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Application of phosphorylated protein in membranous nephropathy

A membranous nephropathy and protein technology, applied in the field of nephropathy, can solve the problems of IMN diagnosis and clinical treatment difficulties, serious physiological, psychological and social burdens, etc.

Pending Publication Date: 2022-01-07
深圳临研医学有限公司
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  • Abstract
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AI Technical Summary

Problems solved by technology

Although some research results have been achieved in IMN disease markers and pathogenesis, the key trigger source of the disease, complement activation mechanism and the specific molecular mechanism leading to podocyte damage have not been fully clarified, which also poses a challenge to the diagnosis and clinical diagnosis of IMN. Treatment brings certain difficulties. Once patients enter the stage of ESRD, they will face more serious physical, psychological and social burdens.

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  • Application of phosphorylated protein in membranous nephropathy
  • Application of phosphorylated protein in membranous nephropathy
  • Application of phosphorylated protein in membranous nephropathy

Examples

Experimental program
Comparison scheme
Effect test

Embodiment 1

[0022] Example 1: Screening of differentially phosphorylated proteins

[0023] 1. Selection of IMN patients and control groups

[0024] The IMN group consisted of 16 patients diagnosed with IMN (including 11 cases of stage II IMN and 5 cases of stage III IMN, so they were divided into stage II IMN group and stage III IMN group). The group selected 10 patients with mild glomerular abnormalities confirmed by pathology, which can be regarded as the control group of healthy people in this experiment, and the basic conditions such as sex and age matched the selected IMN patients. The diagnosis of IMN patients is confirmed by pathological diagnosis of renal biopsy (light microscope and electron microscope pathology), and secondary MN such as tumor, infection, drug, autoimmune disease such as systemic lupus erythematosus is excluded clinically. Renal biopsy tissue samples and clinical data, relevant laboratory test results and pictures of pathological test reports were collected in ...

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Abstract

The invention discloses application of a reagent for quantitatively detecting the phosphorylation level of a T567 site of a protein EZR in preparation of a membranous nephropathy diagnostic reagent. In the research process, the applicant finds that the phosphorylation level of the EZR phosphorylation site T567 is obviously reduced in an IMN group compared with a control group, and the phosphorylation level is possibly gradually reduced along with disease progression. Downregulation of the phosphorylation level of T567 may participate in podocyte damage in the IMN disease progression process. And the statistical results of the immunohistochemical staining intensity and the cell positive rate of the slice further prove that the phosphorylation level of the EZRT567 site is indeed reduced in the renal biopsy tissue of the IMN patient, so that the membranous nephropathy can be diagnosed through the reagent capable of quantitatively detecting the phosphorylation level of the T567 site of the protein EZR.

Description

technical field [0001] The application relates to the technical field of nephropathy, in particular to the application of phosphorylated protein in membranous nephropathy. Background technique [0002] Membranous nephropathy (MN) is the most common cause of nephrotic syndrome in adults. According to different etiologies, MN can be divided into idiopathic membranous nephropathy (IMN) and secondary membranous nephropathy (SMN), of which IMN accounts for about 75%, and the etiology is unknown; SMN etiology is relatively clear , tumors, infections, drugs, autoimmune diseases such as systemic lupus erythematosus, etc. can lead to SMN. Patients with MN usually present with severe proteinuria, edema, hypoalbuminemia, and hyperlipidemia, and the diagnosis depends on the pathology of renal biopsy. With capillary wall deposition, electron microscopy shows the formation of electron-dense material under the visceral epithelial cells of the glomeruli; however, IMN can only be diagnosed...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): G01N33/68A61K45/00A61P13/12
CPCG01N33/6893A61K45/00A61P13/12G01N2800/347G01N2333/47
Inventor 戴勇李珊珊汤冬娥何敬全
Owner 深圳临研医学有限公司
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