公开(公告)号：US20120244542A1

公开(公告)日：2012-09-27

申请号：US13438464

申请日：2012-04-03

Applicant: Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C12Q1/68

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

公开(公告)号：US20090311694A1

公开(公告)日：2009-12-17

申请号：US12386146

申请日：2009-04-14

Applicant: Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C12Q1/68 ,  C07H21/02

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

Abstract translation: 公开了由人IL-23R mRNA的选择性剪接引起的人IL-23R剪接变体的克隆和鉴定。 通过在IL-23R基因内跳过一个，多个完整外显子或部分外显子，发生替代的mRNA形式。 共鉴定了25种不同的IL-23R转录物。 公开了白细胞介素23受体中的新型外显子缺失（外显子9）同种型，表示为Delta9。 本申请还描述了用于测量不同IL-23R同种型的定量测定。 检测IL-23R的Delta9同种型主要存在于结肠和子宫颈组织中。 在Crohn患者的发炎结肠组织中观察到Delta9的减少。 公开了通过测量IL-23R的Delta9同种型来预测克罗恩病的方法。

公开(公告)号：US20130196333A1

公开(公告)日：2013-08-01

申请号：US13764827

申请日：2013-02-12

Applicant: Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C12Q1/68

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

Abstract translation: 公开了由人IL-23R mRNA的选择性剪接引起的人IL-23R剪接变体的克隆和鉴定。 通过在IL-23R基因内跳过一个，多个完整外显子或部分外显子，发生替代的mRNA形式。 共鉴定了25种不同的IL-23R转录物。 公开了白细胞介素23受体中的新型外显子缺失（外显子9）同种型，表示为Delta9。 本申请还描述了用于测量不同IL-23R同种型的定量测定。 检测IL-23R的Delta9同种型主要存在于结肠和子宫颈组织中。 在Crohn患者的发炎结肠组织中观察到Delta9的减少。 公开了通过测量IL-23R的Delta9同种型来预测克罗恩病的方法。

公开(公告)号：US08404824B2

公开(公告)日：2013-03-26

申请号：US13438456

申请日：2012-04-03

Applicant: Gant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Gant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C07H21/02 ,  C12P19/34

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

Abstract translation: 公开了由人IL-23R mRNA的选择性剪接引起的人IL-23R剪接变体的克隆和鉴定。 通过在IL-23R基因内跳过一个，多个完整外显子或部分外显子，发生替代的mRNA形式。 共鉴定了25种不同的IL-23R转录物。 公开了白细胞介素23受体中的新型外显子缺失（外显子9）同种型，表示为＆Dgr; 9。 本申请还描述了用于测量不同IL-23R同种型的定量测定。 检测IL-23R的＆Dgr。9同种型主要存在于结肠和子宫颈组织中。 在克罗恩病患者的发炎结肠组织中观察到“Dgr”降低9。 公开了通过测量IL-23R的Dgr 9同种型来预测克罗恩病的方法。

公开(公告)号：US20120245325A1

公开(公告)日：2012-09-27

申请号：US13438456

申请日：2012-04-03

Applicant: Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C07K14/54

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

Abstract translation: 公开了由人IL-23R mRNA的选择性剪接引起的人IL-23R剪接变体的克隆和鉴定。 通过在IL-23R基因内跳过一个，多个完整外显子或部分外显子，发生替代的mRNA形式。 共鉴定了25种不同的IL-23R转录物。 公开了白细胞介素23受体中的新型外显子缺失（外显子9）同种型，表示为＆Dgr; 9。 本申请还描述了用于测量不同IL-23R同种型的定量测定。 检测IL-23R的＆Dgr。9同种型主要存在于结肠和子宫颈组织中。 在克罗恩病患者的发炎结肠组织中观察到“Dgr”降低9。 公开了通过测量IL-23R的Dgr 9同种型来预测克罗恩病的方法。

公开(公告)号：US08206925B2

公开(公告)日：2012-06-26

申请号：US12386146

申请日：2009-04-14

Applicant: Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

Inventor： Grant Gallagher ,  Raymond Yu ,  Shih-hsin Kan ,  Giacomo Mancini

IPC: C12Q1/68 ,  C12P19/34 ,  C07H21/04

CPC classification number: C12Q1/6876 ,  C12Q1/6883 ,  C12Q2600/156 ,  C12Q2600/158

Abstract: There is disclosed the cloning and identification of human IL-23R splice variants caused by alternative splicing of the IL-23R mRNA in human. Alternative mRNA forms occur through skipping one, multiple full exons or partial exons, within the IL-23R gene. A total of twenty-five (25) different IL-23R transcripts were identified. A novel exon deletion (exon 9) isoform in the interleukin 23 receptor is disclosed, denoted as Δ9. The present application also describes a quantitative assay to measure different IL-23R isoform. Detection of Δ9 isoform of IL-23R is predominantly present in colon and cervical tissues. A decrease in Δ9 is observed in inflamed colon tissues in Crohn's patients. There is disclosed a method of predicting Crohn's disease by measuring Δ9 isoform of IL-23R.

Abstract translation: 公开了由人IL-23R mRNA的选择性剪接引起的人IL-23R剪接变体的克隆和鉴定。 通过在IL-23R基因内跳过一个，多个完整外显子或部分外显子，发生替代的mRNA形式。 共鉴定了25种不同的IL-23R转录物。 公开了白细胞介素23受体中的新型外显子缺失（外显子9）同种型，表示为＆Dgr; 9。 本申请还描述了用于测量不同IL-23R同种型的定量测定。 检测IL-23R的＆Dgr。9同种型主要存在于结肠和子宫颈组织中。 在克罗恩病患者的发炎结肠组织中观察到“Dgr”降低9。 公开了通过测量IL-23R的Dgr 9同种型来预测克罗恩病的方法。