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Diagnosis Method Of Alcoholic Or Non-Alcoholic Steato-Hepatitis Using Biochemical Markers

a technology of steato-hepatitis and biochemical markers, which is applied in the direction of biochemistry apparatus and processes, instruments, material analysis, etc., can solve the problems of liver transplantation and death, no such diagnosis test is currently available for the more precise diagnosis of ash, and none of these studies has really identified an accurate combination of ash markers, so as to reduce the number of biopsy indications and reduce the risk of liver biopsies. , the effect of reducing the cost and the risk o

Inactive Publication Date: 2008-06-19
ASSISTANCE PUBLIQUE HOPITAUX DE PARIS
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

The present invention provides a way to diagnose alcoholic or non-alcoholic steato-hepatitis by measuring certain substances in a patient's blood. This method can predict who will develop the disease with a high degree of accuracy, which can help reduce the need for liver biopsies and lower the cost and risk to patients and society.

Problems solved by technology

Chronic alcoholic liver disease affects millions of individuals worldwide and is a major cause of liver transplantation and death.
1995;22(2 Suppl):96-9), but none of these studies has really identified an accurate combination of markers of ASH.
However, no such diagnosis test is currently available for the more precise diagnosis of ASH or NASH.

Method used

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  • Diagnosis Method Of Alcoholic Or Non-Alcoholic Steato-Hepatitis Using Biochemical Markers
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  • Diagnosis Method Of Alcoholic Or Non-Alcoholic Steato-Hepatitis Using Biochemical Markers

Examples

Experimental program
Comparison scheme
Effect test

example 1

[0081]Patients and Methods

1.1. Patients

[0082]Patients with heavy alcohol consumption, available serum and a consistent liver biopsy were included (FIG. 1). The criteria of inclusion was that all included patients had a self-reported daily alcohol consumption equivalent to at least 50 gm of pure ethanol during the preceding year, with a mean of 146 (se=80) gm per day for 17 years. The patient's families were also interviewed, when possible. All patients gave informed consent for the use of data and serum for research purposes. Non-inclusion criteria included concomitant liver diseases (the presence of HCV antibodies or HBs antigen, hemochromatosis, cholestatic disease, autoimmune disease), HIV antibodies and Immunosuppression, non-available serum, non-available biopsies and patients for whom biopsy and serum were collected more than one month apart.

[0083]The analysis was performed on a first group (training group) and validated on 2 different groups (validation groups).

[0084]Training...

example 2

Statistical Analysis

[0100]Statistical analysis used Fisher's exact test, the chi-square test, Student's t test, the Mann-Whitney test and variance analysis using the Bonferroni all-pair wise and Tukey-Kramer multiple-comparison tests to take into account the multiple comparisons and multiple logistic regression for multivariate analysis. The analysis was performed on a first group (training group) and validated on 2 different groups (validation groups 1 and 2), in cohorts of patients as in Table 1.

[0101]According to the ASH scoring system, patients were divided into several groups.

[0102]The primary outcome was the identification of patients with alcoholic hepatitis (mild, moderate or severe).

[0103]In a secondary analysis, patients were classified according to the presence of each elementary feature of alcoholic hepatitis and according to a 4 scale scoring system.

[0104]The first stage consisted of identifying factors which differed significantly between these groups by unidimensiona...

example 3

Determination of the Logistic Function

[0111]The AshTest score is defined as the logistic regression function combining the independent factors that returns the best index in term of discrimination between the presence or absence of ASH.

[0112]In Table 2 are given the characteristics of patients according to the presence of alcoholic steato-hepatitis for each of the seven biochemical markers, the AST / ALT ratio, the Maddrey function, the FibroTest score, the ActiTest score, and the AshTest score, as well as their independent association with fibrosis (P value).

TABLE 2Characteristics of patients according to the presence of alcoholic hepatitisAlcoholic hepatitisIn the training groupAlcoholic hepatitisAlcoholic hepatitisNo n = 28In the Validation group 1In the Validation group 2Characteristicm (SD)Yes n = 42P valueNo n = 50Yes n = 12P valueNo n = 71Yes n = 22P valueDemographicsAge at biopsy, years53.9 (11.2)53.4 (10.7)0.6655.2 (7.2) 47.8 (8.3) 0.00546.3 (10.2)50.5 (11.5)0.22Male gender  ...

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Abstract

The present invention is drawn to a new diagnosis method for detecting the extent of alcoholic or non-alcoholic steato-hepatitis in a patient, in particular in a patient suffering from a disease involving alcoholic or non-alcoholic steato-hepatitis or who already had a positive diagnosis test of liver fibrosis and / or presence of liver necroinfiammatory lesions, by using the serum concentration of easily detectable biological markers. The invention is also drawn to diagnosis kits for the implementation of the method.

Description

FIELD OF THE INVENTION[0001]The present invention is drawn to a new diagnosis method for detecting the extent of alcoholic steato-hepatitis (ASH) or non-alcoholic steato-hepatitis (NASH) in a patient, in particular in a patient suffering from a disease involving alcoholic or non-alcoholic steato-hepatitis or who already had a positive diagnosis test of liver fibrosis and / or presence of liver necroinflammatory lesions, by using the serum concentration of easily detectable biological markers. The invention is also drawn to diagnosis kits for the implementation of the method.BACKGROUND OF THE INVENTION[0002]Chronic alcoholic liver disease affects millions of individuals worldwide and is a major cause of liver transplantation and death. Although the majority will not develop complications, 15-40% may develop serious liver sequelae, including end-stage liver disease and hepatocellular carcinoma. Those at the highest risk include patients with cirrhosis and alcoholic steato-hepatitis (Mat...

Claims

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Application Information

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Patent Type & Authority Applications(United States)
IPC IPC(8): G01N33/53G06F19/00
CPCC12Q1/48G01N33/92G01N33/576
Inventor POYNARD, THIERRY
Owner ASSISTANCE PUBLIQUE HOPITAUX DE PARIS
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