公开(公告)号：US20130330724A1

公开(公告)日：2013-12-12

申请号：US13966996

申请日：2013-08-14

Applicant: Academia Sinica

Inventor： Yuan-Tsong Chen ,  Shuen-lu Hung ,  Wen-hung Chung ,  Jer-Yuarn Wu

IPC: C12Q1/68

CPC classification number: C12Q1/6881 ,  C12Q1/6883 ,  C12Q2600/156 ,  G01N33/94

Abstract: The present invention provides a method of predicting the risk of a patient for developing adverse drug reactions, particularly SJS or TEN. It was discovered that an HLA-B allele, HLA-B* 1502, is associated with SJS/TEN that is induced by a variety of drugs. The correlation with HLA-B* 1502 is most significant for carbamazepine-induced SJS/TEN, wherein all the patients tested have the HLA-B* 1502 allele. In addition, another HLA-B allele, HLA-B*5801, is particularly associated with SJS/TEN induced by allopurinol. Milder cutaneous reactions, such as maculopapular rash, erythema multiforme (EM), urticaria, and fixed drug eruption, are particularly associated with a third allele, HLA-B *4601. For any of the alleles, genetic markers (e.g., HLA markers, microsatellite, or single nucleotide polymorphism markers) located between DRB1 and HLA-A region of the specific HLA-B haplotype can also be used for the test.

Abstract translation: 本发明提供了一种预测患者发展不良药物反应（特别是SJS或TEN）的风险的方法。 发现HLA-B等位基因HLA-B * 1502与由各种药物诱导的SJS / TEN相关。 与HLA-B * 1502的相关性对于卡马西平诱导的SJS / TEN是最显着的，其中所有测试的患者具有HLA-B * 1502等位基因。 另外HLA-B等位基因HLA-B * 5801与别嘌呤醇诱导的SJS / TEN特别相关。 特别是与第三等位基因HLA-B * 4601相关的皮肤反应较轻，如斑丘疹，多形性红斑，荨麻疹和固定药物爆发。 对于任何等位基因，位于特异性HLA-B单倍型的DRB1和HLA-A区之间的遗传标记（例如HLA标记，微卫星或单核苷酸多态性标记）也可用于测试。

公开(公告)号：US09562268B2

公开(公告)日：2017-02-07

申请号：US13966996

申请日：2013-08-14

Applicant: Academia Sinica

Inventor： Yuan-Tsong Chen ,  Shuen-lu Hung ,  Wen-hung Chung ,  Jer-Yuarn Wu

IPC: C12Q1/68 ,  C12P19/34 ,  G01N33/94 ,  C12M1/34

CPC classification number: C12Q1/6881 ,  C12Q1/6883 ,  C12Q2600/156 ,  G01N33/94

Abstract: The present invention provides a method of predicting the risk of a patient for developing adverse drug reactions, particularly SJS or TEN. It was discovered that an HLA-B allele, HLA-B* 1502, is associated with SJS/TEN that is induced by a variety of drugs. The correlation with HLA-B* 1502 is most significant for carbamazepine-induced SJS/TEN, wherein all the patients tested have the HLA-B* 1502 allele. In addition, another HLA-B allele, HLA-B*5801, is particularly associated with SJS/TEN induced by allopurinol. Milder cutaneous reactions, such as maculopapular rash, erythema multiforme (EM), urticaria, and fixed drug eruption, are particularly associated with a third allele, HLA-B *4601. For any of the alleles, genetic markers (e.g., HLA markers, microsatellite, or single nucleotide polymorphism markers) located between DRB1 and HLA-A region of the specific HLA-B haplotype can also be used for the test.

Abstract translation: 本发明提供了一种预测患者发展不良药物反应（特别是SJS或TEN）的风险的方法。 发现HLA-B等位基因HLA-B * 1502与由各种药物诱导的SJS / TEN相关。 与HLA-B * 1502的相关性对于卡马西平诱导的SJS / TEN是最显着的，其中所有测试的患者具有HLA-B * 1502等位基因。 另外HLA-B等位基因HLA-B * 5801与别嘌呤醇诱导的SJS / TEN特别相关。 特别是与第三等位基因HLA-B * 4601相关的皮肤反应较轻，如斑丘疹，多形性红斑，荨麻疹和固定药物爆发。 对于任何等位基因，位于特异性HLA-B单倍型的DRB1和HLA-A区之间的遗传标记（例如HLA标记，微卫星或单核苷酸多态性标记）也可用于测试。

公开(公告)号：US20230243810A1

公开(公告)日：2023-08-03

申请号：US18116952

申请日：2023-03-03

Applicant: ACADEMIA SINICA

Inventor： Yuan-Tsong Chen ,  Yi-Ching Lee ,  Jer-Yuarn Wu ,  Hsiao-Jung Kao

IPC: G01N33/50 ,  A61P19/00 ,  A61P35/00 ,  A01K67/027 ,  A61K31/409 ,  A61K36/21

CPC classification number: G01N33/502 ,  A61P19/00 ,  A61P35/00 ,  A01K67/0278 ,  A61K31/409 ,  A61K36/21 ,  A01K2217/072 ,  A01K2227/105 ,  A01K2267/0331 ,  G01N2500/10

Abstract: A method of inhibiting an overactive fibroblast growth factor receptor 3 (FGFR3) in a cell by contacting the cell with a composition that contains an effective amount of Pheophorbide a, Pyropheophorbide a, or an active derivative thereof. Also disclosed is a method for treating a disorder associated with an overactive FGFR3 with a composition containing an effective amount of Pheophorbide a, Pyropheophorbide a, or an active derivative thereof. Further, a composition for treating a disorder associated with an overactive FGFR3 is described. The composition contains an ethanol extract of Amaranthus viridis.

公开(公告)号：US20170153250A1

公开(公告)日：2017-06-01

申请号：US15327280

申请日：2015-07-23

Applicant: Academia Sinica

Inventor： Yuan-Tsong Chen ,  Jer-Yuarn Wu ,  Tai-Ming Ko ,  Ho-Chang Kuo ,  Jeng-Sheng Chang

IPC: G01N33/68 ,  A61K31/56 ,  A61K39/395

CPC classification number: G01N33/6893 ,  A61K31/56 ,  A61K39/395 ,  A61K2039/505 ,  C07K16/00 ,  G01N33/6863 ,  G01N33/6869 ,  G01N2333/522 ,  G01N2333/54 ,  G01N2333/5418 ,  G01N2333/7056 ,  G01N2333/70578 ,  G01N2800/328

Abstract: Described is a method of diagnosing, treating, or monitoring a treatment for Kawasaki disease in a subject. The method includes detecting the level of a biomarker in a sample obtained from the subject, the biomarker being IL-7F, sCD40L, MPIF-1, E-selectin, IP-10, or IL-33. The level is compared to a cut-off level. Also described is a kit for carrying out the method.

公开(公告)号：US10983133B2

公开(公告)日：2021-04-20

申请号：US15327280

申请日：2015-07-23

Applicant: Academia Sinica

Inventor： Yuan-Tsong Chen ,  Jer-Yuarn Wu ,  Tai-Ming Ko ,  Ho-Chang Kuo ,  Jeng-Sheng Chang

IPC: A61K39/395 ,  G01N33/68 ,  C07K16/00 ,  A61K31/56 ,  A61K39/00

Abstract: Described is a method of diagnosing, treating, or monitoring a treatment for Kawasaki disease in a subject. The method includes detecting the level of a biomarker in a sample obtained from the subject, the biomarker being IL-7F, sCD40L, MPIF-1, E-selectin, IP-10, or IL-33. The level is compared to a cut-off level. Also described is a kit for carrying out the method.