{"search_session":{},"preferences":{"l":"en","queryLanguage":"en"},"patentId":"US_2011_0035815_A1","frontPageModel":{"patentViewModel":{"ref":{"entityRefType":"PATENT","entityRefId":"102-916-007-423-080"},"entityMetadata":{"linkedIds":{"empty":true},"tags":[],"collections":[{"id":11699,"type":"PATENT","title":"Oregon State University - Patent Portfolio","description":"","access":"OPEN_ACCESS","displayAvatar":true,"attested":false,"itemCount":2728,"tags":[],"user":{"id":91044780,"username":"Cambialens","firstName":"","lastName":"","created":"2015-05-04T00:55:26.000Z","displayName":"Cambialens","preferences":"{\"usage\":\"public\",\"beta\":false}","accountType":"PERSONAL","isOauthOnly":false},"notes":[{"id":8353,"type":"COLLECTION","user":{"id":91044780,"username":"Cambialens","firstName":"","lastName":"","created":"2015-05-04T00:55:26.000Z","displayName":"Cambialens","preferences":"{\"usage\":\"public\",\"beta\":false}","accountType":"PERSONAL","isOauthOnly":false},"text":"
Search Applicants and Owners separately: oregon state uni*
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Search Applicants and Owners separately:Univ* Oregon. Select more for logical variants. Add to collection. Select all patents in the collection and expand by simple families. Add to collection. Total patents: 690
Search Applicants and Owners separately: oregon state uni*
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Add to collection.
Select all patents in the collection and expand by simple families.
Add to collection. Total patents: 2512
Search Applicants and Owners separately:Univ* Oregon. Select more for logical variants. Add to collection. Select all patents in the collection and expand by simple families. Add to collection. Total patents: 690
a) a first nucleic acid molecule comprising a first promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of a green fluorescent protein (GFP) and a C-terminal portion of a tdTomato (tdT) fluorescent protein, wherein the N-terminal portion of the GFP and the C-terminal portion of the tdT protein are separated by a β-globin intron comprising a first loxP site, and wherein the first nucleic acid molecule is present at a locus of a first chromosome 11 of a chromosome 11 pair;\n
b) a second nucleic acid molecule comprising a second promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of the tdT protein and a C-terminal portion of the GFP, wherein the N-terminal portion of the tdT protein and the C-terminal portion of the GFP are separated by the β-globin intron comprising a second loxP site, and wherein the second nucleic acid molecule is present at the homologous locus of the second chromosome 11 of the chromosome 11 pair;\n
c) a mutated gene selected from the group consisting of a heterozygous null mutation in the p53 gene on the second chromosome 11 of the chromosome 11 pair, a heterozygous floxed neurofibromatosis type 1 (NF1) gene on the second chromosome 11 of the chromosome 11 pair, and a combination thereof; and\n
d) a third nucleic acid molecule encoding a Cre recombinase operably linked to a third promoter, wherein Cre recombinase-promoted somatic recombination between the first and second loxP sites occurs in at least one cell of the transgenic mouse resulting in at least a first cell comprising a first recombined nucleic acid molecule encoding a functional GFP and a homozygous null mutated gene and at least a second cell comprising a second recombined nucleic acid molecule encoding a functional tdT protein and a homozygous wild type mutated gene."],"number":1,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 1, wherein the nucleic acid molecule encoding the Cre recombinase is operably linked to a human glial fibrillary acidic protein (GFAP) promoter."],"number":2,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 1, wherein the locus of the first and second nucleic acid molecules on the chromosome 11 pair is between an Eif4enif1 gene and a Drg1 gene."],"number":3,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 1, wherein the first promoter or the second promoter comprises a CMV (3-actin promoter."],"number":4,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 1, wherein the transgenic mouse develops a glioma, wherein the glioma comprises at least one cell comprising the first recombined nucleic acid molecule encoding the functional GFP, the homozygous null mutation in the p53 gene, and the homozygous null mutation in the NF1 gene."],"number":5,"annotation":false,"title":false,"claim":true},{"lines":["A method for identifying a compound for treating or preventing a tumor, comprising:\n
administering at least one test compound to the transgenic mouse of claim 1;\n
determining a phenotype of the transgenic mouse; and\n
selecting a test compound that decreases the phenotype of the transgenic mouse as compared to a control, thereby identifying a compound that treats or prevents the tumor."],"number":6,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 6, wherein the phenotype of the transgenic mouse comprises a number of cells expressing GFP or a tumor characteristic."],"number":7,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 7, wherein the tumor characteristic is selected from the group consisting of tumor size, tumor cell gene expression, tumor growth, tumor number, tumor metastasis, and tumor recurrence."],"number":8,"annotation":false,"title":false,"claim":true},{"lines":["A method for identifying a compound for treating or preventing a tumor, comprising:\n
culturing in vitro at least one first cell from the transgenic mouse of claim 1;\n
contacting the first cell with at least one test compound;\n
determining a phenotype of the first cell; and\n
selecting a test compound that alters the phenotype of the first cell as compared to a control, thereby identifying a compound that treats or prevents the tumor."],"number":9,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 9, further comprising:\n
co-culturing in vitro the at least one first cell with at least one second cell from the transgenic mouse of claim 1."],"number":10,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 9, wherein the phenotype comprises cell number, cell proliferation, cell cycle stage, cell death, cell morphology, cell gene expression, or presence of one or more tumor sphere characteristic."],"number":11,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 11, wherein the selected test compound decreases cell number, cell proliferation, or gene expression of the first cell as compared to the control."],"number":12,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 11, wherein the selected test compound increases cell death of the first cell as compared to the control."],"number":13,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 10, wherein the at least one first cell and at least one second cell are initially present in the in vitro culture at a 1:1 ratio."],"number":14,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 14, wherein the phenotype is the ratio of the at least one first cell to the at least one second cell."],"number":15,"annotation":false,"title":false,"claim":true},{"lines":["The method of claim 15, wherein the selected compound decreases the ratio of the at least one first cell to the at least one second cell."],"number":16,"annotation":false,"title":false,"claim":true},{"lines":["A transgenic mouse the genome of which comprises:\n
a) a nucleic acid molecule comprising a promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of a tdTomato (tdT) fluorescent protein and a C-terminal portion of a green fluorescent protein (GFP), wherein the N-terminal portion of the tdT protein and the C-terminal portion of the GFP are separated by a β-globin intron comprising a first loxP site, and wherein the first nucleic acid molecule is present at a locus of a both chromosomes 11 of a chromosome 11 pair;\n
b) a heterozygous null mutation in the p53 gene on a first chromosome 11 of the chromosome 11 pair; and\n
c) a heterozygous floxed neurofibromatosis type 1 (NF1) gene on the first chromosome 11 of the chromosome 11 pair"],"number":17,"annotation":false,"title":false,"claim":true},{"lines":["A transgenic mouse the genome of which comprises a first nucleic acid molecule comprising a first promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of a green fluorescent protein (GFP) and a C-terminal portion of a tdTomato (tdT) fluorescent protein, wherein the N-terminal portion of the GFP and the C-terminal portion of the tdT protein are separated by a β-globin intron comprising a first loxP site, and wherein the nucleic acid molecule is present at a locus i of both chromosomes 11 of a chromosome 11 pair."],"number":18,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 18, further comprising a second nucleic acid molecule encoding a Cre recombinase operably linked to a promoter."],"number":19,"annotation":false,"title":false,"claim":true},{"lines":["A transgenic mouse the genome of which comprises:\n
a) a nucleic acid molecule comprising a promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of a green fluorescent protein (GFP) and a C-terminal portion of a tdTomato (tdT) fluorescent protein, wherein the N-terminal portion of the GFP and the C-terminal portion of the tdT protein are separated by a β-globin intron comprising a first loxP site, and wherein the first nucleic acid molecule is present at a locus of a both chromosomes 11 of a chromosome 11 pair;\n
b) a heterozygous null mutation in the p53 gene on a first chromosome 11 of the chromosome 11 pair; and\n
c) a heterozygous floxed neurofibromatosis type 1 (NF1) gene on the first chromosome 11 of the chromosome 11 pair"],"number":20,"annotation":false,"title":false,"claim":true},{"lines":["A transgenic mouse the genome of which comprises a first nucleic acid molecule comprising a first promoter operably linked to a nucleic acid molecule encoding an N-terminal portion of a tdTomato (tdT) fluorescent protein and a C-terminal portion of a green fluorescent protein (GFP), wherein the N-terminal portion of the tdT protein and the C-terminal portion of the GFP are separated by a β-globin intron comprising a first loxP site, and wherein the nucleic acid molecule is present at a locus of both chromosomes 11 of a chromosome 11 pair."],"number":21,"annotation":false,"title":false,"claim":true},{"lines":["The transgenic mouse of claim 18, further comprising a second nucleic acid molecule encoding a Cre recombinase operably linked to a promoter."],"number":22,"annotation":false,"title":false,"claim":true}]}},"filters":{"npl":[],"notNpl":[],"applicant":[],"notApplicant":[],"inventor":[],"notInventor":[],"owner":[],"notOwner":[],"tags":[],"dates":[],"types":[],"notTypes":[],"j":[],"notJ":[],"fj":[],"notFj":[],"classIpcr":[],"notClassIpcr":[],"classNat":[],"notClassNat":[],"classCpc":[],"notClassCpc":[],"so":[],"notSo":[],"sat":[]},"sequenceFilters":{"s":"SEQIDNO","d":"ASCENDING","p":0,"n":10,"sp":[],"si":[],"len":[],"t":[],"loc":[]}}