HB2661 Enrolled LRB098 09098 RPM 39235 b
1		AN ACT concerning health facilities.
2		Be it enacted by the People of the State of Illinois,
3		represented in the General Assembly:
4		Section 5. The Newborn Metabolic Screening Act is amended
5		by changing Sections 1, 1.5, and 2 and by adding Sections 1.10,
6		3.1, 3.2, and 3.3 as follows:
7		(410 ILCS 240/1)  (from Ch. 111 1/2, par. 4903)
8		Sec. 1. The Illinois Department of Public Health shall
9		promulgate and enforce rules and regulations requiring that
10		every newborn be subjected to tests for genetic,
11		phenylketonuria, hypothyroidism, galactosemia and such other
12		metabolic, and congenital anomalies diseases as the Department
13		may deem necessary from time to time. The Department is
14		empowered to promulgate such additional rules and regulations
15		as are found necessary for the administration of this Act,
16		including mandatory reporting of the results of all tests for
17		these conditions to the Illinois Department of Public Health.
18		(Source: P.A. 83-87.)
19		(410 ILCS 240/1.5)
20		Sec. 1.5. Definitions. In this Act:
21		"Accredited laboratory" means any laboratory that holds a
22		valid certificate issued under the Clinical Laboratory

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1		Improvement Amendments of 1988, 102 Stat. 2903, 42 U.S.C. 263a,
2		as amended, and that reports its screening results by using
3		normal pediatric reference ranges.
4		"Department" means the Department of Public Health.
5		"Expanded screening" means screening for genetic and
6		metabolic disorders, including but not limited to amino acid
7		disorders, organic acid disorders, fatty acid oxidation
8		disorders, and other abnormal profiles, in newborn infants that
9		can be detected through the use of a tandem mass spectrometer.
10		"Tandem mass spectrometer" means an analytical instrument
11		used to detect numerous genetic and metabolic disorders at one
12		time.
13		(Source: P.A. 92-701, eff. 7-19-02.)
14		(410 ILCS 240/1.10 new)
15		Sec. 1.10. Critical congenital heart disease.
16		(a) The General Assembly finds as follows:
17		(1) According to the United States Secretary of Health
18		and Human Services Advisory Committee on Heritable
19		Disorders in Newborns and Children, congenital heart
20		disease affects approximately 7 to 9 of every 1,000 live
21		births in the United States and Europe. The federal Centers
22		for Disease Control and Prevention state that critical
23		congenital heart disease is the leading cause of infant
24		death due to birth defects.
25		(2) Many newborn lives could potentially be saved by

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1		earlier detection and treatment of critical congenital
2		heart disease if health care facilities in the State were
3		required to perform a simple, non-invasive newborn
4		screening in conjunction with current screening methods.
5		(b) The Department shall require that screening tests for
6		critical congenital heart defects be performed at birthing
7		hospitals and birth centers in accordance with a testing
8		protocol adopted by the Department, by rule, in line with
9		current standards of care, such as pulse oximetry screening,
10		and may authorize screening tests for additional congenital
11		anomalies to be performed at birthing hospitals and birth
12		centers in accordance with a testing protocol adopted by the
13		Department, by rule.
14		(c) The Department may authorize health care facilities to
15		report screening test results and follow-up information.
16		(410 ILCS 240/2)  (from Ch. 111 1/2, par. 4904)
17		Sec. 2. General provisions. The Department of Public Health
18		shall administer the provisions of this Act and shall:
19		(a) Institute and carry on an intensive educational program
20		among physicians, hospitals, public health nurses and the
21		public concerning disorders included in newborn screening the
22		diseases phenylketonuria, hypothyroidism, galactosemia and
23		other metabolic diseases. This educational program shall
24		include information about the nature of the diseases and
25		examinations for the detection of the diseases in early infancy

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1		in order that measures may be taken to prevent the intellectual
2		disabilities resulting from the diseases.
3		(a-5) Require that Beginning July 1, 2002, provide all
4		newborns be screened with expanded screening tests for the
5		presence of certain genetic, metabolic, and congenital
6		anomalies as determined by the Department, by rule.
7		(a-5.1) Require that all blood and biological specimens
8		collected pursuant to this Act or the rules adopted under this
9		Act be submitted for testing to the nearest Department
10		laboratory designated to perform such tests. The following
11		provisions shall apply concerning testing:
12		(1) The Department may develop a reasonable fee
13		structure and may levy fees according to such structure to
14		cover the cost of providing this testing service and for
15		the follow-up of infants with an abnormal screening test.
16		Fees collected from the provision of this testing service
17		shall be placed in the Metabolic Screening and Treatment
18		Fund. Other State and federal funds for expenses related to
19		metabolic screening, follow-up, and treatment programs may
20		also be placed in the Fund.
21		(2) Moneys shall be appropriated from the Fund to the
22		Department solely for the purposes of providing newborn
23		screening, follow-up, and treatment programs. Nothing in
24		this Act shall be construed to prohibit any licensed
25		medical facility from collecting additional specimens for
26		testing for metabolic or neonatal diseases or any other

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1		diseases or conditions, as it deems fit. Any person
2		violating the provisions of this subsection (a-5.1) is
3		guilty of a petty offense. endocrine, or other metabolic
4		disorders, including phenylketonuria, galactosemia,
5		hypothyroidism, congenital adrenal hyperplasia,
6		biotinidase deficiency, and sickling disorders, as well as
7		other amino acid disorders, organic acid disorders, fatty
8		acid oxidation disorders, and other abnormalities
9		detectable through the use of a tandem mass spectrometer.
10		(3) If by July 1, 2002, the Department is unable to
11		provide the expanded screening using the State Laboratory,
12		it shall temporarily provide such screening through an
13		accredited laboratory selected by the Department until the
14		Department has the capacity to provide screening through
15		the State Laboratory. If expanded screening is provided on
16		a temporary basis through an accredited laboratory, the
17		Department shall substitute the fee charged by the
18		accredited laboratory, plus a 5% surcharge for
19		documentation and handling, for the fee authorized in this
20		subsection (a-5.1) (e) of this Section.
21		(a-5.2) Maintain a registry of cases, including
22		information of importance for the purpose of follow-up services
23		to assess long-term outcomes.
24		(a-5.3) Supply the necessary metabolic treatment formulas
25		where practicable for diagnosed cases of amino acid metabolism
26		disorders, including phenylketonuria, organic acid disorders,

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1		and fatty acid oxidation disorders for as long as medically
2		indicated, when the product is not available through other
3		State agencies.
4		(a-5.4) Arrange for or provide public health nursing,
5		nutrition, and social services and clinical consultation as
6		indicated.
7		(a-5.5) The Department shall utilize the Genetic and
8		Metabolic Diseases Advisory Committee established under the
9		Genetic and Metabolic Diseases Advisory Committee Act to
10		provide guidance and recommendations to the Department's
11		newborn screening program. The Genetic and Metabolic Diseases
12		Advisory Committee shall review the feasibility and
13		advisability of including additional metabolic, genetic, and
14		congenital disorders in the newborn screening panel, according
15		to a review protocol applied to each suggested addition to the
16		screening panel. The Department shall consider the
17		recommendations of the Genetic and Metabolic Diseases Advisory
18		Committee in determining whether to include an additional
19		disorder in the screening panel prior to proposing an
20		administrative rule concerning inclusion of an additional
21		disorder in the newborn screening panel. Notwithstanding any
22		other provision of law, no new screening may begin prior to the
23		occurrence of all the following:
24		(1) the establishment and verification of relevant and
25		appropriate performance specifications as defined under
26		the federal Clinical Laboratory Improvement Amendments and

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1		regulations thereunder for U.S. Food and Drug
2		Administration-cleared or in-house developed methods,
3		performed under an institutional review board-approved
4		protocol, if required;
5		(2) the availability of quality assurance testing
6		methodology for the processes set forth in item (1) of this
7		subsection (a-5.5);
8		(3) the acquisition and installment by the Department
9		of the equipment necessary to implement the screening
10		tests;
11		(4) the establishment of precise threshold values
12		ensuring defined disorder identification for each
13		screening test;
14		(5) the authentication of pilot testing achieving each
15		milestone described in items (1) through (4) of this
16		subsection (a-5.5) for each disorder screening test; and
17		(6) the authentication of achieving the potential of
18		high throughput standards for statewide volume of each
19		disorder screening test concomitant with each milestone
20		described in items (1) through (4) of this subsection
21		(a-5.5).
22		(a-6) (Blank). In accordance with the timetable specified
23		in this subsection, provide all newborns with expanded
24		screening tests for the presence of certain Lysosomal Storage
25		Disorders known as Krabbe, Pompe, Gaucher, Fabry, and
26		Niemann-Pick. The testing shall begin within 6 months following

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1		the occurrence of all of the following:
2		(i) the establishment and verification of relevant and
3		appropriate performance specifications as defined under
4		the federal Clinical Laboratory Improvement Amendments and
5		regulations thereunder for Federal Drug
6		Administration-cleared or in-house developed methods,
7		performed under an institutional review board approved
8		protocol, if required;
9		(ii) the availability of quality assurance testing
10		methodology for these processes;
11		(iii) the acquisition and installment by the
12		Department of the equipment necessary to implement the
13		expanded screening tests;
14		(iv) establishment of precise threshold values
15		ensuring defined disorder identification for each
16		screening test;
17		(v) authentication of pilot testing achieving each
18		milestone described in items (i) through (iv) of this
19		subsection (a-6) for each disorder screening test; and
20		(vi) authentication achieving potentiality of high
21		throughput standards for statewide volume of each disorder
22		screening test concomitant with each milestone described
23		in items (i) through (iv) of this subsection (a-6).
24		It is the goal of Public Act 97-532 that the expanded
25		screening for the specified Lysosomal Storage Disorders begins
26		within 2 years after August 23, 2011 (the effective date of

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1		Public Act 97-532). The Department is authorized to implement
2		an additional fee for the screening prior to beginning the
3		testing in order to accumulate the resources for start-up and
4		other costs associated with implementation of the screening and
5		thereafter to support the costs associated with screening and
6		follow-up programs for the specified Lysosomal Storage
7		Disorders.
8		(a-7) (Blank). In accordance with the timetable specified
9		in this subsection (a-7), provide all newborns with expanded
10		screening tests for the presence of Severe Combined
11		Immunodeficiency Disease (SCID). The testing shall begin
12		within 12 months following the occurrence of all of the
13		following:
14		(i) the establishment and verification of relevant and
15		appropriate performance specifications as defined under
16		the federal Clinical Laboratory Improvement Amendments and
17		regulations thereunder for Federal Drug
18		Administration-cleared or in-house developed methods,
19		performed under an institutional review board approved
20		protocol, if required;
21		(ii) the availability of quality assurance testing and
22		comparative threshold values for SCID;
23		(iii) the acquisition and installment by the
24		Department of the equipment necessary to implement the
25		initial pilot and expanded statewide volume of screening
26		tests for SCID;

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1		(iv) establishment of precise threshold values
2		ensuring defined disorder identification for SCID;
3		(v) authentication of pilot testing achieving each
4		milestone described in items (i) through (iv) of this
5		subsection (a-7) for SCID; and
6		(vi) authentication achieving potentiality of high
7		throughput standards for statewide volume of the SCID
8		screening test concomitant with each milestone described
9		in items (i) through (iv) of this subsection (a-7).
10		It is the goal of Public Act 97-532 that the expanded
11		screening for Severe Combined Immunodeficiency Disease begins
12		within 2 years after August 23, 2011 (the effective date of
13		Public Act 97-532). The Department is authorized to implement
14		an additional fee for the screening prior to beginning the
15		testing in order to accumulate the resources for start-up and
16		other costs associated with implementation of the screening and
17		thereafter to support the costs associated with screening and
18		follow-up programs for Severe Combined Immunodeficiency
19		Disease.
20		(a-8) (Blank). In accordance with the timetable specified
21		in this subsection (a-8), provide all newborns with expanded
22		screening tests for the presence of certain Lysosomal Storage
23		Disorders known as Mucopolysaccharidosis I (Hurlers) and
24		Mucopolysaccharidosis II (Hunters). The testing shall begin
25		within 12 months following the occurrence of all of the
26		following:

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1		(i) the establishment and verification of relevant and
2		appropriate performance specifications as defined under
3		the federal Clinical Laboratory Improvement Amendments and
4		regulations thereunder for Federal Drug
5		Administration-cleared or in-house developed methods,
6		performed under an institutional review board approved
7		protocol, if required;
8		(ii) the availability of quality assurance testing and
9		comparative threshold values for each screening test and
10		accompanying disorder;
11		(iii) the acquisition and installment by the
12		Department of the equipment necessary to implement the
13		initial pilot and expanded statewide volume of screening
14		tests for each disorder;
15		(iv) establishment of precise threshold values
16		ensuring defined disorder identification for each
17		screening test;
18		(v) authentication of pilot testing achieving each
19		milestone described in items (i) through (iv) of this
20		subsection (a-8) for each disorder screening test; and
21		(vi) authentication achieving potentiality of high
22		throughput standards for statewide volume of each disorder
23		screening test concomitant with each milestone described
24		in items (i) through (iv) of this subsection (a-8).
25		It is the goal of Public Act 97-532 that the expanded
26		screening for the specified Lysosomal Storage Disorders begins

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1		within 3 years after August 23, 2011 (the effective date of
2		Public Act 97-532). The Department is authorized to implement
3		an additional fee for the screening prior to beginning the
4		testing in order to accumulate the resources for start-up and
5		other costs associated with implementation of the screening and
6		thereafter to support the costs associated with screening and
7		follow-up programs for the specified Lysosomal Storage
8		Disorders.
9		(b) (Blank). Maintain a registry of cases including
10		information of importance for the purpose of follow-up services
11		to prevent intellectual disabilities.
12		(c) (Blank). Supply the necessary metabolic treatment
13		formulas where practicable for diagnosed cases of amino acid
14		metabolism disorders, including phenylketonuria, organic acid
15		disorders, and fatty acid oxidation disorders for as long as
16		medically indicated, when the product is not available through
17		other State agencies.
18		(d) (Blank). Arrange for or provide public health nursing,
19		nutrition and social services and clinical consultation as
20		indicated.
21		(e) (Blank). Require that all specimens collected pursuant
22		to this Act or the rules and regulations promulgated hereunder
23		be submitted for testing to the nearest Department of Public
24		Health laboratory designated to perform such tests. The
25		Department may develop a reasonable fee structure and may levy
26		fees according to such structure to cover the cost of providing

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1		this testing service. Fees collected from the provision of this
2		testing service shall be placed in a special fund in the State
3		Treasury, hereafter known as the Metabolic Screening and
4		Treatment Fund. Other State and federal funds for expenses
5		related to metabolic screening, follow-up and treatment
6		programs may also be placed in such Fund. Moneys shall be
7		appropriated from such Fund to the Department of Public Health
8		solely for the purposes of providing metabolic screening,
9		follow-up and treatment programs. Nothing in this Act shall be
10		construed to prohibit any licensed medical facility from
11		collecting additional specimens for testing for metabolic or
12		neonatal diseases or any other diseases or conditions, as it
13		deems fit. Any person violating the provisions of this
14		subsection (e) is guilty of a petty offense.
15		(Source: P.A. 97-227, eff. 1-1-12; 97-532, eff. 8-23-11;
16		97-813, eff. 7-13-12.)
17		(410 ILCS 240/3.1 new)
18		Sec. 3.1. Lysosomal storage disorders. In accordance with
19		the timetable specified in this Section, the Department shall
20		provide all newborns with screening tests for the presence of
21		certain lysosomal storage disorders known as Krabbe, Pompe,
22		Gaucher, Fabry, and Niemann-Pick. The testing shall begin
23		within 6 months following the occurrence of all of the
24		following:
25		(1) the establishment and verification of relevant and

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1		appropriate performance specifications as defined under
2		the federal Clinical Laboratory Improvement Amendments and
3		regulations thereunder for Federal Drug
4		Administration-cleared or in-house developed methods,
5		performed under an institutional review board approved
6		protocol, if required;
7		(2) the availability of quality assurance testing
8		methodology for these processes;
9		(3) the acquisition and installment by the Department
10		of the equipment necessary to implement the screening
11		tests;
12		(4) the establishment of precise threshold values
13		ensuring defined disorder identification for each
14		screening test;
15		(5) the authentication of pilot testing achieving each
16		milestone described in items (1) through (4) of this
17		Section for each disorder screening test; and
18		(6) the authentication of achieving the potential of
19		high throughput standards for statewide volume of each
20		disorder screening test concomitant with each milestone
21		described in items (1) through (4) of this Section.
22		It was the goal of Public Act 97-532 that the screening for
23		the specified lysosomal storage disorders begins within 2 years
24		after August 23, 2011 (the effective date of Public Act
25		97-532). The Department is authorized to implement an
26		additional fee for the screening prior to beginning the testing

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1		in order to accumulate the resources for start-up and other
2		costs associated with implementation of the screening and
3		thereafter to support the costs associated with screening and
4		follow-up programs for the specified lysosomal storage
5		disorders.
6		(410 ILCS 240/3.2 new)
7		Sec. 3.2. Severe combined immunodeficiency disease. In
8		accordance with the timetable specified in this Section, the
9		Department shall provide all newborns with screening tests for
10		the presence of severe combined immunodeficiency disease
11		(SCID). The testing shall begin within 12 months following the
12		occurrence of all of the following:
13		(1) the establishment and verification of relevant and
14		appropriate performance specifications as defined under
15		the federal Clinical Laboratory Improvement Amendments and
16		regulations thereunder for Federal Drug
17		Administration-cleared or in-house developed methods,
18		performed under an institutional review board approved
19		protocol, if required;
20		(2) the availability of quality assurance testing and
21		comparative threshold values for SCID;
22		(3) the acquisition and installment by the Department
23		of the equipment necessary to implement the initial pilot
24		and statewide volume of screening tests for SCID;
25		(4) the establishment of precise threshold values

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1		ensuring defined disorder identification for SCID;
2		(5) the authentication of pilot testing achieving each
3		milestone described in items (1) through (4) of this
4		Section for SCID; and
5		(6) the authentication of achieving the potential of
6		high throughput standards for statewide volume of the SCID
7		screening test concomitant with each milestone described
8		in items (1) through (4) of this Section.
9		It was the goal of Public Act 97-532 that the screening for
10		severe combined immunodeficiency disease begins within 2 years
11		after August 23, 2011 (the effective date of Public Act
12		97-532). The Department is authorized to implement an
13		additional fee for the screening prior to beginning the testing
14		in order to accumulate the resources for start-up and other
15		costs associated with implementation of the screening and
16		thereafter to support the costs associated with screening and
17		follow-up programs for severe combined immunodeficiency
18		disease.
19		(410 ILCS 240/3.3 new)
20		Sec. 3.3. Mucopolysacchardosis disorders. In accordance
21		with the timetable specified in this Section, the Department
22		shall provide all newborns with screening tests for the
23		presence of certain lysosomal storage disorders known as
24		mucopolysaccharidosis I (Hurlers) and mucopolysaccharidosis II
25		(Hunters). The testing shall begin within 12 months following

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1		the occurrence of all of the following:
2		(1) the establishment and verification of relevant and
3		appropriate performance specifications as defined under
4		the federal Clinical Laboratory Improvement Amendments and
5		regulations thereunder for Federal Drug
6		Administration-cleared or in-house developed methods,
7		performed under an institutional review board approved
8		protocol, if required;
9		(2) the availability of quality assurance testing and
10		comparative threshold values for each screening test and
11		accompanying disorder;
12		(3) the acquisition and installment by the Department
13		of the equipment necessary to implement the initial pilot
14		and statewide volume of screening tests for each disorder;
15		(4) the establishment of precise threshold values
16		ensuring defined disorder identification for each
17		screening test;
18		(5) the authentication of pilot testing achieving each
19		milestone described in items (1) through (4) of this
20		Section for each disorder screening test; and
21		(6) the authentication of achieving the potential of
22		high throughput standards for statewide volume of each
23		disorder screening test concomitant with each milestone
24		described in items (1) through (4) of this Section.
25		It was the goal of Public Act 97-532 that the screening for
26		the specified lysosomal storage disorders begins within 3 years

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1		after August 23, 2011 (the effective date of Public Act
2		97-532). The Department is authorized to implement an
3		additional fee for the screening prior to beginning the testing
4		in order to accumulate the resources for start-up and other
5		costs associated with implementation of the screening and
6		thereafter to support the costs associated with screening and
7		follow-up programs for the specified lysosomal storage
8		disorders.
9		Section 10. The Genetic and Metabolic Diseases Advisory
10		Committee Act is amended by changing Section 5 as follows:
11		(410 ILCS 265/5)
12		Sec. 5. Genetic and Metabolic Diseases Advisory Committee.
13		(a) The Director of Public Health shall create the Genetic
14		and Metabolic Diseases Advisory Committee to advise the
15		Department of Public Health regarding issues relevant to
16		newborn screenings of metabolic diseases.
17		(b) The purposes of Metabolic Diseases Advisory Committee
18		are all of the following:
19		(1) Advise the Department regarding issues relevant to
20		its Genetics Program.
21		(2) Advise the Department regarding optimal laboratory
22		methodologies for screening of the targeted conditions.
23		(3) Recommend to the Department consultants who are
24		qualified to diagnose a condition detected by screening,

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1		provide management of care, and genetic counseling for the
2		family.
3		(4) Monitor the incidence of each condition for which
4		newborn screening is done, evaluate the effects of
5		treatment and genetic counseling, and provide advice on
6		disorders to be included in newborn screening panel.
7		(5) Advise the Department on educational programs for
8		professionals and the general public.
9		(6) Advise the Department on new developments and areas
10		of interest in relation to the Genetics Program.
11		(7) Any other matter deemed appropriate by the
12		Committee and the Director.
13		(c) The Committee shall consist of 20 members appointed by
14		the Director of Public Health. Membership shall include
15		physicians, geneticists, nurses, nutritionists, and other
16		allied health professionals, as well as patients and parents.
17		Ex-officio members may be appointed, but shall not have voting
18		privileges.
19		(d) Members of the Committee may receive compensation for
20		necessary expenses incurred in the performance of their duties.
21		(Source: P.A. 95-695, eff. 11-5-07.)
22		Section 99. Effective date. This Act takes effect upon
23		becoming law.