Laboratory Management 2

Management of Delta Check In
Laboratory
Osman Sianipar
Department of Clinical Pathology and Laboratory

Medicine Universitas Gadjah Mada/Dr. Sardjito Hospital
Yogyakarta
08/05/2018 Simposium CPD CPLM Joglosemar X 1

Clasic parameters of Quality Control
Control of specimen acquisition
Control of method
Control of instrument
Control of reagents
Control of data distribution

Am J Clin Pathol. 1974, 62: 707–712
History
Lindberg alluded to Delta checking when he suggested that there
were limits (fluctuations) in hemoglobins or hematocrits
Method Inform Med., 1967, 6:97-107
Nosanchuk and Gottmann introduced Cum and delta check as a

systematic approach to quality control
Am J Clin Pathol.1974;62(5):707-712
Ladenson introduced a computer-based system of quality control

where patients were placed as their own controls to detect
laboratory error and called it as delta check system
Clin Chem.1975;21(11):1648-1653
Laboratory Error
Steps Type of error Rates
(%)
Pre- Inappropriate test request, Order entry error, 46-68
analytical Misidentification of patient, Container inappropriate,
Sample collection & transport inadequate, Inadequate
sample/anticoagulant volume ratio, Insuffiicient
sample volume, Sorting & routing errors, Labelling
error
Analytical Equipment malfunction, sample mix-ups/interference, 7 - 13
undetected failure in QC, Procedure not follow
Post Failure in reporting, errorneous validation of analytical 18.5 - 47
analytical data, inproper data entry
Clin. Chem. 2002, 48, 691–698

Labmedicine, 2012, 43(2): 41-44
Delta Check
• Can be expressed as the absolute or the
percent difference between two consecutive
results
• Can be an absolute limit
• Can be percent delta: the difference between
the larger result and the smaller result divided
by the smaller result.
• Time interval is flexible. Most hospital
laboratories choose 24 or 48 hours
http://www.clinlabnavigator.com/delta-check.html

A 36 yo woman, probable Pneumonia
Date 9/17 9/18 9/17
Time drawn 8 pm 7 am Re-check
WBC 6.800 4.300 4.000
RBC : M: 5.4 ± 0.8/cmm 4.7 4.9 4.9
F : 4.8 ± 0.6/cmm
Hemoglobin 15.1 13.1 13.1
Hematokrit 46 40 41
MCV 78 – 94 µ3 98 81 81
MCH 27-32 µµg 32 26 26
MCHC 32-36% 33 33 32
Explanation: wrong sample recorded Am J Clin Pathol. 1974, 62: 707–712

> 60% > 60%
Date/time of results for 03/09/2015 03/09/2015 03/09/2015

Patient @ 18:40 @ 23:10 @ 23:50
Creatinine 1.67mg/dL (↑) 0.35 mg/dL (↓) 1.83 mg/dL (↑)
Reference interval: 0.52 – [147.7 µmol/L] [31.0 µmol/L] [161.8 µmol/L]
1.04 mg/dL [45.6–92.0
µmol/L]
Potassium 5.0 mmol/L 1.2 mmol/L (↓) 4.9 mmol/L
Reference interval: 3.4–5.3
mmol/L
Urea Nitrogen 90 mg/dL (↑) 21 mg/dL 88 mg/dL (↑)
Reference interval: 7–30 [32.1 mmol/L] [7.5 mmol/L] [31.4 mmol/L]
mg/dL [2.5 –10.7 mmol/L]
Gruenberg et al., Clinical Biochemistry 2018 ( in press)

Causes of discrepant results
• Pre-analytical variations
– Patient misidentification
– Specimen related issues
– Post- collection
• Analytical variations
– Instrument
– Methods
• Biological variations
– Rhythmic changes
– Lifespan
– Treatment

Limits used to signal a delta check alert
• Derived from Biological Variation

– Sources of variation in laboratory measurements
– Biological variation
– Reference change values (RCV)
• Derived from Patient Data
– The empirical approach
– Delta check limits derived from the distribution of delta
values in the patient population
• Time interval between specimens, rate checks,
and clinically significant change
– Used in LIS

Index of Individuality (II)
Index of individuality (II) = (CVI2 + CVA2)1/2/CVG
If CVA < CVI, then the formula can be simplified
Index of individuality (II) = CVI /CVG
II ≥ 1.4 ---→ low

II ≤ 0.6 ---→ high
CVA = Analytical or day to day coefficient of variation
CVI = Intra-individual coefficient of variation
CVG = inter-individual coefficient of variation
J Avian Med Surg., 2014, 28(2): 118 - 126
Reference change value (RCV)
RCV = 1.414 X Zscore X [CVA2 + CVI2]1/2

CVA = analytical coeficient of variation
CVI = intra-individual biological coeficient of variation
individual
Z score 95% CI =1.96
Z score 99% CI = 2.58
Z score 99.9% CI = 3.29

Delta check limits based on RCV (%)
Clinica Chimica Acta., 2016, 463: 18 - 21

Clinically significant change
• PSA velocity
– > 2.0 ng/mL/year (> 2.0 μg/L/year)
– Stated in terms of rate checks
– Monitored on outpatients
• Rate of Troponin rise indicative of an acute coronary
event
– Various suggestions in the literature range from a 20% to a
50% rise from the previous result
– Stated in terms of absolute or percentage absolute terms
without specifying the time interval between specimens
– Monitored on inpatients

Delta Check Limit
• The allowable difference between consecutive
results for a specific analyte on the same
patient within a certain time interval.
• Should be set so that true changes in patient
test results are not flagged but improbable
changes are flagged as delta check failures.
• Should be based upon the total expected
variation, which include biological and
analytical variation

Delta check parameters
1. WBC change > 25%
2. RBC change > 25%
3. Hb change > 1 gr or 1%
4. Hct change > 3%
5. MCV change > 2 u3
6. MCH change 2 pg
7. MCHC change 2%
8. Segs or lymphs change by 25%
9. Bands change by more than 100%
10. Monos change by more than 100%
11. Eos change by more than 100%
Am J Clin Pathol. 1974, 62: 707–712
Single Parameter Check
• Anytime technologist has a question
• Unusual morphology: atypia, immaturity
• WBC < 3.000 or > 18.000
• MCV < 75 or > 105
• MCH > 32
• MCHC > 36
• Reticulocyte > 5%
• Low or high platelet estimates
• When techs rechecking disagree
Am J Clin Pathol. 1974, 62: 707–712
Delta Limit Time Frame
Analyte
Sodium 8 meq/L 30 hours
Chloride 8 meq/L 30 hours
Potassium 20% 30 hours
Carbon Dioxide 10 meq/L 30 hours
Creatinine 1.0 mg/dL 30 hours Recommended
BUN 20 mg/dL 30 hours parameter for delta
Calcium 2.0 mg/dL 30 hours check in clinical
Magnesium 1.0 mg/dL 30 hours chemistry
Phosphorus 2.0 mg/dL 30 hours
Albumin 1.5 mg/dL 30 hours
Total protein 2.0 mg/dL 30 hours
Recommended parameter for delta
check in hematology
• Delta checks should be applied to parameters that show
the least short-term biological variation
• MCV and MCHC are extremely stable in a patient over a
short interval, such as 24 hours
• The diurnal biological coefficient of variation in MCV is
only 0.5%.
• In emergency cases, such as hemorrhage, MCV and
MCHC do not change significantly since the reticulocyte
response does not begin for two to three days.
Recommended parameter for delta
check in hematology
• MCHC has the added benefit of detecting instrument
malfunction because it is calculated from hemoglobin,
MCV and RBC count
• Suggested delta check limits for MCV and MCHC are +/-
5 fl and +/-5.0 g/dL, respectively
• Delta checks are not recommended for other
hematology parameters including hemoglobin,
hematocrit, RBC count, WBC count or platelet count.
Delta Check Etiology
1968 1973
Explained by patient 94% 98%
pathophysiology, therapy or
natural course of disease
Unexplained 1% 1%
Laboratory-induced 5% < 1%
Am J Clin Pathol. 1974, 62: 707–712

Delta check for blood group
AJTS, 2017, 11(1): 18-21

Summary
• Delta check: comparing current patient values
to previous ones
• It is a systematic approach in addition to
quality control in order to improve quality of
care and patient safety and also to reduce
laboratory error
• It needs delta check limit for analysis

Summary
• The laboratory parameters which have the
lowest biological variation
• It is also can be applied for nominal data

28
08/05/2018 Simposium CPD CPLM Joglosemar X

Laboratory Management 2

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Management of Delta Check In

Department of Clinical Pathology and Laboratory

08/05/2018 Simposium CPD CPLM Joglosemar X 1

Control of specimen acquisition

Control of data distribution

Nosanchuk and Gottmann introduced Cum and delta check as a

Ladenson introduced a computer-based system of quality control

Clin. Chem. 2002, 48, 691–698

08/05/2018 Simposium CPD CPLM Joglosemar X 7

Explanation: wrong sample recorded Am J Clin Pathol. 1974, 62: 707–712

Date/time of results for 03/09/2015 03/09/2015 03/09/2015

Gruenberg et al., Clinical Biochemistry 2018 ( in press)

08/05/2018 Simposium CPD CPLM Joglosemar X 10

• Derived from Biological Variation

08/05/2018 Simposium CPD CPLM Joglosemar X 12

If CVA < CVI, then the formula can be simplified

Index of individuality (II) = CVI /CVG

II ≥ 1.4 ---→ low

RCV = 1.414 X Zscore X [CVA2 + CVI2]1/2

08/05/2018 Simposium CPD CPLM Joglosemar X 14

Clinica Chimica Acta., 2016, 463: 18 - 21

08/05/2018 Simposium CPD CPLM Joglosemar X 16

08/05/2018 Simposium CPD CPLM Joglosemar X 17

Am J Clin Pathol. 1974, 62: 707–712

AJTS, 2017, 11(1): 18-21

08/05/2018 Simposium CPD CPLM Joglosemar X 26

08/05/2018 Simposium CPD CPLM Joglosemar X 27

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