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October 2009
NBS03-ANewborn Screening for Preterm, Low Birth Weight, and Sick Newborns; Approved Guideline
This guideline outlines the recommended protocols for screening preterm, sick, or low birth weight infants for hearing loss and disorders detectable through dried blood spot testing.
A guideline for global application developed through the Clinical and Laboratory Standards Institute consensus process.
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Clinical and Laboratory Standards InstituteSetting the standard for quality in clinical laboratory testing around the world.
The Clinical and Laboratory Standards Institute (CLSI) is a not-for-profit membership organization that brings together the varied perspectives and expertise of the worldwide laboratory community for the advancement of a common cause: to foster excellence in laboratory medicine by developing and implementing clinical laboratory standards and guidelines that help laboratories fulfill their responsibilities with efficiency, effectiveness, and global applicability. Consensus Process
Consensus—the substantial agreement by materially affected, competent, and interested parties—is core to the development of all CLSI documents. It does not always connote unanimous agreement, but does mean that the participants in the development of a consensus document have considered and resolved all relevant objections and accept the resulting agreement. Commenting on Documents
CLSI documents undergo periodic evaluation and modification to keep pace with advancements in technologies, procedures, methods, and protocols affecting the laboratory or health care.
CLSI’s consensus process depends on experts who volunteer to serve as contributing authors and/or as participants in the reviewing and commenting process. At the end of each comment period, the committee that developed the document is obligated to review all comments, respond in writing to all substantive comments, and revise the draft document as appropriate.
Comments on published CLSI documents are equally essential, and may be submitted by anyone, at any time, on any document. All comments are addressed according to the consensus process by a committee of experts. Appeals Process
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For further information on committee participation or to submit comments, contact CLSI.
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NBS03-A
Vol. 29 No. 24
ISBN 1-56238-710-3 Formerly I/LA31-A
ISSN 0273-3099 Vol. 29 No. 24
Newborn Screening for Preterm, Low Birth Weight, and Sick Newborns;
Approved Guideline
Volume 29 Number 24 Julie Miller, BS
Judith Tuerck, MS, BS, RN
Khalid Awad, MD
Donald H. Chace, PhD, MSFS
Sara Copeland, MD
Sonja A. Rasmussen, MD, MS
Leanne Rien, RN, BS
Christina J. Valentine, MD, MS, RD
Dianne R. Webster, PhD, FHGSA
Bridget Wilcken, MBChB, FRACP, FRCPA
Abstract Clinical and Laboratory Standards Institute document NBS03-A—Newborn Screening for Preterm, Low Birth Weight, and Sick
Newborns; Approved Guideline addresses newborn screening of preterm, low birth weight (LBW), and sick newborns worldwide
to detect treatable conditions before physical damage can occur to the infant. In developed countries, advances in the treatment
they receive have improved survival rates, making the early detection of conditions detected by newborn screening even more
important. The physiological states associated with preterm, LBW, and sick newborns, and the treatments they receive, directly
affect the reliability of results for many conditions screened in public health dried blood spot and newborn hearing screening
systems. This guideline describes the effects of maternal and infant conditions, as well as treatments given to newborns. It also
provides the rationale for the recommended intervals for screening designed to minimize the risk of missing or delaying a
diagnosis in an affected newborn. It is intended for use by those involved in any aspect of newborn screening specimen collection
or hearing screening testing and follow-up, including health care providers, parents, public health professionals, and others
concerned with the health and welfare of newborns.
Clinical and Laboratory Standards Institute (CLSI). Newborn Screening for Preterm, Low Birth Weight, and Sick Newborns;
Approved Guideline. CLSI document NBS03-A (ISBN 1-56238-710-3). Clinical and Laboratory Standards Institute, 950 West
Valley Road, Suite 2500, Wayne, Pennsylvania 19087 USA, 2009.
The Clinical and Laboratory Standards Institute consensus process, which is the mechanism for moving a document through
two or more levels of review by the health care community, is an ongoing process. Users should expect revised editions of any
given document. Because rapid changes in technology may affect the procedures, methods, and protocols in a standard or
guideline, users should replace outdated editions with the current editions of CLSI documents. Current editions are listed in
the CLSI catalog and posted on our website at www.clsi.org. If your organization is not a member and would like to become
one, and to request a copy of the catalog, contact us at: Telephone: 610.688.0100; Fax: 610.688.0700; E-Mail:
[email protected]; Website: www.clsi.org.
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Number 24 NBS03-A
ii
Copyright ©2009 Clinical and Laboratory Standards Institute. Except as stated below, any reproduction of
content from a CLSI copyrighted standard, guideline, companion product, or other material requires
express written consent from CLSI. All rights reserved. Interested parties may send permission requests to
CLSI hereby grants permission to each individual member or purchaser to make a single reproduction of
this publication for use in its laboratory procedure manual at a single site. To request permission to use
this publication in any other manner, e-mail [email protected].
Suggested Citation
CLSI. Newborn Screening for Preterm, Low Birth Weight, and Sick Newborns; Approved Guideline.
CLSI document NBS03-A. Wayne, PA: Clinical and Laboratory Standards Institute; 2009.
Proposed Guideline December 2008
Approved Guideline October 2009
ISBN 1-56238-710-3
ISSN 0273-3099
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Volume 29 NBS03-A
v
Contents
Abstract .................................................................................................................................................... i
Committee Membership ........................................................................................................................ iii
Foreword .............................................................................................................................................. vii
1 Scope .......................................................................................................................................... 1
2 Introduction ................................................................................................................................ 1
3 Standard Precautions .................................................................................................................. 2
4 Terminology ............................................................................................................................... 3
4.1 A Note on Terminology ................................................................................................ 3 4.2 Definitions .................................................................................................................... 3 4.3 Abbreviations and Acronyms ....................................................................................... 5
5 General Considerations .............................................................................................................. 6
6 Maternal Conditions and Treatment and Their Effects on Newborn Screening Results ........... 6
6.1 Thyroid Dysfunction ..................................................................................................... 6 6.2 Steroids ......................................................................................................................... 7 6.3 Maternal and Infant Conditions Detectable by Tandem Mass Spectrometry ............... 7
7 Effects of Preterm Birth and Special Care Baby Unit Interventions on Newborn Screening .... 8
7.1 Routine Special Care Baby Unit Interventions ............................................................. 8
8 Disorders on Screening Panels ................................................................................................. 11
8.1 Cystic Fibrosis ............................................................................................................ 14 8.2 Congenital Hypothyroidism ........................................................................................ 14 8.3 Urea Cycle Defects, Organic Acidemias, and Aminoacidopathies ............................. 15 8.4 Fatty Acid Oxidation Defects ..................................................................................... 16 8.5 Enzymopathies: Galactosemia and Biotinidase Deficiency ........................................ 16 8.6 Sickle Cell Disease and Hemoglobinopathies ............................................................ 17
9 Difficulties With Current Special Care Baby Unit Protocols for Newborn Screening ............ 17
9.1 Pretreatment Screening ............................................................................................... 18
10 General Recommendations for Blood Spot Screening of Preterm, Low Birth Weight,
and Sick Infants ....................................................................................................................... 19
10.1 Blood Spot Screening Primary Recommendation ...................................................... 19 10.2 On Admission to the Special Care Baby Unit for Blood Spot Testing ....................... 19 10.3 Day of Life 48 to 72 Hours ......................................................................................... 20 10.4 Day of Life 28 ............................................................................................................. 21 10.5 Alternative Recommendation for Blood Spot Collection Timing .............................. 23 10.6 Admission to the Special Care Baby Unit After 24 to 48 Hours of Life
or Pretransfusion, Preparenteral Nutrition .................................................................. 24
11 Recommendations for Special Care Baby Unit Infants Not Screened as Recommended ....... 24
11.1 Special Considerations for Timing of Blood Specimen Collection
(in the Event of Deviation From Established Protocols) ............................................ 24
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Contents (Continued)
12 Hearing Screening for Special Care Baby Unit Infants ........................................................... 24
12.1 Risk Factors for Hearing Loss in the Special Care Baby Unit .................................... 24 12.2 Special Circumstances Related to the Special Care Baby Unit .................................. 25
13 Roles of the Newborn Screening Follow-up ............................................................................ 25
14 Evaluation and Quality Assurance ........................................................................................... 26
15 Research Opportunities and Education .................................................................................... 27
References ............................................................................................................................................. 29
Appendix A. Summary of Factors in Preterm/Sick Infants Affecting Reliability of Newborn
Screening Results .................................................................................................................................. 32
Appendix B. Summary of Conditions Included on Screening Panels................................................... 34
Summary of Delegate Comments and Subcommittee Responses ......................................................... 48
The Quality Management System Approach ........................................................................................ 68
Related CLSI Reference Materials ....................................................................................................... 69
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Foreword
There are approximately 127 million births per year worldwide.1 In the United States, in 2005 4.1 million
infants were born, and 8.2% of those infants were low birth weight, 12.7% were preterm (< 37 weeks’
gestation), and 3% were born with birth defects.2 In developed and developing countries, these infants are
usually cared for in specially equipped wards or units such as special care baby units (SCBUs) sometimes
referred to as neonatal intensive care units (NICUs). For the purpose of this document, SCBU is used to
represent these levels of nursery care.
Preterm birth is defined as a gestational age of less than 37 completed weeks and low birth weight (LBW)
as less than 2500 g. In some countries, approximately 25% of infants are less than this weight and may or
may not be considered candidates in need of the specialized care. Tremendous advances in the care of
preterm infants have resulted in improved survivability for increasingly smaller and more preterm infants.
Today in developed countries, infants of 28 weeks’ gestation or older have a > 96% chance of survival,
with the lower limits of viability at about 22 weeks, with only 2% of these infants surviving.2
Newborn screening (NBS) systems and laboratory technology have evolved as well, with the addition of
isoelectric focusing and high-performance liquid chromatography for hemoglobinopathies, enzyme assays
for biotinidase deficiency and galactosemia, DNA analysis for cystic fibrosis and hemoglobinopathy
screening, and tandem mass spectrometry (MS/MS) for metabolic disorders and other multiplex screening
tests. It is now possible to screen for a large number of conditions. As of 2008, more than 50 conditions
are included in blood spot screening panels in some NBS programs.3 In addition, most infants are now
screened for hearing loss before discharge from the birth facility. Including hearing screening, the
collective incidence of disorders for which NBS is available is 1:250 infants compared with 1:3000 only
10 years ago.4 New tests for additional conditions are under development, undergoing pilot testing, or
both in many parts of the world. With the pace of technologic and therapeutic advances, it is certain that
more conditions will be added to NBS panels in the future.
As more conditions are added, it becomes increasingly difficult to advise practitioners about the ideal
time to collect an NBS specimen. Each condition has its own best ‘screening window’ when there is the
greatest chance of diagnosing and treating the disorder in question before symptoms or permanent
damage occurs. Some conditions, such as maple syrup urine disease (MSUD), galactosemia, and
congenital adrenal hyperplasia, have very short screening windows, with abnormal analytes present in the
first day or so of life, illness beginning by the end of the first week, and death in the second week if not
diagnosed. Therefore, the best time to collect specimens for those disorders that necessitate early
treatment is in the first 24 to 48 hours, and specimens collected after four days may be too late to prevent
death or damage. Other conditions, such as homocystinuria, are difficult to detect on a specimen collected
in the first 24 to 48 hours of life because the analyte currently used in many programs, methionine, rises
very slowly in affected infants and may not be elevated for several days to a week. Likewise, in some
infants with congenital hypothyroidism, the decline in thyroid hormone (thyroxine – T4) and rise in
thyroid-stimulating hormone (thyrotropin – TSH), analytes commonly used to detect the condition, may
not occur for several days (or longer) if the infant has a large ectopic gland producing sufficient T4 to
suppress TSH production at birth. Because maturation of the hypothalamic-pituitary axis at birth is
insufficient to produce TSH in very low birth weight (VLBW) infants, these infants with hypothyroidism
often have low or normal TSH levels at birth and may not be identified on a screening specimen collected
at less than one week of age.5 Specimen collection timing varies around the world; in Europe and
Australia-Asia, most specimens are collected at 48 to 72 hours of age; in the United States, before 48
hours of age; and in Great Britain, infants are not screened until the fifth to eighth day of life.6 No
published data on age at collection were found for the Latin American or Middle East/South African
regions.
Unfortunately, SCBU infants are at greater risk for missed or incomplete NBS than normal newborns
owing to the focus on the critical activities surrounding their care, their pre- and postnatal environments,
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the treatments given to them, and the unique genetic and biochemical nature of the infants themselves.
These factors can negatively affect both the quality and validity of the screening results for many of the
disorders included in NBS panels. As a result, SCBU infants are much more likely to have false-positive
or false-negative results after NBS and thus, they account for a disproportionate follow-up effort,
compared with normal newborns. Preterm, LBW, or sick term infants often have multiple NBSs and
diagnostic specimens collected in an attempt to clarify the significance of an out-of-range result. At the
other extreme, collection of NBS specimens can be overlooked in the complexity of activities that occur
in the SCBU. These factors increase the chance that a newborn requiring SCBU care will not have a
condition detectable by NBS identified in a timely manner, with potentially catastrophic results.7-9
Although a few case reports have documented the presence of this problem, studies assessing its
magnitude have not been performed.
During the development of this guideline, experts in neonatology, NBS, endocrinology, metabolism,
hematology, hearing loss, genetics, and cystic fibrosis worked collectively to outline factors that interfere
with the reliability of NBS, review the significance and duration of the interference, and provide
recommendations for NBS specimen collection, including information on timing and number of
specimens. This guideline is in agreement with existing consensus guidelines, including those from CLSI
(see CLSI documents I/LA2710 and LA0411) and various neonatology organizations.12-14 This guideline
provides reference for NBS programs and SCBUs to develop and provide screening, testing and follow-
up protocols. The goal is to complete NBS for every SCBU infant in the shortest period of time, with the
highest degree of reliability and using the fewest number of specimens. It is hoped that individual NBS
programs will adopt this guideline to standardize procedures for intensive care practitioners, and most
important, to improve the quality of NBS and follow-up for all infants in their jurisdictions.
Key Words
Best practices, congenital anomalies, low birth weight, newborn hearing screening, newborn screening,
preterm birth, sick infants, special care baby unit
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Volume 29 NBS03-A
©Clinical and Laboratory Standards Institute. All rights reserved. 1
Newborn Screening for Preterm, Low Birth Weight, and Sick Newborns;
Approved Guideline
1 Scope
This guideline addresses best practices for SCBU personnel, as well as primary health care providers,
laboratory, and follow-up personnel to provide all preterm, LBW, and sick infants with valid newborn
blood spot and hearing screening. Best practices are defined with consideration of the conditions screened
for and timing of screening events. Special circumstances include the condition of the infant, treatments
given, maternal conditions/therapies, and other factors. This document does not intend to dictate SCBU
care practices.
Goals of this guideline are to
1) Ensure rapid, consistent, and complete blood spot and hearing screening, including appropriate
follow-up to ensure early diagnosis and treatment for preterm, LBW, or sick newborns affected with a
screened condition.
2) Minimize the risk of a missed or delayed diagnosis and treatment for all screened conditions.
3) Optimize the timing and minimize the number of blood spot specimen collections and hearing
screening events.
4) Define essential elements of quality assurance relevant to this guideline.
5) Provide education on the effects of SCBU treatments on newborn blood spot and hearing screening.
6) Identify areas needing further research.
2 Introduction
This guideline is a part of a series produced by CLSI over the last several years that includes related CLSI
documents LA0411 and I/LA27.10 These documents provide more detail regarding the structure and
function of specific elements of NBS systems, and this information is not duplicated here, except for a
discussion of proposed reporting and follow-up algorithms. This document focuses on treatments and
practices within the SCBU and neonatal conditions that are either known or suspected to interfere with
valid NBS, the consequences of the interference, and recommendations for avoiding or counteracting
these problems.
Care and treatment of preterm, LBW, and sick infants and improvements to NBS programs have made
great advancements, but little is known as to the impact of one on the other. The effects of preterm birth
and its associated treatment are partially understood for certain disorders on NBS panels, for example,
endocrine disorders, hemoglobinopathies, enzymopathies such as galactosemia, and cystic fibrosis (CF).
However, very little is known about most metabolic disorders. Simple questions such as how long
parenteral nutrition (PN) affects results on amino acid tests are unknown at this time, and this document
reflects areas where no data exist. Further research is urgently needed. Because no test has been proven to
produce results consistently with 100% sensitivity and specificity, including those used in NBS,
practitioners should be reminded to remain vigilant for signs and symptoms associated with screened
conditions, even in the presence of normal NBS results.
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©Clinical and Laboratory Standards Institute. All rights reserved. 2
Beyond individual case reports, the number of affected SCBU infants missed because of incomplete or no
screening is unknown. Any missed case, however, represents a failure of the system and a double tragedy
for the infant and family, who have already endured the rigors of survival for preterm birth, LBW, or
other neonatal illness and now must face lifelong damage to their child usually as a result of a simple
mistake or omission.
The complexity and number of factors in SCBU infants and the associated treatments that can affect NBS
assays are challenging; and an even larger number of factors are not currently understood. This
underscores a need for more consultation between neonatologists and NBS professionals. With the
addition of more conditions to NBS panels and continuous advances and new treatments in SCBUs, the
problem will only grow with time. It is advisable to have formal working relationships between NBS
programs and neonatologists on the local level, and for neonatologists to be involved at the national and
international level in advising on NBS policy issues. All NBS and SCBU staff urgently need to be
educated about all the known factors, to implement SCBU standard protocols within screening
jurisdictions, and to encourage research collaboration. This guideline does not attempt to address data
systems in SCBUs that might facilitate implementation of this document. However, the document does
recognize that more than one SCBU may be located in different cities, which could greatly enhance the
complexity of implementation of laboratory information system (LIS) codes and procedures that should
be uniform for all babies.
Those professionals who work in NBS programs and SCBU units are well aware of the frequency of
“flagged” results among these infants. Even with adjusted cutoffs, many if not most LBW infants have
some abnormality on NBS that must be resolved. This results in more screening specimens, confirmatory
testing, or both being ordered; the vast majority eventually provided false-positive results. Unfortunately,
sensitivity and specificity of non–DNA-based assays are inversely related, making it impossible to
calibrate NBS assays to find no false-positive results, because this would greatly increase the probability
of a false-negative finding, defeating the goal of NBS to find the maximum number of affected infants.
As a result, approximately 2% to 10% of all NBS specimens are flagged as abnormal or the specimen
itself is rejected for collection and handling problems. Of all abnormal NBS specimens, 10% to 40%
belong to infants in SCBUs. With no standard protocol for screening or follow-up in this population,
neonatologists and other nursery staff must cope with different recommendations that vary from program
to program. Uniform recommendations crossing jurisdictional boundaries would perhaps increase
adherence to them.
This guideline represents a starting point for developing harmonious consensus with NBS programs and
SCBUs worldwide, but consensus requires NBS programs to adopt and evaluate the guidelines and to
recommend adjustments as necessary. It is very important to ensure that guidelines improve screening for
SCBU infants and prevent infants from being missed.
3 Standard Precautions
Because it is often impossible to know what isolates or specimens might be infectious, all patient and
laboratory specimens are treated as infectious and handled according to “standard precautions.” Standard
precautions are guidelines that combine the major features of “universal precautions and body substance
isolation” practices. Standard precautions cover the transmission of all infectious agents and thus are
more comprehensive than universal precautions, which are intended to apply only to transmission of
blood-borne pathogens. Standard and universal precaution guidelines are available from the US Centers
for Disease Control and Prevention.15 For specific precautions for preventing the laboratory transmission
of all infectious agents from laboratory instruments and materials and for recommendations for the
management of exposure to all infectious diseases, refer to CLSI document M29.16
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©
Clinical and Laboratory Standards Institute. All rights reserved. 68
The Quality Management System Approach Clinical and Laboratory Standards Institute (CLSI) subscribes to a quality management system approach in the
development of standards and guidelines, which facilitates project management; defines a document structure via a
template; and provides a process to identify needed documents. The approach is based on the model presented in the
most current edition of CLSI/NCCLS document HS01—A Quality Management System Model for Health Care. The
quality management system approach applies a core set of “quality system essentials” (QSEs), basic to any
organization, to all operations in any health care service’s path of workflow (ie, operational aspects that define how
a particular product or service is provided). The QSEs provide the framework for delivery of any type of product or
service, serving as a manager’s guide. The QSEs are
Documents and Records Equipment Information Management Process Improvement
Organization Purchasing and Inventory Occurrence Management Customer Service
Personnel Process Control Assessment—External
and Internal
Facilities and Safety
NBS03-A addresses the QSEs indicated by an “X.” For a description of the other documents listed in the grid, please
refer to the Related CLSI Reference Materials section on the following page.
Do
cum
ents
and
Rec
ord
s
Org
aniz
atio
n
Per
son
nel
Equ
ipm
ent
Pu
rchas
ing
and
Inv
ento
ry
Pro
cess
Co
ntr
ol
Info
rmat
ion
Man
agem
ent
Occ
urr
ence
Man
agem
ent
Ass
essm
ent—
Exte
rnal
and
Inte
rnal
Pro
cess
Imp
rov
emen
t
Cu
sto
mer
Ser
vic
e
Fac
ilit
ies
and
Saf
ety
X
I/LA27
LA04
M29
M29
Adapted from CLSI/NCCLS document HS01—A Quality Management System Model for Health Care.
Path of Workflow
A path of workflow is the description of the necessary steps to deliver the particular product or service that the
organization or entity provides. For example, CLSI/NCCLS document GP26Application of a Quality
Management System Model for Laboratory Services defines a clinical laboratory path of workflow, which consists
of three sequential processes: preexamination, examination, and postexamination. All clinical laboratories follow
these processes to deliver the laboratory’s services, namely quality laboratory information.
NBS03-A addresses the clinical laboratory path of workflow steps indicated by an “X.” For a description of the
other documents listed in the grid, please refer to the Related CLSI Reference Materials section on the following
page.
Preexamination Examination Postexamination
Ex
amin
atio
n
ord
erin
g
Sam
ple
co
llec
tio
n
Sam
ple
tra
nsp
ort
Sam
ple
rece
ipt/
pro
cess
ing
Ex
amin
atio
n
Res
ult
s re
vie
w
and
fo
llo
w-u
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Inte
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on
Res
ult
s re
po
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and
arc
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ing
Sam
ple
man
agem
ent
LA04 LA04 LA04 LA04 LA04 LA04
Adapted from CLSI/NCCLS document HS01—A Quality Management System Model for Health Care.
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Volume 29 NBS03-A
©Clinical and Laboratory Standards Institute. All rights reserved. 69
Related CLSI Reference Materials I/LA27-A Newborn Screening Follow-up; Approved Guideline (2006). This guideline describes the basic
principles, scope, and range of follow-up activities within the newborn screening system.
LA04-A5 Blood Collection on Filter Paper for Newborn Screening Programs; Approved Standard—Fifth
Edition (2007). This document addresses the issues associated with specimen collection, the filter paper
collection device, and the application of blood to filter paper, and provides uniform techniques for
collecting the best possible specimen for use in newborn screening programs.
M29-A3 Protection of Laboratory Workers From Occupationally Acquired Infections; Approved
Guideline—Third Edition (2005). Based on US regulations, this document provides guidance on the
risk of transmission of infectious agents by aerosols, droplets, blood, and body substances in a
laboratory setting; specific precautions for preventing the laboratory transmission of microbial infection
from laboratory instruments and materials; and recommendations for the management of exposure to
infectious agents.
CLSI documents are continually reviewed and revised through the CLSI consensus process; therefore, readers should refer to
the most current editions.
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