Celine - Automation

Question 1

Why is micro slow to change over to automation?
(5)

Answer 1

Micro too complex to automate -> there is a large variety of specimens, specimen collection systems, specimen processing and culture requirements

Automation can’t replace subjective decision, making skills and interpretative expertise required

High cost - complexity of specimens poor return on instrument investment

Scale of economy lost in micro - large scale tracking automation systems under-utilised

Microbiologists don’t like change

Question 2

What are the four main drivers for automation in micro

Answer 2

Increased demands on service increase by 10% per year

More challenges - mutli-resistant organisms, new pathogens

Reduced funding - reduced budget and staff number

Accreditation - need for standardisation and traceability

Question 3

Explain why automation is being introduced to the micro lab
(3)

Answer 3

Lab under immense pressure to produce faster, better, standardised results in face of increasing work volume

Microbiologist recognise that automation need not replace cognitive decision-making but rather replace tedious, repetitive steps

Automation offers the opportunity to reduce TAT, optimise workflow and reduce costs

Question 4

What happens on Day 1
(4)

Answer 4

Specimen in
- Microscopy
- Processing
- Culture
- Isolate

Question 5

What happens on day 2?

Answer 5

Identify
Susceptibility

Question 6

Comment on automation for day 1 specimen processing
(2)

Answer 6

Automated systems for specimen preparation and culture are complex

Front end processing only recently developed and only evident in large diagnostic micro labs

Question 7

Comment on automation for day 2, pathogen

Answer 7

Austomated systems for ID and AST first developed widespread use in all diagnostic micro labs

Question 8

Where is the most manual work done in micro

Answer 8

Plate and broth medium inoculation
Medium and plate reading

Question 9

Write about the role of automation in Day 1: Microscopic investigation of clinical specimen
(6)

Answer 9

Microscopic investigation consists of direct gram stain and/or white cell count (CSF and Urine)

Direct gram stain can be automated but microscopy is still manual

Microscopic cell count increasingly automated

Urine is the most common sample in the lab

Automation of urine microscopy using fluorescence flow cytometry

Negative screening method for urine -> 60-80% negative, if WCC count normal no need for culture

Question 10

What machine can be used for urine microscopy?

Answer 10

Sysmex UF-5000 - urine microscopy

Question 11

How does the Sysmex UF-5000 work?
(3)

Answer 11

Urine flow cytometer

Enumerates WBC, RBC, bacteria and epithelial cells by cell size and staining with fluorescent dyes

105 samples/hour

Question 12

Comment on the role of automation in Day 1 processing and culture
(6)

Answer 12

Remains largely manual

Front end processing evolving at a rapid pace

Liquid samples readily compatible with automation but swabs required manual handling

Liquid-based ESwab facilitated change

The Eswab sits in liquid media - vortex so flocked head releases organism into liquid media -> this allows for automated smear preparation for gram stain and for plate inoculation

New generation of liquid-based specimen processors now in large diagnostic labs with high specimen throughput

Question 13

Explain the role of Eswabs in automation

Answer 13

The Eswab sits in liquid media - vortex so flocked head releases organism into liquid media -> this allows for automated smear preparation for gram stain and for plate inoculation

Question 14

Give an example of a specimen processor used in the labs, capable of plate culture

Answer 14

WASP Processor (Copan Diagnostics)

Question 15

What is the WASP processor and how does it work
(8)

Answer 15

2 robot arms which move specimens and plates

Can work with all specimen types

Has 9 media silos and a capacity of 370 plates

Uses reusable chrome loops

Can inoculate 180 plates per hour

Can gram stain prep

Capable of auto decapping and recapping

Only one installed in Ireland

Question 16

Write about the role of automation in blood culture processing
(4)

Answer 16

Automation is important for the early detection of BSIs -> rapid diagnosis, prognosis and appropriate therapy

Automation for Blood cultures is well established

BacT/Alert SD is the most common BC system available

BacT/Alert SD allows for the continuous monitoring for detection of bacteria, fungi and mycobacteria

Question 17

What is a BC bottle
(3)

Answer 17

A blood culture bottle is used to investigate BSI

Blood is injected into bottles with culture media at bedside

The BC is then sent to the lab

Question 18

What is the most common BC automation system

Answer 18

BacT/Alert 3D

Question 19

What is the principle behind the BacT detecion system
(5)

Answer 19

If organisms are present in blood they will multiply in nutritious liquid media in BC bottle to generate CO2

CO2 production lowers the pH of the medium and produces a colour change in a sensor at the base of each bottle

Resins in the media neutralise antimicrobials in patient blood enhancing early recovery of pathogens

The bottles are constantly agitated and read every 10 minutes

When the bottle flags positive the bottle is removed from the BacTAlert -> withdraw a sample and perform a gram stain and culture on appropriate culture plates

Question 20

What is present in BC bottles that neutralise antimicrobials?

Answer 20

Resins

Question 21

What two aspects of confirming identification on Day 2 is compatible with automation

Answer 21

Detection of biochemical properties via Vitek/Manual

Determine protein profile via MALDI

Question 22

In general what is the Vitek 2 capable of doing

Answer 22

Identifying biochemical properties

Antimicrobial Susceptibility Testing

Question 23

In general what is the MALDI TOFF capable of doing

Answer 23

Id only based on protein profile

Question 24

In general what is the pheonix capable of?

Answer 24

Biochemical properties and AST

Question 25

Why is automation so important in pathogen identification
(2)

Answer 25

These systems (Vitek and MALDI) are reproducible, reduce hands on time and quicker turn around time

Systems are also interfaced with hospital computer systems - automate result entry

Question 26

What is the Vitek comprised of and how does it work?

Answer 26

Filler-sealer module -> draw bacterial suspension in 64 microwell card

Incubator and photometer to detect optical density for bacterial growth and biochemical reaction colour

Question 27

What are the five ID cards for the Vitek 2?
(5)

Answer 27

Gram negative
Gram positive
YST(Yeast)
Neisseria/Haemophilus
ANC (anaerobe)

Question 28

Explain in your own words how the vitek is used
(6)

Answer 28

Select the correct ID card

The Vitek will draw the bacterial suspension into the 64 microwells of the ID cardd

These wells contain test substrates which are used to measure a variety of metabolic activities, enzyme hydrolysis and growth in presence of inhibitory substrate

The growth/colour change is determined every 15 minutes

The series of 64 biochemical reactions is then compared to a database of known organisms

Gives results in 8 to 16 hours

Question 29

What is measured by the Vitek?
(2)

Answer 29

Metabolic activities

Enzyme hydrolysis and growth in presence of inhibitory substrate

Question 30

What does MALDI TOF stand for

Answer 30

Matrix-Assisted Laser Desorption/Ionisation - Time of Flight

Question 31

What is the MALDI-TOF MS used for

Answer 31

MALDI-TOF mass spectrometry used for species ID

Question 32

What are some of the benefits of MALDI?
(6)

Answer 32

Widely used for ID of bacteria and fungi

Its reproducible and sensitive - powerful tool

Analysis is very short -> TAT only takes 6 minutes/bacteria

Simple sample preparation and result acquisition

Cost is 5 times cheaper than conventional ID

MALDI analyses the protein composition of the organism -> there is no need to wait for growth -> can test directly on colony

Question 33

How is the MALDI used/How does it work?
(8)

Answer 33

Prepared single colonies from Day 2 plate used (directly or inactivated)

Spot colony on biotarget teflon plate

Add matrix (crystallized molecules), air dry, place on MALDI

Sample ionised with laser burst, releasing ‘cloud’ of proteins

Proteins accelerated with an electric charge through a flight tube to mass spectrometer

Time of flight recorder, lighter proteins travel faster than slower heavier ones

Protein profile determined by mass/charge ratio

Protein profile of test organism compared with profile database of well-characterized strains

Question 34

How do you prepare your colonies for MALDI

Answer 34

Single colonies from Day 2 plate used directly or inactivated with alcohol/formic acid which allows for cell wall disruption and protein extraction

Question 35

Where do you add your colony for the MALDI?

Answer 35

On biotarget teflon plate

Question 36

What do you add to your colony on the teflon plate for MALDI

Answer 36

Add matrix (crystallized molecules), air dry then place on MALDI

Question 37

What is the point of the matrix for MALDI

Answer 37

Acts as a buffer between bacteria and laser and helps ionise the sample, carrying it along the flight tube

Question 38

What is the most common MALDI-TOF instrument

Answer 38

Bruker Biotyper system

Question 39

Write about the Burker Biotyper system, how accurate is it?

Answer 39

98% ID at genus level
87% ID at species level
Misidentification most common in S. pneumonia, coagulase negative staph, and shigella Vs E. Coli
The database will expand to resolve many of the current identification problems

Question 40

Comment on the role of automation in AST
(5)

Answer 40

Many automated ID systems are adapted to accommodate automated susceptibility testing

Most common automated AST system is the Vitek 2

The AST cards contain 64 micro wells with a range of 8 to 9 antibiotics suitable for a wide range of organisms

Each antibiotic present at concentrations that convers the threshold/breakpoint for susceptible, intermediate and resistant

Employ short incubate with results in 8 to 16 hours

Question 41

AST can be measured using the VITEK for which organisms
(4)

Answer 41

Staphylococci
Streptococci
Enterobacterales
Pseudomonas

Question 42

Comment on future total lab automation
(2)

Answer 42

There are 2 Total lab automation microbiology systems in development

Th most common TLA system in Micro is the Kiestra

Question 43

What are some common features of the TLA systems
(4)

Answer 43

Robotic plate management to automate specimen processing and workup

Conveyor/track systems to move plates to and from incubators

Automated incubators with digital reading stations

Digital cameras capture plate images at timed intervals

Question 44

Is TLA a reality?
(7)

Answer 44

Total processing time takes 26 hours and AST appears feasible

They have been said to improve turn around time which could have a positive impact on clinical decisions and patient outcome

But there are few peer-reviewed publications

Benefits are inferred not proven

Need large studies to accurately assess the financial operation and clinical impacts of TLA

There have been 68 installations to date

One study found 2 fold in lab productivity despite 27% increase in workload but there was a decrease in 2.4 staff members

Question 45

What is molecular diagnostics considered the gold standard for?
(5)

Answer 45

Non-culturable organisms - viruses, chylamdiae
Fastidious organisms - N. gonorrhoeae
Slow growing orgnaisms - Mycobacteria
Important HCAI pathogens - MRSA, VRE
Multiple potential pathogens implicated

Question 46

Give an example of a piece of automation used for molecular diagnostics

Answer 46

COBAS 4800 Ct/Ng assay

Question 47

What is the COBAS 4800 Ct/Ng assay
(5)

Answer 47

Multi-plex Realtime PCR-C trachomatis and N. gonorrhoeae

System combines fully automated DNA extraction followed by PCR preparation + Real time PCR detection

97% sensitivity

Specimens include urine samples and genital samples

Processes 94 specimens in 5 hours with only 40 minutes hands-on-time

Question 48

Give the most commonly used automation in molecular diagnostics
(4)

Answer 48

GeneXpert Real Time PCR

DNA extraction, amplification and detection in a single cartridge

60 minutes turn around time

Swab samples transferred to cartridges and then inserted into machine

Question 49

Write about the Real-Time Enteric Bio Assay
(6)

Answer 49

EntericBio Gastro Panel 1

Real time PCR kit for simultaneous detection Campylobacter spp, Salmonella enterica, Shigella spp and Vero Cytotoxigenic E. Coli (VTEC)

Panel 2 plus Cryptosopidium + Giardia

Multiplex detection of pathogens directly from faeces without pre-enrichment or DNA extraction

PCR performed on Roche 480 Light Cycler Platform

3 hour turn around time

Question 50

Comment on automation in serology
(5)

Answer 50

Manual methods utilise ELISA-based micro-titre plate which is very labour intensive

Fully automated systems are widely used for Serology

Main application diagnosis of infection caused by non-culturable/slow growing/fastidious pathogens

Main application in virology for HBV, HCV, HIV, CMV

Main application in syphilis serology - STI agent

Question 51

Give three applications of automation in serology

Answer 51

Main application diagnosis of infection caused by non-culturable/slow growing/fastidious pathogens

Main application in virology for HBV, HCV, HIV, CMV

Main application in syphilis serology - STI agent

Question 52

Give an example of an analyser used in the automation of serology
(6)

Answer 52

Immunoassay analyser

Assays in Clinical Chemistry and Microbiology

Primary sampling - no sample separation required

Random access - multiple tests performed at the same time

65 sample load

Throughput 50-100 tests/hr