Rep. Robyn Gabel
Filed: 3/19/2013
 
 

 

 

 
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1
AMENDMENT TO HOUSE BILL 2661




2    AMENDMENT NO. ______. Amend House Bill 2661 by replacing 
3everything after the enacting clause with the following:

 
4    "Section 5. The Newborn Metabolic Screening Act is amended  
5by changing Sections 1, 1.5, and 2 and by adding Sections 1.10, 
63.1, 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 
9promulgate and
enforce rules and regulations requiring that 
10every newborn be subjected
to tests for genetic, 
11phenylketonuria, hypothyroidism, galactosemia and such
other 
12metabolic, and congenital anomalies diseases as the
Department 
13may deem necessary from time to time. The Department is

14empowered to promulgate such additional rules and regulations 
15as are
found necessary for the administration of this Act, 
16including mandatory
reporting of the results of all tests for 
 
 
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1these conditions to the
Illinois Department of Public Health.

2(Source: P.A. 83-87.)

 



3    (410 ILCS 240/1.5)



4    Sec. 1.5. Definitions. In this Act:

5    "Accredited laboratory" means any laboratory that holds a 
6valid
certificate issued under the Clinical Laboratory 
7Improvement
Amendments of 1988, 102 Stat. 2903, 42 U.S.C. 263a, 
8as amended,
and that reports its screening results by using 
9normal pediatric reference
ranges.

10    "Department" means the Department of Public Health. 
11    "Expanded screening" means screening for genetic and 
12metabolic disorders,
including but not limited to amino acid 
13disorders, organic acid disorders,
fatty acid oxidation 
14disorders, and other abnormal profiles,
in newborn infants that 
15can be detected through the use of a tandem
mass
spectrometer.

16    "Tandem mass spectrometer" means an analytical instrument 
17used to detect
numerous genetic and metabolic disorders at one 
18time.

19(Source: P.A. 92-701, eff. 7-19-02.)

 
20    (410 ILCS 240/1.10 new)
21    Sec. 1.10. Critical congenital heart disease.
22    (a) The General Assembly finds as follows: 
23        (1) According to the United States Secretary of Health 
24    and Human Services Advisory Committee on Heritable 
 
 
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1    Disorders in Newborns and Children, congenital heart 
2    disease affects approximately 7 to 9 of every 1,000 live 
3    births in the United States and Europe.  The federal Centers 
4    for Disease Control and Prevention state that critical 
5    congenital heart disease is the leading cause of infant 
6    death due to birth defects.
7        (2) Many newborn lives could potentially be saved by 
8    earlier detection and treatment of critical congenital 
9    heart disease if health care facilities in the State were 
10    required to perform a simple, non-invasive newborn 
11    screening in conjunction with current screening methods. 
12    (b) The Department may authorize screening tests for 
13congenital anomalies, including, but not limited to, a 
14screening for critical congenital heart defects, to be 
15performed at a health care facility that provides newborn 
16infant care and that complies with the test procedures and the 
17standards of accuracy and precision required by the Department.
18    (c) The Department may authorize health care facilities to 
19report screening test results and follow-up information. 
 



20    (410 ILCS 240/2)  (from Ch. 111 1/2, par. 4904)



21    Sec. 2. General provisions. The Department of Public Health 
22shall administer the
provisions of this Act and shall:

23    (a) Institute and carry on an intensive educational program 
24among
physicians, hospitals, public health nurses and the 
25public concerning disorders included in newborn screening
the 
 
 
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1diseases phenylketonuria, hypothyroidism, galactosemia and 
2other
metabolic diseases. This
educational program shall 
3include information about the nature of the
diseases and 
4examinations for the detection of the diseases in early
infancy 
5in order that measures may be taken to prevent the intellectual 
6disabilities resulting from the diseases.

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

8    hypothyroidism, congenital adrenal hyperplasia, 
9    biotinidase deficiency,
and sickling disorders, as well as 
10    other amino acid disorders, organic
acid disorders, fatty 
11    acid oxidation disorders, and other abnormalities

12    detectable through the use of a tandem mass spectrometer.
13        (3) If by July 1,
2002, the Department is unable to 
14    provide the expanded screening using the
State Laboratory, 
15    it shall temporarily provide such screening
through an 
16    accredited laboratory selected by the Department until the

17    Department has the capacity to provide screening through 
18    the State
Laboratory. If expanded screening is provided on 
19    a temporary basis
through an accredited laboratory, the 
20    Department shall substitute the fee
charged by the 
21    accredited laboratory, plus a 5% surcharge for

22    documentation and handling, for the fee authorized in this 
23    subsection (a-5.1) (e) of
this Section.
24    (a-5.2) Maintain a registry of cases, including 
25information of importance for the purpose of follow-up services 
26to assess long-term outcomes. 
 
 
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1    (a-5.3) Supply the necessary metabolic treatment formulas 
2where practicable for diagnosed cases of amino acid metabolism 
3disorders, including phenylketonuria, organic acid disorders, 
4and fatty acid oxidation disorders for as long as medically 
5indicated, when the product is not available through other 
6State agencies.
7    (a-5.4) Arrange for or provide public health nursing, 
8nutrition, and social services and clinical consultation as 
9indicated.
10    (a-5.5) The Director shall appoint a Genetic and Metabolic 
11Diseases Advisory Committee to provide guidance and 
12recommendations to the Department's newborn screening program.  
13The Genetic and Metabolic Diseases Advisory Committee shall 
14review the feasibility of including additional metabolic, 
15genetic, and congenital disorders in the newborn screening 
16panel.  The Genetic and Metabolic Diseases Advisory Committee 
17shall be comprised of health and medical experts and consumer 
18representatives.  The Department shall consider the 
19recommendations of the Genetic and Metabolic Diseases Advisory 
20Committee in determining whether to include an additional 
21disorder in the screening panel prior to adopting 
22administrative rules.  Members of the Genetic and Metabolic 
23Diseases Advisory Committee may receive compensation for 
24necessary expenses incurred in the performance of their duties. 

25    (a-6) (Blank). In accordance with the timetable specified 
26in this subsection, provide all newborns with expanded 
 
 
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1screening tests for the presence of certain Lysosomal Storage 
2Disorders known as Krabbe, Pompe, Gaucher, Fabry, and 
3Niemann-Pick. The testing shall begin within 6 months following 
4the occurrence of all of the following:
5        (i) the establishment and verification of relevant and 
6    appropriate performance specifications as defined under 
7    the federal Clinical Laboratory Improvement Amendments and 
8    regulations thereunder for Federal Drug 
9    Administration-cleared or in-house developed methods, 
10    performed under an institutional review board approved 
11    protocol, if required;
12        (ii) the availability of quality assurance testing 
13    methodology for these processes;
14        (iii) the acquisition and installment by the 
15    Department of the equipment necessary to implement the 
16    expanded screening tests;
17        (iv) establishment of precise threshold values 
18    ensuring defined disorder identification for each 
19    screening test;
20        (v) authentication of pilot testing achieving each 
21    milestone described in items (i) through (iv) of this 
22    subsection (a-6) for each disorder screening test; and
23        (vi)
authentication achieving potentiality of high 
24    throughput standards for statewide volume of each disorder 
25    screening test concomitant with each milestone described 
26    in items (i) through (iv) of this subsection (a-6). 
 
 
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1    It is the goal of Public Act 97-532 that the expanded 
2screening for the specified Lysosomal Storage Disorders begins 
3within 2 years after August 23, 2011 (the effective date of 
4Public Act 97-532). The Department is authorized to implement 
5an additional fee for the screening prior to beginning the 
6testing in order to accumulate the resources for start-up and 
7other costs associated with implementation of the screening and 
8thereafter to support the costs associated with screening and 
9follow-up programs for the specified Lysosomal Storage 
10Disorders.

11    (a-7) (Blank).  In accordance with the timetable specified 
12in this
subsection (a-7), provide all newborns with expanded 
13screening tests
for the presence of Severe Combined 
14Immunodeficiency Disease (SCID). The testing shall begin 
15within 12 months following the occurrence of all of the 
16following:
17        (i) the establishment and verification of relevant and 
18    appropriate performance specifications as defined under 
19    the federal Clinical Laboratory Improvement Amendments and 
20    regulations thereunder for Federal Drug 
21    Administration-cleared or in-house developed methods, 
22    performed under an institutional review board approved 
23    protocol, if required;
24        (ii) the availability of quality assurance testing and 
25    comparative threshold values for SCID;
26        (iii) the acquisition and installment by the 
 
 
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1    Department of the equipment necessary to implement the 
2    initial pilot and expanded statewide volume of  screening 
3    tests for SCID;
4        (iv) establishment of precise threshold values 
5    ensuring defined disorder identification for SCID;
6        (v) authentication of pilot testing achieving each 
7    milestone described in items (i) through (iv) of this 
8    subsection (a-7) for SCID; and
9        (vi) authentication achieving potentiality of high 
10    throughput standards for statewide volume of the SCID 
11    screening test concomitant with each milestone described 
12    in items (i) through (iv) of this subsection (a-7).
13    It is the goal of Public Act 97-532 that the expanded 
14screening for Severe Combined Immunodeficiency Disease begins 
15within 2 years after August 23, 2011 (the effective date of 
16Public Act 97-532). The Department is authorized to
implement 
17an additional fee for the screening prior to
beginning the 
18testing in order to accumulate the resources for
start-up and 
19other costs associated with implementation of the
screening and 
20thereafter to support the costs associated with
screening and 
21follow-up programs for Severe Combined Immunodeficiency 
22Disease.
23    (a-8) (Blank). In accordance with the timetable specified 
24in this subsection (a-8), provide all newborns with expanded 
25screening tests
for the presence of certain Lysosomal Storage 
26Disorders known as Mucopolysaccharidosis I (Hurlers) and 
 
 
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1Mucopolysaccharidosis II (Hunters).  The testing shall begin 
2within 12 months following the occurrence of all of the 
3following:
4        (i) the establishment and verification of relevant and 
5    appropriate performance specifications as defined under 
6    the federal Clinical Laboratory Improvement Amendments and 
7    regulations thereunder for Federal Drug 
8    Administration-cleared or in-house developed methods, 
9    performed under an institutional review board approved 
10    protocol, if required;
11        (ii) the availability of quality assurance testing and 
12    comparative threshold values for each screening test and 
13    accompanying disorder;
14        (iii) the acquisition and installment by the 
15    Department of the equipment necessary to implement the 
16    initial pilot and expanded statewide volume of  screening 
17    tests for each disorder;
18        (iv) establishment of precise threshold values 
19    ensuring defined disorder identification for each 
20    screening test;
21        (v) authentication of pilot testing achieving each 
22    milestone described in items (i) through (iv) of this 
23    subsection (a-8) for each disorder screening test; and
24        (vi) authentication achieving potentiality of high 
25    throughput standards for statewide volume of each disorder 
26    screening test concomitant with each milestone described 
 
 
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1    in items (i) through (iv) of this subsection (a-8).
2    It is the goal of Public Act 97-532 that the expanded 
3screening for the specified
Lysosomal Storage Disorders begins 
4within 3 years after August 23, 2011 (the effective date of 
5Public Act 97-532). The Department is authorized to
implement 
6an additional fee for the screening prior to beginning the 
7testing in order to accumulate the resources for
start-up and 
8other costs associated with implementation of the screening and 
9thereafter to support the costs associated with
screening and 
10follow-up programs for the specified Lysosomal Storage 
11Disorders. 
12    (b) (Blank). Maintain a registry of cases including 
13information of importance
for the purpose of follow-up services 
14to prevent intellectual disabilities.

15    (c) (Blank). Supply the necessary metabolic treatment 
16formulas
 where practicable for
diagnosed cases of amino acid 
17metabolism disorders, including phenylketonuria, organic acid 
18disorders, and fatty acid oxidation disorders for as long as 
19medically indicated, when the product is
not available through 
20other State agencies.

21    (d) (Blank). Arrange for or provide public health nursing, 
22nutrition and
social services and clinical consultation as 
23indicated.

24    (e) (Blank). Require that all specimens collected pursuant 
25to this Act or the rules
and regulations promulgated hereunder 
26be submitted for testing to the nearest
Department of Public 
 
 
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1Health laboratory designated to perform such tests.
The 
2Department may develop a reasonable fee structure and may levy 
3fees
according to such structure to cover the cost of providing 
4this testing
service.  Fees collected from the provision of this 
5testing service shall
be placed in a special fund in the State 
6Treasury, hereafter known as the
Metabolic Screening and 
7Treatment Fund.  Other State and federal funds for
expenses 
8related to metabolic screening, follow-up and treatment 
9programs
may also be placed in such Fund.  Moneys shall be 
10appropriated from such
Fund to the Department of Public Health 
11solely for the purposes of providing
metabolic screening, 
12follow-up and treatment programs.  Nothing in this
Act shall be 
13construed to prohibit any licensed medical facility from

14collecting
additional specimens for testing for metabolic or 
15neonatal diseases or any
other diseases or conditions, as it 
16deems fit. Any person
violating the provisions of this 
17subsection (e) is guilty of a petty offense.

18(Source: P.A. 97-227, eff. 1-1-12; 97-532, eff. 8-23-11; 
1997-813, eff. 7-13-12.)

 
20    (410 ILCS 240/3.1 new)
21    Sec. 3.1. Lysosomal storage disorders. In accordance with 
22the timetable specified in this Section, the Department shall 
23provide all newborns with screening tests for the presence of 
24certain lysosomal storage disorders known as Krabbe, Pompe, 
25Gaucher, Fabry, and Niemann-Pick. The testing shall begin 
 
 
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1within 6 months following the occurrence of all of the 
2following:
3        (1) the establishment and verification of relevant
and 
4    appropriate performance specifications as defined under 
5    the federal Clinical Laboratory Improvement Amendments and 
6    regulations thereunder for Federal Drug 
7    Administration-cleared or in-house developed methods, 
8    performed under an institutional review board approved 
9    protocol, if required;
10        (2) the availability of quality assurance testing 
11    methodology for these processes;
12        (3) the acquisition and installment by the Department 
13    of the equipment necessary to implement the screening 
14    tests;
15        (4) establishment of precise threshold values ensuring 
16    defined disorder identification for each screening test;
17        (5) authentication of pilot testing achieving each 
18    milestone described in items (1) through (4) of this 
19    Section  for each disorder screening test; and
20        (6) 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 (1) through (4) of this Section. 
24    It is the goal of Public Act 97-532 that the screening for 
25the specified lysosomal storage disorders begins within 2 years 
26after August 23, 2011 (the effective date of Public Act 
 
 
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197-532). The Department is authorized to implement an 
2additional fee for the screening prior to beginning the testing 
3in order to accumulate the resources for start-up and other 
4costs associated with implementation of the screening and 
5thereafter to support the costs associated with screening and 
6follow-up programs for the specified lysosomal storage 
7disorders. 
 
8    (410 ILCS 240/3.2 new)
9    Sec. 3.2. Severe combined immunodeficiency disease. In 
10accordance with the timetable specified in this Section, the 
11Department shall provide all newborns with screening tests for 
12the presence of severe combined immunodeficiency
disease 
13(SCID). The testing shall begin within 12 months following the 
14occurrence of all of the following:
15        (1) the establishment and verification of relevant and

16    appropriate performance specifications as defined under

17    the federal Clinical Laboratory Improvement Amendments and

18    regulations thereunder for Federal Drug

19    Administration-cleared or in-house developed methods,

20    performed under an institutional review board approved

21    protocol, if required;
22        (2) the availability of quality assurance testing and

23    comparative threshold values for SCID;
24        (3) the acquisition and installment by the
Department 
25    of the equipment necessary to implement the
initial pilot 
 
 
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1    and statewide volume of screening
tests for SCID;
2        (4) establishment of precise threshold values
ensuring 
3    defined disorder identification for SCID;
4        (5) authentication of pilot testing achieving each

5    milestone described in items (1) through (4) of this

6    Section for SCID; and
7        (6) authentication achieving potentiality of high

8    throughput standards for statewide volume of the SCID

9    screening test concomitant with each milestone described

10    in items (1) through (4) of this Section. 
11    It is the goal of Public Act 97-532 that the screening for 
12severe combined immunodeficiency disease begins within 2 years 
13after August 23, 2011 (the effective date of Public Act 
1497-532). The Department is authorized to implement an 
15additional fee for the screening prior to beginning the testing 
16in order to accumulate the resources for start-up and other 
17costs associated with implementation of the screening and 
18thereafter to support the costs associated with screening and 
19follow-up programs for severe combined immunodeficiency 
20disease. 
 
21    (410 ILCS 240/3.3 new)
22    Sec. 3.3. Mucopolysacchardosis disorders. In accordance 
23with the timetable specified in this Section, the Department 
24shall provide all newborns with screening tests for the 
25presence of certain lysosomal storage disorders
known as 
 
 
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1mucopolysaccharidosis I (Hurlers) and mucopolysaccharidosis II 
2(Hunters). The testing shall begin within 12 months following 
3the occurrence of all of the following:
4        (1) the establishment and verification of relevant and

5    appropriate performance specifications as defined under

6    the federal Clinical Laboratory Improvement Amendments and

7    regulations thereunder for Federal Drug 
8    Administration-cleared or in-house developed methods, 
9    performed under an institutional review board approved 
10    protocol, if required;
11        (2) the availability of quality assurance testing and 
12    comparative threshold values for each screening test and 
13    accompanying disorder;
14        (3) the acquisition and installment by the Department 
15    of the equipment necessary to implement the initial pilot 
16    and statewide volume of screening tests for each disorder;
17        (4) establishment of precise threshold values ensuring 
18    defined disorder identification for each screening test;
19        (5) authentication of pilot testing achieving each 
20    milestone described in items (1) through (4) of this 
21    Section for each disorder screening test; and
22        (6) authentication achieving potentiality of high 
23    throughput standards for statewide volume of each disorder 
24    screening test concomitant with each milestone described 
25    in items (1) through (4) of this Section. 
26    It is the goal of Public Act 97-532 that the screening for 
 
 
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1the specified lysosomal storage disorders begins within 3 years 
2after August 23, 2011 (the effective date of Public Act 
397-532). The Department is authorized to implement an 
4additional fee for the screening prior to beginning the testing 
5in order to accumulate the resources for start-up and other 
6costs associated with implementation of the screening and 
7thereafter to support the costs associated with screening and 
8follow-up programs for the specified lysosomal storage

9disorders.

 
10    Section 99. Effective date. This Act takes effect upon 
11becoming law.".