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| 1 | HOUSE RESOLUTION
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| 2 | WHEREAS, First described in 1826, more than 170 years ago, | ||||||
| 3 | Batten Disease (Neuronal Ceroid Lipofuscinoses), thought to be | ||||||
| 4 | one of the most common neurodegenerative diseases, remains an | ||||||
| 5 | unsolved mystery today, a puzzling disease that assures its | ||||||
| 6 | victims of only one consistent manifestation, early death; and
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| 7 | WHEREAS, An inherited, degenerative, neurological disease, | ||||||
| 8 | Batten Disease may affect persons of any age, but primarily | ||||||
| 9 | affects infants, toddlers, and school age children, beginning | ||||||
| 10 | unexpectedly and leading to a progressive loss of brain | ||||||
| 11 | function that later destroys bodily functions, eventually | ||||||
| 12 | leaving the victim totally helpless; and
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| 13 | WHEREAS, Whether in the case of infantile (Santavnori), | ||||||
| 14 | late infantile (Jansky, Bielschowsky), juvenile (Batten, | ||||||
| 15 | Spielmeyer, Sjogren), or adult type (Kuf, Parry), the early | ||||||
| 16 | symptoms of Batten Disease are confusing ones; it strikes | ||||||
| 17 | without warning, affecting vision, and causing seizures or | ||||||
| 18 | convulsions; and
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| 19 | WHEREAS, Possibly most frustrating of all is the fact that | ||||||
| 20 | Batten Disease is rarely diagnosed immediately, often being | ||||||
| 21 | mistaken for epilepsy or mental retardation, even | ||||||
| 22 | schizophrenia; and once diagnosed, there is no satisfactory | ||||||
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| 1 | treatment and no cure; the clinical course of the disease | ||||||
| 2 | includes a marked decline in cognitive function; personality | ||||||
| 3 | and behavior changes; loss of communication and motor skills; | ||||||
| 4 | poor circulation; decrease in muscle mass; hyperventilation; | ||||||
| 5 | hallucinations, and, finally, deterioration to a vegetative | ||||||
| 6 | state that ends in death; and
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| 7 | WHEREAS, Batten Disease is named after the British | ||||||
| 8 | pediatrician who first described it in 1903; also known as | ||||||
| 9 | Spielmeyer-Vogt-Sjogren-Batten Disease, it is the most common | ||||||
| 10 | form of a group of disorders called Neuronal Ceroid | ||||||
| 11 | Lipofuscinoses (or NCLs); and
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| 12 | WHEREAS, Although Batten Disease is usually regarded as the | ||||||
| 13 | juvenile form of NCL, it has now become the term to encompass | ||||||
| 14 | all forms of NCL; and
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| 15 | WHEREAS, The forms of NCL are classified by age of onset | ||||||
| 16 | and have the same basic cause, progression and outcome but are | ||||||
| 17 | all genetically different; over time, affected children suffer | ||||||
| 18 | mental impairment, worsening seizures, and progressive loss of | ||||||
| 19 | sight and motor skills; eventually, children with Batten | ||||||
| 20 | Disease/NCL become blind, bedridden, and unable to communicate | ||||||
| 21 | and it is presently always fatal; Batten Disease is not | ||||||
| 22 | contagious or, at this time, preventable; and | ||||||
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| 1 | WHEREAS, The first probable instances of this condition | ||||||
| 2 | were reported in 1826 in a Norwegian medical journal by Dr. | ||||||
| 3 | Christian Stengel, who described 4 affected siblings in a small | ||||||
| 4 | mining community in Norway; although no pathological studies | ||||||
| 5 | were performed on these children, the clinical descriptions are | ||||||
| 6 | so succinct that the diagnosis of the Spielmeyer-Sjogren | ||||||
| 7 | (juvenile) type is fully justified; and
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| 8 | WHEREAS, More fundamental observations were reported by F. | ||||||
| 9 | E. Batten in 1903, and by Vogt in 1905, who performed extensive | ||||||
| 10 | clinicopathological studies on several families; | ||||||
| 11 | retrospectively, these papers disclose that the authors | ||||||
| 12 | grouped together different types of the syndrome; and
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| 13 | WHEREAS, Furthermore Batten, at least for some time, | ||||||
| 14 | insisted that the condition that he described was distinctly | ||||||
| 15 | different from Tay-Sachs Disease, the prototype of a neuronal | ||||||
| 16 | lysosomal disorder now identified as GM2-Gangliosidosis type | ||||||
| 17 | A; around the same time, Spielmeyer reported detailed studies | ||||||
| 18 | on three siblings, suffering from the Spielmeyer-Sjogren | ||||||
| 19 | (juvenile) type, which led him to the very firm statement that | ||||||
| 20 | this malady is not related to Tay-Sachs Disease; subsequently, | ||||||
| 21 | however, the pathomorphological studies of Schaffer made these | ||||||
| 22 | authors change their minds to the extent that they reclassified | ||||||
| 23 | their respective observations as variants of Tay-Sachs | ||||||
| 24 | Disease, which caused confusion lasting about 50 years; and
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| 1 | WHEREAS, In 1913-14, M. Bielschowsky delineated the Late | ||||||
| 2 | Infantile form of NCL; however, all forms were still thought to | ||||||
| 3 | belong in the group of "familial amaurotic idiocies", of which, | ||||||
| 4 | Tay-Sachs was the prototype; in 1931, the Swedish psychiatrist | ||||||
| 5 | and geneticist, Torben Sjogren, presented 115 cases with | ||||||
| 6 | extensive clinical and genetic documentation and came to the | ||||||
| 7 | conclusion that the disease which we now call the | ||||||
| 8 | Spielmeyer-Sjogren (juvenile) type is genetically separate | ||||||
| 9 | from Tay Sachs; and
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| 10 | WHEREAS, Departing from the careful morophological | ||||||
| 11 | observations of Spielmeyer, Hurst, and Sjovall and Ericsson, | ||||||
| 12 | Zeman and Alpert made a determined effort to document the | ||||||
| 13 | previously suggested pigmentary nature of the neuronal | ||||||
| 14 | deposits in certain types of storage disorders; | ||||||
| 15 | simultaneously, Terry and Korey and Svennerholm demonstrated a | ||||||
| 16 | specific ultrastructure and biochemistry for Tay Sachs | ||||||
| 17 | Disease, and these developments led to the distinct | ||||||
| 18 | identification and also separation of the NCLs from Tay Sachs | ||||||
| 19 | Disease by Zeman and Donahue; at that time, it was proposed | ||||||
| 20 | that the Late Infantile (Jansky-Bielschowsky), the Juvenile | ||||||
| 21 | (Spielmeyer-Vogt), and the adult form (Kufs) were quite | ||||||
| 22 | different from Tay-Sachs Disease with respect to chemical | ||||||
| 23 | pathology and ultrastructure and also different from other | ||||||
| 24 | forms of sphingolipidoses; and
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| 1 | WHEREAS, Subsequently, it was shown by Santavuori and | ||||||
| 2 | Haltia that an infantile form of NCL exists, which Zeman and | ||||||
| 3 | Dyken had included with the Jansky Bielschowsky type; and
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| 4 | WHEREAS, There are four main types of NCL, including two | ||||||
| 5 | forms that begin earlier in childhood and a very rare form that | ||||||
| 6 | strikes adults; the symptoms are similar but they become | ||||||
| 7 | apparent at different ages and progress at different rates: | ||||||
| 8 | Infantile NCL (Santavuori-Haltia disease): begins between | ||||||
| 9 | about 6 months and 2 years of age and progresses rapidly; | ||||||
| 10 | affected children fail to thrive and have abnormally small | ||||||
| 11 | heads (microcephaly); also typical are short, sharp muscle | ||||||
| 12 | contractions called myoclonic jerks; initial signs of this | ||||||
| 13 | disorder include delayed psychomotor development with | ||||||
| 14 | progressive deterioration, other motor disorders, or | ||||||
| 15 | seizures; the infantile form has the most rapid progression | ||||||
| 16 | and children live into their mid childhood years; | ||||||
| 17 | Late Infantile NCL (Jansky-Bielschowsky disease): begins | ||||||
| 18 | between ages 2 and 4; the typical early signs are loss of | ||||||
| 19 | muscle coordination (ataxia) and seizures along with | ||||||
| 20 | progressive mental deterioration; this form progresses | ||||||
| 21 | rapidly and ends in death between ages 8 and 12; | ||||||
| 22 | Juvenile NCL (Batten Disease): begins between the ages of 5 | ||||||
| 23 | and 8 years of age; the typical early signs are progressive | ||||||
| 24 | vision loss, seizures, ataxia, or clumsiness; this form | ||||||
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| 1 | progresses less rapidly and ends in death in the late teens | ||||||
| 2 | or early 20s, although some may live into their 30s; | ||||||
| 3 | Adult NCL (Kufs Disease or Parry's Disease): generally | ||||||
| 4 | begins before the age of 40, causes milder symptoms that | ||||||
| 5 | progress slowly, and does not cause blindness; although age | ||||||
| 6 | of death is variable among affected individuals, this form | ||||||
| 7 | does shorten life expectancy; and
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| 8 | WHEREAS, Batten Disease/NCL is relatively rare, occurring | ||||||
| 9 | in an estimated 2 to 4 of every 100,000 births in the United | ||||||
| 10 | States; the diseases have been identified worldwide; although | ||||||
| 11 | NCLs are classified as rare diseases, they often strike more | ||||||
| 12 | than one person in families that carry the defective gene; and
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| 13 | WHEREAS, Childhood NCLs are autosomal recessive disorders; | ||||||
| 14 | that is, they occur only when a child inherits two copies of | ||||||
| 15 | the defective gene, one from each parent; when both parents | ||||||
| 16 | carry one defective gene, each of their children faces one in | ||||||
| 17 | four chance of developing NCL; at the same time, each child | ||||||
| 18 | also faces a one in two chance of inheriting just one copy of | ||||||
| 19 | the defective gene; individuals who have only one defective | ||||||
| 20 | gene are known as carriers, meaning they do not develop the | ||||||
| 21 | disease, but they can pass the gene on to their own children; | ||||||
| 22 | and
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| 23 | WHEREAS, Adult NCL may be inherited as an autosomal | ||||||
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| 1 | recessive (Kufs) or, less often, as an autosomal dominant | ||||||
| 2 | (Parrys) disorder; in autosomal dominant inheritance, all | ||||||
| 3 | people who inherit a single copy of the disease gene develop | ||||||
| 4 | the disease; as a result, there are no unaffected carriers of | ||||||
| 5 | the gene; symptoms of Batten Disease/NCLs are linked to a | ||||||
| 6 | buildup of substances called lipopigments in the body's | ||||||
| 7 | tissues; these lipopigments are made up of fats and proteins; | ||||||
| 8 | their name comes from the technical word lipo, which is short | ||||||
| 9 | for "lipid" or fat, and from the term pigment, used because | ||||||
| 10 | they take on a greenish-yellow color when viewed under an | ||||||
| 11 | ultraviolet light microscope; and
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| 12 | WHEREAS, The lipopigments build up in cells of the brain | ||||||
| 13 | and the eye as well as in skin, muscle, and many other tissues; | ||||||
| 14 | inside the cells, these pigments form deposits with distinctive | ||||||
| 15 | shapes that can be seen under an electron microscope; some look | ||||||
| 16 | like half-moons (or comas) and are called curvilinear bodies, | ||||||
| 17 | others look like fingerprints and are called fingerprint | ||||||
| 18 | inclusion bodies, and still others resemble gravel (or sand) | ||||||
| 19 | and are called granual osmophilic deposits (grods); these | ||||||
| 20 | deposits are what doctors look for when they examine a skin | ||||||
| 21 | sample to diagnose Batten Disease; the diseases cause death of | ||||||
| 22 | neurons (specific cells found in the brain, retina and central | ||||||
| 23 | nervous system); the reason for neuron death is still not | ||||||
| 24 | known; and
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| 1 | WHEREAS, Because vision loss is often an early sign, Batten | ||||||
| 2 | Disease/NCL may be first suspected during an eye exam; an eye | ||||||
| 3 | doctor can detect a loss of cells within the eye that occurs in | ||||||
| 4 | the three childhood forms of Batten Disease/NCL; however, | ||||||
| 5 | because such cell loss occurs in other eye diseases, the | ||||||
| 6 | disorder cannot be diagnosed by this sign alone; and
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| 7 | WHEREAS, Often an eye specialist or other physician who | ||||||
| 8 | suspects Batten Disease/NCL may refer the child to a | ||||||
| 9 | neurologist, a doctor who specializes in disease of the brain | ||||||
| 10 | and nervous system; in order to diagnose Batten Disease/NCL, | ||||||
| 11 | the neurologist needs the patient's medical history and | ||||||
| 12 | information from various laboratory tests; diagnostic tests | ||||||
| 13 | used for Batten Disease/NCLs include: | ||||||
| 14 | Skin or tissue sampling; the doctor can examine a small | ||||||
| 15 | piece of tissue under an electron microscope; the powerful | ||||||
| 16 | magnification of the microscope helps the doctor spot | ||||||
| 17 | typical NCL deposits; these deposits are found in many | ||||||
| 18 | different tissues, including skin, muscle, conjunctiva, | ||||||
| 19 | rectal, and others; blood can also be used; | ||||||
| 20 | electroencephalogram or EEG; an EEG uses special patches | ||||||
| 21 | placed on the scalp to record electrical currents inside | ||||||
| 22 | the brain; this helps doctors see telltale patterns in the | ||||||
| 23 | brain's electrical activity that suggest a patient has | ||||||
| 24 | seizures; | ||||||
| 25 | Electrical studies of the eyes; these tests, which include | ||||||
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| 1 | visual-evoked responses (VER) and electro-retinagrams | ||||||
| 2 | (ERG), can detect various eye problems common in childhood | ||||||
| 3 | Batten Disease/NCLs; | ||||||
| 4 | Brain scans; imaging can help doctors look for changes in | ||||||
| 5 | the brain's appearance; the most commonly used imaging | ||||||
| 6 | technique is computed tomography (CT), which uses x-rays | ||||||
| 7 | and a computer to create a sophisticated picture of the | ||||||
| 8 | brain's tissues and structures; a CT scan may reveal brain | ||||||
| 9 | areas that are decaying in NCL patients; a second imaging | ||||||
| 10 | technique that is increasingly common is magnetic | ||||||
| 11 | resonance imaging, or MRI; MRI uses a combination of | ||||||
| 12 | magnetic fields and radio waves, instead of radiation, to | ||||||
| 13 | create a picture of the brain; | ||||||
| 14 | Enzyme assay; a recent development in diagnosis of Batten | ||||||
| 15 | Disease/NCL is the use of enzyme assays that look for | ||||||
| 16 | specific missing lysosomal enzymes for Infantile and Late | ||||||
| 17 | Infantile only; this is a quick and easy diagnostic test; | ||||||
| 18 | Genetic/DNA testing; each form of Batten disease is the | ||||||
| 19 | result of a different gene; genes for eight or the ten | ||||||
| 20 | forms have been identified; testing for these is available | ||||||
| 21 | for diagnosis as well as carrier and prenatal; and
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| 22 | WHEREAS, As yet, no specific treatment is known that can | ||||||
| 23 | halt or reverse the symptoms of Batten Disease/NCL; however, | ||||||
| 24 | seizures can be reduced or controlled with anticonvulsant | ||||||
| 25 | drugs, and other medical problems can be treated appropriately | ||||||
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| 1 | as they arise; at the same time, physical and occupational | ||||||
| 2 | therapy may help patients retain function as long as possible; | ||||||
| 3 | and
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| 4 | WHEREAS, Some reports have described a slowing of the | ||||||
| 5 | disease in children with Batten Disease who were treated with | ||||||
| 6 | vitamins C and E and with diets low in vitamin A; however, | ||||||
| 7 | these treatments did not prevent the fatal outcome of the | ||||||
| 8 | disease; and
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| 9 | WHEREAS, Support and encouragement can help children and | ||||||
| 10 | families cope with the profound disability and losses caused by | ||||||
| 11 | NCLs; the Batten Disease Support and Research Association | ||||||
| 12 | enables affected children, adults, and families to share common | ||||||
| 13 | concerns and experiences; meanwhile, scientists pursue medical | ||||||
| 14 | research that will someday yield an effective treatment; and
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| 15 | WHEREAS, Within the federal government, the focal point for | ||||||
| 16 | research on Batten Disease and other neurogenetic disorders is | ||||||
| 17 | the National Institute of Neurological Disorders and Stroke | ||||||
| 18 | (NINDS); the NINDS, a part of the National Institutes of Health | ||||||
| 19 | (NIH), is responsible for supporting and conducting research on | ||||||
| 20 | the brain and central nervous system; the Batten Disease | ||||||
| 21 | Support and Research Association and the Children's Brain | ||||||
| 22 | Diseases Foundation also provide financial assistance for | ||||||
| 23 | research; and
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| 1 | WHEREAS, Through the work of several scientific teams, the | ||||||
| 2 | search for the genetic cause of NCLs is gathering speed; in | ||||||
| 3 | September 1995, The International Batten Disease Consortium | ||||||
| 4 | announced the identification of the gene for the juvenile form | ||||||
| 5 | of Batten Disease; the specific gene, CLN3, located on | ||||||
| 6 | Chromosome 16, has a deletion or piece missing; this gene | ||||||
| 7 | accounts for 73% of all cases of Juvenile Batten Disease; the | ||||||
| 8 | rest are the result of other defects of the same gene; and
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| 9 | WHEREAS, Also, in 1995, scientists in Finland announced the | ||||||
| 10 | identification of the gene responsible for the infantile form | ||||||
| 11 | of Batten Disease; the gene, CLN1, is located on Chromosome 1; | ||||||
| 12 | in September 1997, scientists at the Robert Woos Johnson | ||||||
| 13 | Medical School and the Institute for Basic Research, New York, | ||||||
| 14 | announced the identification of the gene for the "classic" Late | ||||||
| 15 | Infantile form of Batten Disease/NCL; the gene, CLN2, is | ||||||
| 16 | located on chromosome 11; and
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| 17 | WHEREAS, Scientists have also identified the genes | ||||||
| 18 | responsible for Finnish Late Infantile (CLN5), variant Late | ||||||
| 19 | Infantile (CLN6), EPMR (CLN8), and Congenital/CTSD (CLN10); | ||||||
| 20 | research also continues toward identification of the gene for | ||||||
| 21 | the adult form of Batten Disease/NCL, also known as Kufs | ||||||
| 22 | Disease; and
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| 1 | WHEREAS, Identification of the specific genes for | ||||||
| 2 | Infantile, Late Infantile, Variant Late Infantile, and | ||||||
| 3 | Juvenile Batten Disease/NCL has led to the development of DNA | ||||||
| 4 | diagnostics, carrier, and prenatal tests; and
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| 5 | WHEREAS, Scientists have discovered that the Infantile and | ||||||
| 6 | Late Infantile diseases are missing key lysosomal enzymes, i.e. | ||||||
| 7 | Palmitoyl Protein Thioesterase 1 (PPT1) for Infantile and | ||||||
| 8 | Tripeptidyl Peptidase 1 (TPP1) for Late Infantile; knowing that | ||||||
| 9 | these enzymes are missing is now leading to the development of | ||||||
| 10 | gene replacement and stem cell transplantation therapies; and
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| 11 | WHEREAS, Recent studies have shown a link between the | ||||||
| 12 | Juvenile form and the body's autoimmune system; although this | ||||||
| 13 | link is not yet fully understood, it may eventually lead to a | ||||||
| 14 | treatment; therefore, be it
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| 15 | RESOLVED, BY THE HOUSE OF REPRESENTATIVES OF THE | ||||||
| 16 | NINETY-SIXTH GENERAL ASSEMBLY OF THE STATE OF ILLINOIS, that we | ||||||
| 17 | declare June 6-7, 2009 Batten Disease Awareness Weekend in the | ||||||
| 18 | State of Illinois and ask people of the State to look at ways | ||||||
| 19 | in which they may help to combat this terrible disease; and be | ||||||
| 20 | it further
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| 21 | RESOLVED, That a suitable copy of this resolution be | ||||||
| 22 | presented to the Batten Disease Research and Support | ||||||
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| 1 | Association as a symbol of our support.
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