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Juvenile hemochromatosis gene (hfe2a), expression products and uses thereof

a technology of juvenile hemochromatosis and gene, applied in the field of juvenile hemochromatosis, can solve the problem of lethal disease, and achieve the effect of high degree of similarity

Inactive Publication Date: 2007-07-19
XENON PHARMACEUTICALS INC
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

[0021]FIG. 6B shows the high degree of similarity b

Problems solved by technology

If untreated, the disease is lethal because of cardiac and other complications.

Method used

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  • Juvenile hemochromatosis gene (hfe2a), expression products and uses thereof
  • Juvenile hemochromatosis gene (hfe2a), expression products and uses thereof
  • Juvenile hemochromatosis gene (hfe2a), expression products and uses thereof

Examples

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example 1

Identification of the Genetic Mutation Responsible for Juvenile Hemochromatosis 2A (HFE2A).

[0232] 3. We have collected ten Greek families including 13 individuals with JHH. Pedigrees of these families are shown in FIGS. 9a-9d. Of these families (JH3-12), five have been reported previously (JH3-7) (Papanikolaou, G. et al. Linkage to chromosome lq in Greek families with juvenile hemochromatosis. Blood Cells Mol. Dis. 27, 744-749 (2001)). Only one family, JH7, is known to be consanguineous. We confirmed that the disease is consistent with linkage to 1 q21 (HFE2A; OMIM 602390) in the new families by using 25 genotype markers, including six new microsatellite markers identified from genomic sequence. While the Build 31 human genome sequence assembly contains gaps and duplications, we were able to estimate the size of the linkage interval, and define the linkage boundaries and gene content based on existing sequence contigs. Homozygosity mapping in JH7 defined the limits of the candidate...

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Abstract

Polynucleotide and polypeptide sequences for HFE2A, as well as mutations associated with juvenile hemochromatosis, and methods of utilizing these for the screening and identification of agents for the treatment of diseases of iron metabolism, including small organic compounds, are disclosed along with methods of treating and / or ameliorating diseases of iron metabolism, especially in human patients are disclosed. Diagnostic compounds, kits and methods using HFE2A are also described.

Description

[0001] 1. This patent application claims priority of U.S. provisional applications Ser. No. 60 / 462,867, filed 15 Apr. 2003, Ser. No. US / 60 / 488,607, filed 18 Jul. 2003, and Ser. No. 60 / 498,458, filed 28 Aug. 2003, the disclosures of which are hereby incorporated by reference in their entirety.FIELD OF THE INVENTION [0002] The present invention relates generally to the field of iron metabolism diseases, especially juvenile hemochromatosis, to a gene associated therewith, and to methods of using this gene, including expression products thereof, for the screening and identification of agents useful in the treatment of diseases of iron metabolism, including methods of such treatment. BACKGROUND OF THE INVENTION [0003] At least 4 iron-overload disorders labeled hemochromatosis have been identified on the basis of clinical, biochemical, and genetic characteristics. Hemochromatosis type 1 is classic hemochromatosis (sometimes designated “HFE”) (see OMIM Number: 235200; Online Mendelian Inhe...

Claims

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Application Information

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IPC IPC(8): A61K48/00A61K38/40C12Q1/68G01N33/567A61K39/395C12N5/08C07K14/47G01N33/50
CPCA61K38/40A61K48/00C07K14/47C12Q1/6883C12Q1/6897Y10T436/143333C12Q2600/158G01N33/5008G01N33/5023G01N33/5091G01N2500/10C12Q2600/156A61P3/00A61P3/10A61P3/12A61P43/00A61P7/06
Inventor SAMUELS, MARKLUDWIG, ERWINMACDONALD, MARCIAFRANCHINI, PATRICKGOLDBERG, YIGALKAMBOJ, RAJENDERPAPANIKOLAOU, GEORGE
Owner XENON PHARMACEUTICALS INC
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