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| 1 | | AN ACT concerning health facilities.
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| 2 | | Be it enacted by the People of the State of Illinois,
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| 3 | | represented in the General Assembly:
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| 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:
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| 7 | | (410 ILCS 240/1) (from Ch. 111 1/2, par. 4903)
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| 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
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| 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.
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| 18 | | (Source: P.A. 83-87.)
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| 19 | | (410 ILCS 240/1.5)
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| 20 | | Sec. 1.5. Definitions. In this Act:
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| 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.
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| 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.
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| 10 | | "Tandem mass spectrometer" means an analytical instrument |
| 11 | | used to detect
numerous genetic and metabolic disorders at one |
| 12 | | time.
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| 13 | | (Source: P.A. 92-701, eff. 7-19-02.)
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| 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.
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| 16 | | (410 ILCS 240/2) (from Ch. 111 1/2, par. 4904)
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| 17 | | Sec. 2. General provisions. The Department of Public Health |
| 18 | | shall administer the
provisions of this Act and shall:
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| 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.
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| 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,
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| 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
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| 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
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| 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
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| 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
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| 25 | | appropriate performance specifications as defined under
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| 26 | | the federal Clinical Laboratory Improvement Amendments and
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| 1 | | regulations thereunder for U.S. Food and Drug
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| 2 | | Administration-cleared or in-house developed methods,
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| 3 | | performed under an institutional review board-approved
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| 4 | | protocol, if required; |
| 5 | | (2) the availability of quality assurance testing
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| 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
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| 9 | | of the equipment necessary to implement the screening
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| 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
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| 15 | | milestone described in items (1) through (4) of this
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| 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).
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| 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.
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| 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.
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| 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.
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| 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.
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| 15 | | (Source: P.A. 97-227, eff. 1-1-12; 97-532, eff. 8-23-11; |
| 16 | | 97-813, eff. 7-13-12.)
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| 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.
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| 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.
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| 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
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| 8 | | disorders.
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| 9 | | Section 10. The Genetic and Metabolic Diseases Advisory |
| 10 | | Committee Act is amended by changing Section 5 as follows:
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| 11 | | (410 ILCS 265/5)
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| 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.
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| 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.
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| 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.
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| 7 | | (5) Advise the Department on educational programs for |
| 8 | | professionals and the general public.
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| 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.
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| 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.)
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| 22 | | Section 99. Effective date. This Act takes effect upon |
| 23 | | becoming law. |