 13s This rule identifies unacceptable random error or possibly the beginning of a large systematic error. Any QC result outside ±3s violates this rule.
  • 26. Rule 22s This rule identifies systematic error only. The criteria for violation of this rule are: • Two consecutive QC results • Greater than 2s • On the same side of the mean There are two applications to this rule: within-run and across runs. The within-run application affects all control results obtained for the current analytical run. • If a normal (Level I) and abnormal (Level II) control are assayed in this run and both levels of control are greater than 2s on the same side of the mean, this run violates the within-run application for systematic error. If however, Level I is -1s and Level II is +2.5s (a violation of the 12s rule), the Level II result from the previous run must be examined. If Level II in the previous run was at +2.0s or greater, then the across run application for systematic error is violated. Violation of the within-run application indicates that systematic error is present and that it affects potentially the entire analytical curve. Violation of the across run application indicates that only a single portion of the analytical curve is affected by the error.
  • 27. • This rule identifies random error only, and is applied only within the current run. If there is at least a 4s difference between control values within a single run, the rule is violated for random error. • For example, assume both Level I and Level II have been assayed within the current run. Level I is +2.8s above the mean and Level II is -1.3s below the mean. The total difference between the two control levels is greater than 4s (e.g. [+2.8s – (-1.3s)] = 4.1s). Rule R4s
  • 28. The criteria which must be met to violate this rule are: • Three consecutive results • Greater than 1s • On the same side of the mean Rule 31s The criteria which must be met to violate this rule are: • Four consecutive results • Greater than 1s • On the same side of the mean Rule 41s There are two applications to the 31s and 41s rule. These are within control material (e.g. all Level I control results) or across control materials (e.g., Level I, II, and III control results in combination). Within control material violations indicate systematic bias in a single area of the method curve while violation of the across control materials application indicates systematic error over a broader concentration
  • 29. Rules 7X 8X 9X 10X12X These rules are violated when there are: 7 or 8, or 9, or 10, or 12 control results On the same side of the mean regardless of the specific standard deviation in which they are located. Each of these rules also has two applications: within control material (e.g., all Level I control results) or across control materials (e.g. Level I, II, and III control results in combination). Within control material violations indicate systematic bias in a single area of the method curve while violation of the across control materials application indicates systematic bias over a broader concentration
  • 30. Coefficient of Variation [CV] • The Coefficient of Variation [CV] is the ratio of the standard deviation to the mean and is expressed as a percentage. • CV allows the technologist to make easier comparisons of the overall precision. • Standard deviation typically increases as the concentration of the analyte increases, the CV can be regarded as a statistical equalizer. • Technologist/technician who is comparing precision for two different methods and uses only standard deviation, can be easily misled • For example, a comparison between hexokinase and glucose oxidase (two methods for assaying glucose) is required. The standard deviation for the hexokinase method is 4.8 and it is 4.0 for glucose oxidase. If the comparison only uses standard deviation, it can be incorrectly assumed that the glucose oxidase method is more precise that the hexokinase method. If, however, a CV is calculated, it might show that both methods are equally precise. Assume the mean for the hexokinase method is 120 and the glucose oxidase mean is 100. The CV then, for both methods, is 4%. They are equally precise.
  • 31. Coefficient of Variation Ratio [CVR] • Accuracy of test results is paramount in the clinical laboratory, precision is just as important • One way a laboratory can determine whether the precision of a specific test is acceptable is to compare its precision to that of another laboratory performing the same test on the same instrument using the same reagents (laboratory peer group) • If the CV for potassium on a particular instrument is 4% and the potassium for all other laboratories using the same instrument is 4.2%, then the coefficient of variation ratio [CVR] is 4/4.2 or 0.95. • Any ratio less than 1.0 indicates that precision is better than the peer group. Any score greater than 1.0 indicates that imprecision is larger • Ratios greater than 1.5 indicate a need to investigate the cause of imprecision and any ratio of 2.0 or greater usually indicates need for troubleshooting and corrective action
  • 32. Standard Deviation Index [SDI] • The standard deviation index [SDI] is a peer-based estimate of reliability. If the peer group mean is defined as XGroup , the standard deviation is defined as SGroup and the laboratory’s mean is defined as Xlab • The target SDI is 0.0 which indicates a perfect comparison with the peer group. The following guidelines may be used with SDI. A value of: • 1.25 or less is considered acceptable. • 1.25 – 1.49 is considered acceptable to marginal performance. Some investigation of • the test system may be required. • 1.5 – 1.99 is considered marginal performance and investigation of the test system is • recommended. • 2.0 or greater is generally considered to be unacceptable performance and remedial action is usually required.