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Salla disease

Salla disease (or Finnish type sialuria) is a syndrome leading to early physical impairment and mental retardation. This is due to a mutation in chromosome 6 (a recessive allele in the gene SLC17A5 the locus of which is 6q14-15). more...

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This gene codes for sialin, a lysosomal membrane protein that transports the charged sugar, N-acetylneuraminic acid (sialic acid), out of lysosomes. The mutation causes sialic acid to build up in the cells.

First described by P Aula et al. in 1979, Salla disease is named after Salla, a municipality in Finnish Lapland. It is one of nearly 40 diseases that make up the Finnish disease heritage. The majority of 100 Salla disease patients in Finland live in Salla or neighboring municipalities; there are maybe 30-40 patients living abroad, majority of them (one source says 27) in Sweden.

Individuals with Salla disease may present with nystagmus in the first months of life as well as hypotonia and cognitive impairment. The most severely impaired children do not ambulate or acquire language, but they do typically learn to walk and speak and have normal life expectancy. The MRI shows arrested or delayed myelination.

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Doctors in Pennsylvania Dutch Country Find New Genetic Links to Half Dozen Diseases in Past Year
From Business Wire, 10/10/05

LANCASTER, Pa. & SANTA CLARA, Calif. -- Microarray-Based SNP Analysis Provides Researchers with Faster, Cheaper and More Definitive Method to Identify and Diagnose Genetic Disorders

In a corner of Pennsylvania Dutch country, doctors at the Clinic for Special Children are using Affymetrix GeneChip(R) microarrays to discover the genetic causes of disease at an unprecedented pace -- more than a half dozen diseases in the past 12 months. In last month's early on-line issue of American Journal of Medical Genetics, the small group of physicians reported their most recent discovery: a mutated gene causing a mysterious developmental disorder in the Mennonite population.

The non-profit, community-supported Clinic -- part of their budget comes from their annual quilt sale -- is staffed by medical director Holmes Morton, MD, pediatrician Kevin Strauss, MD, and geneticist Erik Puffenberger, PhD. Morton and his wife Caroline started the clinic nearly 20 years ago to try to find treatments for a variety of rare genetic diseases that have long afflicted children in Plain sect communities, such as the Amish. In just the past year though, using a new GeneChip microarray technology from Affymetrix (Nasdaq:AFFX), Morton and colleagues have made breakthrough discoveries for genetic causes of at least six different diseases. While these scientists are studying diseases far more common in the Plain sects, their findings have worldwide ramifications, providing the basis for genetic tests of rare diseases in the general population.

The most recent discovery began when the parents of a 4 year-old girl suffering from slow growth and developmental delay informed the Clinic doctors of a cousin with similar symptoms, raising suspicion that the disease was hereditary. While recent estimates place about 25,000 genes in the human genome, the team narrowed their search to just 55 genes on chromosome 6 by using GeneChip Mapping 10K microarrays to scan 10,000 genetic variations from the two affected cousins and each of their parents. The team suspected two of the genes were involved in the disease and found that one of them -- SLC17A5 -- was mutated in the developmentally-delayed patients. The mutation turned out to be the identical one that causes Salla disease in the Finnish population; the Clinic physicians were then able to diagnose Salla disease in 4 additional individuals by testing for the SLC17A5 mutation directly in patients who had similar disease symptoms.

"Our most recent study using GeneChip arrays took less than one month to complete and cost less than $4,000 dollars to make a definitive diagnosis of Salla disease," said Strauss. "That same patient had undergone four years of standard medical exams, totaling nearly $20,000 dollars, but the diagnosis was elusive until we looked at her genome with the 10K microarray."

Affymetrix Microarray Technology

The key to these doctors' genetic discoveries is that they used the 10K microarray to look at the genome more quickly, more affordably, and in far greater detail than ever before. The experiments are not complicated. The scientists process only a handful of DNA samples and use little more than Microsoft(R) Excel for their statistical analyses. However, these physician-scientists work closely with their patients to understand disease symptoms; they then tease out causative mutations using high-density GeneChip microarrays as a powerful lens to view their patients' genomes, uncovering any hidden mutations.

To accelerate their discoveries, Affymetrix has donated a GeneChip system to the Clinic for Special Children; the donation comprises an annual number of GeneChip microarrays, a FS400 Fluidics Station to perform the microarray experiment, a GCS 3000 Scanner to image the microarrays, and all the software required to control the system and analyze array data.

"The goal is to identify the molecular lesions causing disease in our patient population. With this information, we can perform molecular genetic testing and identify affected individuals before they are symptomatic," said Puffenberger. "Currently, the most effective tool for us to map disease genes and identify the disease-causing mutations is the GeneChip mapping array."

Other Recent Findings

1. Cortical Dysplasia and Focal Epilepsy

The Clinic team used the 10K to scan the genome of four Amish patients and mapped the disease mutation to a small part of chromosome 7 containing 83 genes. The scientists sequenced two of those genes in their patients and identified a single base deletion in all four patients. By screening all their seizure patients for this mutation, they were able to diagnose six other children with the same condition (research publication forthcoming).

2. "Pretzel" syndrome

Studying just seven families, each with at least one affected child, the Clinic team discovered a small genetic deletion in a single gene located on chromosome 17 that had been previously missed. They made the discovery by noticing that one of the 10,000 SNPs on the microarray was missing in all seven patients; that missing SNP was part of the DNA deleted in the Pretzel syndrome patients (research publication forthcoming).

Pretzel syndrome is a previously undescribed disorder characterized by skeletal deformity, malformation of the brain (with accompanying seizures), electrolyte imbalances, and variable malformations of the heart and other organs.

3. Down Syndrome, Patau Syndrome and other chromosomal disorders

Using microarrays to genotype 10,000 SNPs from infants seen at the Clinic, the team quickly detected chromosomal copy number disorders like Trisomy 21 (Down syndrome) and Trisomy 13 (Patau syndrome) that are caused by having too many or too few chromosomes. With a basic 10K microarray scan, they found one patient with trisomy 13, confirmed two suspected cases of Down, identified a deletion on chromosome 13 in another patient, and discovered a 23 megabase duplication of chromosome 2 in yet another patient (research publication forthcoming).

Trisomy occurs when a patient has three chromosomes instead of two, and is typically diagnosed by looking for extra chromosomes with a microscope. While SNP genotyping can confirm simple diagnoses of common chromosome duplications, they can also detect duplications or deletions of small parts of chromosomes that cause similar hereditary disease and are more difficult to diagnose than having an extra chromosome.

4. Sudden Infant Death with Dysgenesis of the Testes (SIDDT)

The scientists identified a gene linked to a form of the largely mysterious sudden infant death syndrome (SIDS). While the genetic basis of SIDS has eluded scientists for decades, the group used the Affymetrix 10K array to analyze the DNA of just four infants, along with their family members, and within two weeks had found the mutation. The Clinic research team published these findings in the August 2004 issue of PNAS.

Upcoming studies

The researchers are currently planning to study a group of over 200 children with undiagnosed developmental delays to find the inherited mutations responsible for disease. Using the 10K array, the team will compare SNP genotypes between their patients with unexplained developmental delay. By grouping patients with the most similar clinical features, they hope to identify shared genomic regions, locate potential candidate genes, identify mutations, and ultimately make a genetic diagnosis. Other ongoing studies include combined variable immune deficiency, epilepsy, and cardiomyopathy.

"These Plain sect studies at the Clinic for Special children are a perfect example of how GeneChip microarrays are enabling scientists to explore the human genome and quickly discover the mutations underpinning disease -- it's a glimpse into the future of medicine," said Greg Yap, vice president of DNA Products at Affymetrix. "While 10,000 SNPs work well for studying small familial populations, 100,000 SNP products and 500,000 SNP products are doing the same thing for studies of complex diseases like diabetes and hypertension."

Broader Implications

Scientists elsewhere are discovering the genetics behind common complex diseases, like hypertension and diabetes, taking an approach similar to the Clinic for Special Children doctors, but using microarrays with far more processing power. Instead of 10,000 SNPs, scientists like Josephine Hoh at Yale University are able to hone in on disease associated mutations by using microarrays that genotype hundreds of thousands of SNPs; these microarrays provide enough genetic information to filter out the normal DNA differences between unrelated people that share the same disease. Hoh's recent study, published in the April 2005 issue of Science, scanned 100,000 SNPs from just 146 people to find a mutation associated with age related macular degeneration. Using previous technologies that looked at far fewer SNPs to generate results with the same scientific significance would have required Hoh to study thousands of people.

About The Clinic for Special Children:

The Clinic for Special Children is a non-profit diagnostic and pediatric medical service for children with genetic disorders in Lancaster County, PA. The clinic was established to provide comprehensive medical care and affordable diagnostic and laboratory services for children with chronic, complex health problems due to inherited disorders. The mission of the clinic also includes improving newborn screening and follow-up services, developing more effective diagnostic methods, advancing clinical research, and acting as an educational resource for those who seek to provide care for children who suffer from rare, inherited diseases.

About Affymetrix:

Affymetrix scientists invented the world's first microarray in 1989 and began selling the first commercial microarray in 1994. Since then, Affymetrix GeneChip(R) technology has become the industry standard in molecular biology research. Affymetrix technology is used by the world's top pharmaceutical, diagnostic and biotechnology companies as well as leading academic, government and not-for-profit research institutes. More than 1,200 GeneChip systems have been shipped around the world and more than 3,000 peer-reviewed papers have been published using the technology. Affymetrix' patented photolithographic manufacturing process provides the most information capacity available today on an array, enabling researchers to use a whole-genome approach to analyze the relationship between genetics and health. Headquartered in Santa Clara, Calif., Affymetrix has subsidiaries in Europe and Asia in addition to manufacturing facilities in Sacramento, Calif. and Bedford, Mass. The company has about 900 employees worldwide. For more information about Affymetrix, please visit the company's website at www.Affymetrix.com

All statements in this press release that are not historical are "forward-looking statements" within the meaning of Section 21E of the Securities Exchange Act as amended, including statements regarding Affymetrix' "expectations," "beliefs," "hopes," "intentions," "strategies" or the like. Such statements are subject to risks and uncertainties that could cause actual results to differ materially for Affymetrix from those projected, including, but not limited to risks of the Company's ability to achieve and sustain higher levels of revenue, higher gross margins, reduced operating expenses, uncertainties relating to technological approaches, manufacturing, product development (including uncertainties relating to the use of the genotyping arrays and outcome of research discussed in this press release), personnel retention, uncertainties related to cost and pricing of Affymetrix products, dependence on collaborative partners, uncertainties relating to sole source suppliers, uncertainties relating to FDA and other regulatory approvals, competition, risks relating to intellectual property of others and the uncertainties of patent protection and litigation. These and other risk factors are discussed in Affymetrix' Form 10-K for the year ended December 31, 2004 and other SEC reports, including its Quarterly Reports on Form 10-Q for subsequent quarterly periods. Affymetrix expressly disclaims any obligation or undertaking to release publicly any updates or revisions to any forward-looking statements contained herein to reflect any change in Affymetrix' expectations with regard thereto or any change in events, conditions, or circumstances on which any such statements are based.

NOTE: Affymetrix, the Affymetrix logo, and GeneChip are registered trademarks owned or used by Affymetrix Inc.

COPYRIGHT 2005 Business Wire
COPYRIGHT 2005 Gale Group

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