Your search keyword '"Ben-Asher, Edna"' showing total 17 results

1. Identification of a Functional Risk Variant for Pemphigus Vulgaris in the ST18 Gene.

Author

Vodo, Dan, Sarig, Ofer, Geller, Shamir, Ben-Asher, Edna, Olender, Tsviya, Bochner, Ron, Goldberg, Ilan, Nosgorodsky, Judith, Alkelai, Anna, Tatarskyy, Pavel, Peled, Alon, Baum, Sharon, Barzilai, Aviv, Ibrahim, Saleh M., Zillikens, Detlef, Lancet, Doron, and Sprecher, Eli

Subjects

PEMPHIGUS treatment, IMMUNOGLOBULINS, PEMPHIGUS, EPITHELIAL cells, IMMUNOSUPPRESSIVE agents, GENETICS

Abstract

Pemphigus vulgaris (PV) is a life-threatening autoimmune mucocutaneous blistering disease caused by disruption of intercellular adhesion due to auto-antibodies directed against epithelial components. Treatment is limited to immunosuppressive agents, which are associated with serious adverse effects. The propensity to develop the disease is in part genetically determined. We therefore reasoned that the delineation of PV genetic basis may point to novel therapeutic strategies. Using a genome-wide association approach, we recently found that genetic variants in the vicinity of the ST18 gene confer a significant risk for the disease. Here, using targeted deep sequencing, we identified a PV-associated variant residing within the ST18 promoter region (p<0.0002; odds ratio = 2.03). This variant was found to drive increased gene transcription in a p53/p63-dependent manner, which may explain the fact that ST18 is up-regulated in the skin of PV patients. We then discovered that when overexpressed, ST18 stimulates PV serum-induced secretion of key inflammatory molecules and contributes to PV serum-induced disruption of keratinocyte cell-cell adhesion, two processes previously implicated in the pathogenesis of PV. Thus, the present findings indicate that ST18 may play a direct role in PV and consequently represents a potential target for the treatment of this disease. [ABSTRACT FROM AUTHOR]

Published

2016

2. General Olfactory Sensitivity Database ( GOSdb): Candidate Genes and their Genomic Variations.

Author

Keydar, Ifat, Ben‐Asher, Edna, Feldmesser, Ester, Nativ, Noam, Oshimoto, Arisa, Restrepo, Diego, Matsunami, Hiroaki, Chien, Ming‐Shan, Pinto, Jayant M., Gilad, Yoav, Olender, Tsviya, and Lancet, Doron

Abstract

ABSTRACT Genetic variations in olfactory receptors likely contribute to the diversity of odorant-specific sensitivity phenotypes. Our working hypothesis is that genetic variations in auxiliary olfactory genes, including those mediating transduction and sensory neuronal development, may constitute the genetic basis for general olfactory sensitivity ( GOS) and congenital general anosmia ( CGA). We thus performed a systematic exploration for auxiliary olfactory genes and their documented variation. This included a literature survey, seeking relevant functional in vitro studies, mouse gene knockouts and human disorders with olfactory phenotypes, as well as data mining in published transcriptome and proteome data for genes expressed in olfactory tissues. In addition, we performed next-generation transcriptome sequencing ( RNA-seq) of human olfactory epithelium and mouse olfactory epithelium and bulb, so as to identify sensory-enriched transcripts. Employing a global score system based on attributes of the 11 data sources utilized, we identified a list of 1,680 candidate auxiliary olfactory genes, of which 450 are shortlisted as having higher probability of a functional role. For the top-scoring 136 genes, we identified genomic variants (probably damaging single nucleotide polymorphisms, indels, and copy number deletions) gleaned from public variation repositories. This database of genes and their variants should assist in rationalizing the great interindividual variation in human overall olfactory sensitivity (http://genome.weizmann.ac.il/GOSdb). [ABSTRACT FROM AUTHOR]

Published

2013

3. DOCK4 and CEACAM21 as novel schizophrenia candidate genes in the Jewish population.

Author

Alkelai, Anna, Lupoli, Sara, Greenbaum, Lior, Kohn, Yoav, Kanyas-Sarner, Kyra, Ben-Asher, Edna, Lancet, Doron, Macciardi, Fabio, and Lerer, Bernard

Abstract

It is well accepted that schizophrenia has a strong genetic component. Several genome-wide association studies (GWASs) of schizophrenia have been published in recent years; most of them population based with a case-control design. Nevertheless, identifying the specific genetic variants which contribute to susceptibility to the disorder remains a challenging task. A family-based GWAS strategy may be helpful in the identification of schizophrenia susceptibility genes since it is protected against population stratification, enables better accounting for genotyping errors and is more sensitive for identification of rare variants which have a very low frequency in the general population. In this project we implemented a family-based GWAS of schizophrenia in a sample of 107 Jewish-Israeli families. We found one genome-wide significant association in the intron of the DOCK4 gene (rs2074127, p value=1.134×10−7) and six additional nominally significant association signals with p<1×10−5. One of the top single nucleotide polymorphisms (p<1×10−5) which is located in the predicted intron of the CEACAM21 gene was significantly replicated in independent family-based sample of Arab-Israeli origin (rs4803480: p value=0.002; combined p value=9.61×10−8), surviving correction for multiple testing. Both DOCK4 and CEACAM21 are biologically reasonable candidate genes for schizophrenia although generalizability of the association of DOCK4 with schizophrenia should be investigated in further studies. In addition, gene-wide significant associations were found within three schizophrenia candidate genes: PGBD1, RELN and PRODH, replicating previously reported associations. By application of a family-based strategy to GWAS, our study revealed new schizophrenia susceptibility loci in the Jewish-Israeli population. [ABSTRACT FROM AUTHOR]

Published

2012

4. Personal receptor repertoires: olfaction as a model.

Author

Olender, Tsviya, Waszak, Sebastian M., Viavant, Maya, Khen, Miriam, Ben-Asher, Edna, Reyes, Alejandro, Nativ, Noam, Wysocki, Charles J., Dongliang Ge, and Lancet, Doron

Subjects

NUCLEOTIDES, GENOMES, OLFACTORY receptors, ALLELES, NEURONS

Abstract

Background: Information on nucleotide diversity along completely sequenced human genomes has increased tremendously over the last few years. This makes it possible to reassess the diversity status of distinct receptor proteins in different human individuals. To this end, we focused on the complete inventory of human olfactory receptor coding regions as a model for personal receptor repertoires. Results: By performing data-mining from public and private sources we scored genetic variations in 413 intact OR loci, for which one or more individuals had an intact open reading frame. Using 1000 Genomes Project haplotypes, we identified a total of 4069 full-length polypeptide variants encoded by these OR loci, average of ~10 per locus, constituting a lower limit for the effective human OR repertoire. Each individual is found to harbor as many as 600 OR allelic variants, ~50% higher than the locus count. Because OR neuronal expression is allelically excluded, this has direct effect on smell perception diversity of the species. We further identified 244 OR segregating pseudogenes (SPGs), loci showing both intact and pseudogene forms in the population, twenty-six of which are annotatively "resurrected" from a pseudogene status in the reference genome. Using a custom SNP microarray we validated 150 SPGs in a cohort of 468 individuals, with every individual genome averaging 36 disrupted sequence variations, 15 in homozygote form. Finally, we generated a multi-source compendium of 63 OR loci harboring deletion Copy Number Variations (CNVs). Our combined data suggest that 271 of the 413 intact OR loci (66%) are affected by nonfunctional SNPs/indels and/or CNVs. Conclusions: These results portray a case of unusually high genetic diversity, and suggest that individual humans have a highly personalized inventory of functional olfactory receptors, a conclusion that might apply to other receptor multigene families. [ABSTRACT FROM AUTHOR]

Published

2012

5. Association of the Type 2 Diabetes Mellitus Susceptibility Gene, TCF7L2, with Schizophrenia in an Arab-Israeli Family Sample.

Author

Alkelai, Anna, Greenbaum, Lior, Lupoli, Sara, Kohn, Yoav, Sarner-Kanyas, Kyra, Ben-Asher, Edna, Lancet, Doron, Macciardi, Fabio, and Lerer, Bernard

Subjects

GENETICS of type 2 diabetes, GENETICS of schizophrenia, ARAB-Israeli conflict, 1993-, ETHNIC groups, GENETIC polymorphisms, ARABS

Abstract

Many reports in different populations have demonstrated linkage of the 10q24-q26 region to schizophrenia, thus encouraging further analysis of this locus for detection of specific schizophrenia genes. Our group previously reported linkage of the 10q24-q26 region to schizophrenia in a unique, homogeneous sample of Arab-Israeli families with multiple schizophrenia-affected individuals, under a dominant model of inheritance. To further explore this candidate region and identify specific susceptibility variants within it, we performed re-analysis of the 10q24-26 genotype data, taken from our previous genome-wide association study (GWAS) (Alkelai et al, 2011). We analyzed 2089 SNPs in an extended sample of 57 Arab Israeli families (189 genotyped individuals), under the dominant model of inheritance, which best fits this locus according to previously performed MOD score analysis. We found significant association with schizophrenia of the TCF7L2 gene intronic SNP, rs12573128, (p = 7.01 × 10-6) and of the nearby intergenic SNP, rs1033772, (p = 6.59 × 10-6) which is positioned between TCF7L2 and HABP2. TCF7L2 is one of the best confirmed susceptibility genes for type 2 diabetes (T2D) among different ethnic groups, has a role in pancreatic beta cell function and may contribute to the comorbidity of schizophrenia and T2D. These preliminary results independently support previous findings regarding a possible role of TCF7L2 in susceptibility to schizophrenia, and strengthen the importance of integrating linkage analysis models of inheritance while performing association analyses in regions of interest. Further validation studies in additional populations are required. [ABSTRACT FROM AUTHOR]

Published

2012

6. Identification of new schizophrenia susceptibility loci in an ethnically homogeneous, family-based, Arab-Israeli sample.

Author

Alkelai, Anna, Lupoli, Sara, Greenbaum, Lior, Giegling, Ina, Kohn, Yoav, Sarner-Kanyas, Kyra, Ben-Asher, Edna, Lancet, Doron, Rujescu, Dan, Macciardi, Fabio, and Lerer, Bernard

Subjects

GENOMES, SAMPLING (Process), GENETICS of schizophrenia, LOCUS (Genetics), CHROMOSOMES, GENETIC polymorphisms, TRANSCRIPTION factors

Abstract

While the use of population-based samples is a common strategy in genome-wide association studies (GWASs), family-based samples have considerable advantages, such as robustness against population stratification and false-positive associations, better quality control, and the possibility to check for both linkage and association. In a genome-wide linkage study of schizophrenia in Arab-Israeli families with multiple affected individuals, we previously reported significant evidence for a susceptibility locus at chromosome 6q23.2-q24.1 and suggestive evidence at chromosomes 10q22.3-26.3, 2q36.1-37.3 and 7p21.1-22.3. To identify schizophrenia susceptibility genes, we applied a family-based GWAS strategy in an enlarged, ethnically homogeneous, Arab-Israeli family sample. We performed genome-wide single nucleotide polymorphism (SNP) genotyping and single SNP transmission disequilibrium test association analysis and found genome-wide significant association (best value of P=1.22x10-11) for 8 SNPs within or near highly reasonable functional candidate genes for schizophrenia. Of particular interest are a group of SNPs within and flanking the transcriptional factor LRRFIP1 gene. To determine replicability of the significant associations beyond the Arab-Israeli population, we studied the association of the significant SNPs in a German case-control validation sample and found replication of associations near die UGT1 subfamily and EFHD1 genes. Applying an exploratory homozygosity mapping approach as a complementary strategy to identify schizophrenia susceptibility genes in our Arab Israeli sample, we identified 8 putative disease loci. Overall, this GWAS, which emphasizes the important contribution of family based studies, identifies promising candidate genes for schizophrenia. [ABSTRACT FROM AUTHOR]

Published

2011

7. Fine mapping of AHI1 as a schizophrenia susceptibility gene: from association to evolutionary evidence.

Author

Torri, Federica, Akelai, Anna, Lupoli, Sara, Sironi, Manuela, Amann-Zalcenstein, Daniela, Fumagalli, Matteo, Dal Fiume, Chiara, Ben-Asher, Edna, Kanyas, Kyra, Cagliani, Rachele, Cozzi, Paolo, Trombetti, Gabriele, Lievers, Luisa Strik, Salvi, Erika, Orro, Alessandro, Beckmann, Jacques S., Lancet, Doron, Kohn, Yoav, Milanesi, Luciano, and Ebstein, Richard B.

Subjects

SCHIZOPHRENIA, GENES, PSYCHIATRY, EPIDEMIOLOGY, META-analysis

Abstract

In previous studies, we identified a locus for schizophrenia on 6q23.3 and proposed the Abelson helper integration site 1 (AHI1) as the candidate gene. AHI1 is expressed in the brain and plays a key role in neurodevelopment, is involved in Joubert syndrome, and has been recently associated with autism. The neurodevelopmental role of AHI1 fits with etiological hypotheses of schizophrenia. To definitively confirm our hypothesis, we searched for associations using a dense map of the region. Our strongest findings lay within the AHI1 gene: single-nucleotide polymorphisms rs11154801 and rs7759971 showed significant associations (P=6.23E-06; P=0.84E-06) and haplotypes gave P values in the 10E-8 to 10E-10 range. The second highest significant region maps close to AHI1 and includes the intergenic region between BC040979 and PDE7B (rs2038549 at P=9.70E-06 and rs1475069 at P=6.97E-06), and PDE7B and MAP7. Using a sample of Palestinian Arab families to confirm these findings, we found isolated signals. While these results did not retain their significance after correction for multiple testing, the joint analysis across the 2 samples supports the role of AHI1, despite the presence of heterogeneity. Given the hypothesis of positive selection of schizophrenia genes, we resequenced a 11 kb region within AHI1 in ethnically defined populations and found evidence for a selective sweep. Network analysis indicates 2 haplotype clades, with schizophrenia-susceptibility haplotypes clustering within the major clade. In conclusion, our data support the role of AHI1 as a susceptibility gene for schizophrenia and confirm it has been subjected to positive selection, also shedding light on new possible candidate genes, MAP7 and PDE7B. [ABSTRACT FROM AUTHOR]

Published

2010

8. Single-nucleotide polymorphisms in the p53 pathway genes modify cancer risk in BRCA1 and BRCA2 carriers of Jewish-Ashkenazi descent.

Author

Yarden, Ronit I., Friedman, Eitan, Metsuyanim, Sally, Olender, Tzvia, Ben-Asher, Edna, and Papa, Moshe Z.

Published

2010

9. MDM2 SNP309 accelerates breast and ovarian carcinogenesis in BRCA1 and BRCA2 carriers of Jewish–Ashkenazi descent.

Author

Yarden, Ronit I., Friedman, Eitan, Metsuyanim, Sally, Olender, Tsviya, Ben-Asher, Edna, and Papa, Moshe Zvi

Abstract

A functional single nucleotide polymorphism in the promoter of the MDM2 gene, SNP309 (T>G), was recently found to accelerate tumorigenesis in early onset cancer cases. The SNP309 G-allele, introduces an SP1 site in the MDM2 promoter, resulting in enhanced MDM2 expression and activity. Thus, the G-allele of MDM2 SNP309 may represent a cancer predisposing allele. In this report, we assessed the role of SNP309 as a modifier of mutant BRCA1/BRCA2 alleles in inherited breast and ovarian cancer cases among Ashkenazi–Jewish (AJ) women. We genotyped several subsets of AJ women: 138 healthy women, 140 affected BRCA1/2 mutation carriers, 120 asymptomatic BRCA1/2 mutation carriers and 187 sporadic breast cancer patients. The frequency of GG genotype of SNP309 was similar among the different groups. Interestingly, we found almost three times higher frequency of the GG genotype among BRCA1/2 carriers diagnosed with breast and/or ovarian cancer at or under the age of 51 years compared with carriers diagnosed with cancer above the age of 51 years (allele frequency, P = 0.019). The GG genotype was significantly associated with breast and ovarian cancer risk among BRCA1/2 carriers diagnosed before 51 years of age (OR, 3.93; 95% CI, 1.41–10.90, P = 0.009). No significant difference in frequency of the GG genotype was observed between early and late onset non-carrier cancer patients and no association with risk, OR, 1.30; 95% CI 0.69–2.47, P = 0.419). These data suggest that MDM2 SNP309 acts as a modifier of mutant BRCA1/2 mutant alleles in AJ and may accelerate breast and ovarian carcinogenesis in genetically predisposed individuals. [ABSTRACT FROM AUTHOR]

Published

2008

10. AHI1, a pivotal neurodevelopmental gene, and C6orf217 are associated with susceptibility to schizophrenia.

Author

Amann-Zalcenstein, Daniela, Avidan, Nili, Kanyas, Kyra, Ebstein, Richard P., Kohn, Yoav, Hamdan, Adnan, Ben-Asher, Edna, Karni, Osnat, Mujaheed, Muhammed, Segman, Ronnen H., Maier, Wolfgang, Macciardi, Fabio, Beckmann, Jacques S., Lancet, Doron, and Lerer, Bernard

Subjects

SCHIZOPHRENIA, NEURODEVELOPMENTAL treatment, GENETIC polymorphisms, GENES, GENE mapping, HUMAN genetics

Abstract

Schizophrenia, a severe neuropsychiatric disorder, is believed to involve multiple genetic factors. A significant body of evidence supports a pivotal role for abnormalities of brain development in the disorder. Linkage signals for schizophrenia map to human chromosome 6q. To obtain a finer localization, we genotyped 180 single nucleotide polymorphisms (SNPs) in a young, inbred Arab-Israeli family sample with a limited number of founders. The SNPs were mostly within a ∼7 Mb region around the strong linkage peak at 136.2 Mb that we had previously mapped. The most significant genetic association with schizophrenia for single SNPs and haplotypes was within a 500 kb genomic region of high linkage disequilibrium (LD) at 135.85 Mb. In a different, outbred, nuclear family sample that was not appropriate for linkage analysis, under-transmitted haplotypes incorporating the same SNPs (but not the individual SNPs) were significantly associated with schizophrenia. The implicated genomic region harbors the Abelson Helper Integration Site 1 (AHI1) gene, which showed the strongest association signal, and an adjacent, primate-specific gene, C6orf217. Mutations in human AHI1 underlie the autosomal recessive Joubert Syndrome with brain malformation and mental retardation. Previous comparative genomic analysis has suggested accelerated evolution of AHI1 in the human lineage. C6orf217 has multiple splice isoforms and is expressed in brain but does not seem to encode a functional protein. The two genes appear in opposite orientations and their regulatory upstream regions overlap, which might affect their expression. Both, AHI1 and C6orf217 appear to be highly relevant candidate genes for schizophrenia.European Journal of Human Genetics (2006) 14, 1111–1119. doi:10.1038/sj.ejhg.5201675; published online 14 June 2006 [ABSTRACT FROM AUTHOR]

Published

2006

11. Genotype phenotype correlations in Israeli colorectal cancer patients.

Author

Starinsky, Sigal, Figer, Arie, Ben-Asher, Edna, Geva, Ravit, Flex, Dov, Fidder, Herma H., Zidan, Jamal, Lancet, Doron, and Friedman, Eitan

Published

2005

12. CATSPER2, a human autosomal nonsyndromic male infertility gene.

Author

Avidan, Nili, Tamary, Hannah, Dgany, Orly, Cattan, Daniel, Pariente, Alexandre, Thulliez, Michel, Borot, Nicolas, Moati, Lucien, Barthelme, Alain, Shalmon, Lea, Krasnov, Tatyana, Ben-Asher, Edna, Olender, Tsvyia, Khen, Miriam, Yaniv, Issac, Zaizov, Rina, Shalev, Hanna, Delaunay, Jean, and Fellous, Marc

Subjects

MALE infertility, MOLECULAR cloning, DEAFNESS, GENETIC mutation, HUMAN fertility

Abstract

In the course of positional cloning of the Congenital Dyserythropoietic Anemia type I (CDAI) [MIM 224120] gene on 15q15.1-15.3, we examined a family of French origin, in which the propositus suffered from asthenoteratozoospermia and nonsyndromic deafness in addition to CDAI. Two of his brothers had a similar phenotype. All three siblings were homozygous carriers of the CDA1 mutation as well as of a distally located ∼70 kb deletion of the proximal copy of a 106 kb tandem repeat on chromosome 15q15. These repeats encode four genes whose distal copies may be considered pseudogenes. Lack of functional stereocilin and CATSPER2 (a voltage-gate cation channel expressed specifically in spermatozoa) may explain the observed deafness and male infertility phenotypes. To the best of our knowledge, the involvement of CATSPER2 in asthenoteratozoospermia is the first description of a human autosomal gene defect associated with nonsyndromic male infertility. [ABSTRACT FROM AUTHOR]

Published

2003

13. USH3A transcripts encode clarin-1, a four-transmembrane-domain protein with a possible role in sensory synapses.

Author

Adato, Avital, Vreugde, Sarah, Joensuu, Tarja, Avidan, Nili, Hamalainen, Riikka, Belenkiy, Olga, Olender, Tsviya, Bonne-Tamir, Batsheva, Ben-Asher, Edna, Espinos, Carmen, Millan, Jose M., Lehesjoki, Anna-Elina, Flannery, John G., Avraham, Karen B., Pietrokovski, Shmuel, Sankila, Eeva-Marja, Beckmann, Jacques S., and Lancet, Doron

Subjects

USHER'S syndrome, SYNAPSES, EXONS (Genetics)

Abstract

Usher syndrome type 3 (USH3) is an autosomal recessive disorder characterised by the association of post-lingual progressive hearing loss, progressive visual loss due to retinitis pigmentosa and variable presence of vestibular dysfunction. Because the previously defined transcripts do not account for all USH3 cases, we performed further analysis and revealed the presence of additional exons embedded in longer human and mouse USH3A transcripts and three novel USH3A mutations. Expression of Ush3a transcripts was Iocalised by whole mount in situ hybridisation to cochlear hair cells and spiral ganglion cells. The full length USH3A transcript encodes clarin-1, a four-transmembrane-domain protein, which defines a novel vertebrate-specific family of three paralogues. Limited sequence homology to stargazin, a cerebellar synapse four-transmembrane-domain protein, suggests a role for clarin-1 in hair cell and photoreceptor cell synapses, as well as a common pathophysiological pathway for different Usher syndromes. [ABSTRACT FROM AUTHOR]

Published

2002

14. Mucolipidosis type IV: Novel MCOLN1 mutations in Jewish and non-Jewish patients and the frequency of the disease in the Ashkenazi Jewish population.

Author

Bargal, Ruth, Avidan, Nili, Olender, Tzvia, Ben Asher, Edna, Zeigler, Marcia, Raas-Rothschild, Annick, Frumkin, Ayala, Ben-Yoseph, Omer, Friedlender, Yechiel, Lancet, Doron, and Bach, Gideon

Published

2001

15. Mechanisms for Evolving Hypervariability: The Case of Conopeptides.

Author

Conticello, Silvestro G., Gilad, Yoav, Avidan, Nili, Ben-Asher, Edna, Levy, Zehava, and Fainzilber, Mike

Abstract

Hypervariability is a prominent feature of large gene families that mediate interactions between organisms, such as venom-derived toxins or immunoglobulins. In order to study mechanisms for evolution of hypervariability, we examined an EST-generated assemblage of 170 distinct conopeptide sequences from the venoms of five species of marine Conus snails. These sequences were assigned to eight gene families, defined by conserved elements in the signal domain and untranslated regions. Order-of-magnitude differences were observed in the expression levels of individual conopeptides, with five to seven transcripts typically comprising over 50% of the sequenced clones in a given species. The conopeptide precursor alignments revealed four striking features peculiar to the mature peptide domain: (1) an accelerated rate of nucleotide substitution, (2) a bias for transversions over transitions in nucleotide substitutions, (3) a position-specific conservation of cysteine codons within the hypervariable region, and (4) a preponderance of nonsynonymous substitutions over synonymous substitutions. We propose that the first three observations argue for a mutator mechanism targeted to mature domains in conopeptide genes, combining a protective activity specific for cysteine codons and a mutagenic polymerase that exhibits transversion bias, such as DNA polymerase V. The high Dn/Ds ratio is consistent with positive or diversifying selection, and further analyses by intraspecific/interspecific gene tree contingency tests weakly support recent diversifying selection in the evolution of conopeptides. Since only the most highly expressed transcripts segregate in gene trees according to the feeding specificity of the species, diversifying selection might be acting primarily on these sequences. The combination of a targeted mutator mechanism to generate high variability with the subsequent action of diversifying selection on highly expressed variants might explain both the hypervariability of conopeptides and the large number of unique sequences per species. [ABSTRACT FROM PUBLISHER]

Published

2001

16. Identification of the gene causing mucolipidosis type IV.

Author

Bargal, Ruth, Avidan, Nili, Ben-Asher, Edna, Olender, Zvia, Zeigler, Marcia, Frumkin, Ayala, Raas-Rothschild, Annick, Glusman, Gustavo, Lancet, Doron, and Bach, Gideon

Subjects

LYSOSOMAL storage diseases, HUMAN gene mapping, GENETICS

Abstract

Mucolipidosis type IV (MLIV) is an autosomal recessive, neurodegenerative, lysosomal storage disorder characterized by psychomotor retardation and ophthalmological abnormalities including corneal opacities, retinal degeneration and strabismus. Most patients reach a maximal developmental level of 12?15 months. The disease was classified as a mucolipidosis following observations by electron microscopy indicating the lysosomal storage of lipids together with water-soluble, granulated substances. Over 80% of the MLIV patients diagnosed are Ashkenazi Jews, including severely affected and mildly affected patients. The gene causing MLIV was previously mapped to human chromosome 19p13.2?13.3 in a region of approximately 1 cM (ref. 7). Haplotype analysis in the MLIV gene region of over 70 MLIV Ashkenazi chromosomes indicated the existence of two founder chromosomes among 95% of the Ashkenazi MLIV families: a major haplotype in 72% and a minor haplotype in 23% of the MLIV chromosomes (ref. 7, and G.B., unpublished data). The remaining 5% are distinct haplotypes found only in single patients. The basic metabolic defect causing the lysosomal storage in MLIV has not yet been identified. Thus, positional cloning was an alternative to identify the MLIV gene. We report here the identification of a new gene in this human chromosomal region in which MLIV-specific mutations were identified. [ABSTRACT FROM AUTHOR]

Published

2000

17. AHI1, a pivotal neurodevelopmental gene, and C6orf217 are associated with susceptibility to schizophrenia.

Author

Amann-Zalcenstein, Daniela, Avidan, Nili, Kanyas, Kyra, Ebstein, Richard P., Kohn, Yoav, Hamdan, Adnan, Ben-Asher, Edna, Karni, Osnat, Mujaheed, Muhammed, Segman, Ronnen H., Maier, Wolfgang, Macciardi, Fabio, Beckmann, Jacques S., Lancet, Doron, and Lerer, Bernard

Subjects

SCHIZOPHRENIA

Abstract

A correction to the article "AHI1, a pivotal neurodevelopmental gene, and C6orf217 are associated with susceptibility to schizophrenia," that was published in the 2006 issue is presented.

Published

2007