1 / 3

Biomarkers and Antibodies Development for Liver Cirrhosis

As a pioneer in the in vitro diagnostic (IVD) field, Creative Biolabs focuses on providing quality and innovative antibodies for IVD use to further serve the clinical market.

bellasmith12
Download Presentation

Biomarkers and Antibodies Development for Liver Cirrhosis

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Biomarkers and Antibodies Development for Liver Cirrhosis As a pioneer in the in vitro diagnostic (IVD) field, Creative Biolabs focuses on providing quality and innovative antibodies for IVD use to further serve the clinical market. We offer first-class antibody development services that target all stages of liver diseases, such as hepatitis, fibrosis, cirrhosis, and liver failure. Introduction of Liver Cirrhosis Liver cirrhosis (LC), the end stage of many forms of chronic hepatitis of different etiologies, is a diffuse process characterized by fibrosis and the conversion of normal liver architecture into structurally abnormal nodules surrounded by annular fibrosis. This chronic progressive clinical condition leads to liver cell failure and portal hypertension, which can favor the onset of hepatocellular carcinoma (HCC). The most common causes of cirrhosis include alcohol, hepatitis B, hepatitis C, and nonalcoholic steatohepatitis (NASH). Fig.1 Comparison between normal liver and liver cirrhosis. The Diagnosis of Liver Cirrhosis Clinically, LC may be divided into two phases: compensated and decompensated. Decompensated LC is easily diagnosed as it presents with a series of clinical and laboratory signs such as ascites, sepsis, variceal bleeding, encephalopathy, and non-obstructive jaundice, while compensated LC may be difficult to differentiate from chronic hepatitis. Consequently, accurate evaluation of the fibrosis stage or of the appearance of overt cirrhosis is

  2. fundamental not only to reach a correct diagnosis but also to commence correct treatment or screening protocols to permit an early diagnosis of the frequent and fatal complications of LC, such as esophageal varices, HCC. The diagnosis approaches of liver cirrhosis mainly include clinical examination, laboratory tests, and ancillary studies. Liver biopsy, which is considered as the reference standard method of fibrosis diagnosis and staging, is usually unnecessary if clinical findings and imaging studies (e.g., evidence of decompensation, with ascites and impaired hepatic biosynthesis) are sufficient for the diagnosis of cirrhosis. In cases of suspected cirrhosis, a transcutaneous liver biopsy is indicated if the clinical findings leave the diagnosis in doubt or if the biopsy is expected to yield information about the cause of cirrhosis that will affect the choice of treatment. However, liver biopsy is of no help in staging cirrhosis. Fig.2 Risk factors that can directly lead to cirrhosis. (Xie, 2017) Noninvasive Diagnostic Evaluation of Cirrhosis Noninvasive methods obviated the need for liver biopsy, including serological tests and imaging instruments, have been developed recently for the diagnostic evaluation of cirrhosis. Serum markers offer a cost-effective alternative to liver biopsy being less invasive and theoretically without complications. They can be classified into direct and indirect markers which may be used alone or in combination to produce composite scores. Diagnostic imaging includes a number of instruments and techniques to estimate liver fibrosis and cirrhosis like ultrasound, elastography techniques, and CT. Currently, it can be affirmed that both serological tests and imaging techniques are quite reliable for

  3. diagnosing LC as well as for excluding the presence of fibrosis. In contrast, in the intermediate stages, their reliability is limited. The continued discovery of novel biomarkers for disease detection and monitoring, as well as the advent of modern antibody techniques, have driven the development of IVD antibodies in the in vitro diagnostic market. With years of experience serving the life science industry, Creative Biolabs provides IVD antibody development services raised against a wide panel of biomarkers for the diagnosis of liver cirrhosis. In addition, our staff scientists and technical team have the knowledge and experience to provide the highest quality services in other areas. Contact us to discuss your specific requirements and experience the great value of our expert services. Biomarker available now for liver cirrhosis diagnosis: Cholinesterase Kallistatin GP73 CD26 C-reactive protein Copeptin Cortisol Vitamin D Reference 1. Xie, J., (2017). "Metabolomic applications in hepatocellular carcinoma: toward the exploration of therapeutics and diagnosis through small molecules." Rsc Advances, 7:28. Related Services: Biomarkers and Antibodies Development for Hepatitis Biomarkers and Antibodies Development for Liver Fibrosis Biomarkers and Antibodies Development for Liver Failure

More Related