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  • Multi Infectious Disease Combo Rapid Test
  • Multi Infectious Disease Combo Rapid Test

Multi Infectious Disease Combo Rapid Test

Usage
The Multi Infectious Disease Combo Rapid Test is multi-line, serological, lateral flow chromatographic immunoassay for the qualitative detection of human immunodeficiency virus (HIV) type 1 antibody, type 2 antibody, hepatitis B virus (HBV) surface antigen, anti-HCV antibodies, and antibodies (IgG and IgM) to Treponema Pallidum in human whole blood, serum, or plasma specimens to aid in the diagnosis of infection with HIV, HBV, HCV, and Syphilis. The test only provides preliminary analysis results but not critical diagnosis criteria. Any reactive specimen with the Multi Infectious Disease Combo Rapid Test must be analyzed and confirmed with alternative testing method(s) and clinical findings. The test is intended for healthcare professional use. Applications of the test including, screening test for sex transmitted diseases (STD’s) among high-risk group of people, regular health examinations, and field screen test for blood bank.

 

Background of Clinical Indications

Human Immunodeficiency Virus type-1 (HIV-1) and type-2 (HIV-2) are enveloped single strand RNA virus that cause acquired immunodeficiency syndrome (AIDS). Current data indicate that the HIV is transmitted through sexual contact, exposure to blood (including sharing contaminated needle and syringe) or certain blood products or from an infected mother to her child during the prenatal period. People with increased risk of HIV infection include intravenous drug users, homosexuals, and hemophiliacs. The presence of antibodies to HIV- 1/HIV-2 indicates previous exposures to HIV-1/HIV-2 virus. Hepatitis B virus (HBV) is the most common cause of persistent viremia and the most important cause of chronic liver disease and hepatocellular carcinoma. Clinically apparent HBV infections may have been in existence for several millennia. It is estimated that there are 300 million chronic carriers of HBV in the world. The carrier rates vary from as little as 0.3% (Western countries) to 20% (Asia, Africa). HBV is a hepatotropic DNA virus. The core of the virus contains a DNA polymerase, the core antigen (HBcAg) and the e antigen (HBeAg). The core of HBV is enclosed in a coat that contains lipid, carbohydrate and protein including an antigen termed hepatitis B surface antigen (HBsAg). HBsAg is the first marker to appear in the blood in acute hepatitis B, detectable 1 week to 2 months after exposure and 2 weeks to 2 months before the onset of symptoms. Three weeks after the onset of acute hepatitis almost half of the patients will still be positive for HBsAg. In the chronic carrier state, HBsAg persists for long periods (6-12 months) with no seroconversion to the corresponding antibodies. Therefore, screening for HBsAg is highly desirable for all donors, pregnant women and people in high-risk groups. Hepatitis C Virus (HCV) is a small, enveloped, positive-sense, single-stranded RNA Virus. HCV is now known to be the major cause of parenterally transmitted non-A, non-B hepatitis. Antibody to HCV is found in over 80% of patients with well-documented non-A, non-B hepatitis. Conventional methods fail to isolate the virus in cell culture or visualize it by electron microscope. Cloning the viral genome has made it possible to develop serologic assays that use recombinant antigens. Compared to the first-generation HCV EIAs using single recombinant antigen, multiple antigens using recombinant protein and/or synthetic peptides have been added in new serologic tests to avoid nonspecific cross-reactivity and to increase the sensitivity of the HCV antibody tests. Dual infection with HBV and HCV is not uncommon in geographic areas where a high endemic level of both infections is reported such as Southeast-Asia and the Mediterranean. In general, the prevalence is around 10-20% in patients with chronic HBV infection, and 2- 10% of anti-HCV-positive patients have markers of HBV infection. Co-infection of HBV and HCV was found to be high in HIV-infected people (66%), particularly in HIV infected drug users (84%). Syphilis is a systemic disease caused by Treponema Pallidum. The signs and symptoms of syphilis vary depending in which of the four stages it presents (primary, secondary, latent, and tertiary). Treponema Pallidum (TP) is the causative agent of the venereal disease Syphilis. TP is a spirochete bacterium with an outer envelope and a cytoplasmic membrane. One study reported a substantial epidemiological correlation between the acquisition and transmission of the HIV virus and Syphilis. Multiple clinical stages and long periods of latent, asymptomatic infection are characteristic of Syphilis. Primary Syphilis is defined by the presence of a chancre at the site of inoculation. The antibodies response to the TP bacterium can be detected within 4 to 7 days after the chancre appears. The infection remains detectable until the patient receives adequate treatment. The Multi Infectious Disease Combo Rapid Test utilizes recombinant HIV antigen coated particle and recombinant HIV antigen immobilized on a membrane to detect HIV type 1 and/or HIV type 2 antibody, anti-HBsAg antibodies to detect elevated levels of HBsAg, recombinant HCV core and non-structure antigens to detect anti-HCV antibodies, and a double antigen combination of a Syphilis antigen coated particle and Syphilis antigen immobilized on membrane to detect anti-TP antibodies (IgG and IgM) qualitatively and selectively in human whole blood, serum, or plasma specimens. This assay can be performed to get test result at 15-20 minutes by minimally trained personnel and without cumbersome laboratory equipment.

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Packing specification

Principle of Inspection

Human Immunodeficiency Virus type-1 (HIV-1) and type-2 (HIV-2) are enveloped single strand RNA virus that cause acquired immunodeficiency syndrome (AIDS). Current data indicate that the HIV is transmitted through sexual contact, exposure to blood (including sharing contaminated needle and syringe) or certain blood products or from an infected mother to her child during the prenatal period. People with increased risk of HIV infection include intravenous drug users, homosexuals, and hemophiliacs. The presence of antibodies to HIV- 1/HIV-2 indicates previous exposures to HIV-1/HIV-2 virus. Hepatitis B virus (HBV) is the most common cause of persistent viremia and the most important cause of chronic liver disease and hepatocellular carcinoma. Clinically apparent HBV infections may have been in existence for several millennia. It is estimated that there are 300 million chronic carriers of HBV in the world. The carrier rates vary from as little as 0.3% (Western countries) to 20% (Asia, Africa). HBV is a hepatotropic DNA virus. The core of the virus contains a DNA polymerase, the core antigen (HBcAg) and the e antigen (HBeAg). The core of HBV is enclosed in a coat that contains lipid, carbohydrate and protein including an antigen termed hepatitis B surface antigen (HBsAg).

HBsAg is the first marker to appear in the blood in acute hepatitis B, detectable 1 week to 2 months after exposure and 2 weeks to 2 months before the onset of symptoms. Three weeks after the onset of acute hepatitis almost half of the patients will still be positive for HBsAg. In the chronic carrier state, HBsAg persists for long periods (6-12 months) with no seroconversion to the corresponding antibodies. Therefore, screening for HBsAg is highly desirable for all donors, pregnant women and people in high-risk groups.

Hepatitis C Virus (HCV) is a small, enveloped, positive-sense, single-stranded RNA Virus. HCV is now known to be the major cause of parenterally transmitted non-A, non-B hepatitis. Antibody to HCV is found in over 80% of patients with well-documented non-A, non-B hepatitis. Conventional methods fail to isolate the virus in cell culture or visualize it by electron microscope. Cloning the viral genome has made it possible to develop serologic assays that use recombinant antigens. Compared to the first-generation HCV EIAs using single recombinant antigen, multiple antigens using recombinant protein and/or synthetic peptides have been added in new serologic tests to avoid nonspecific cross-reactivity and to increase the sensitivity of the HCV antibody tests.

Dual infection with HBV and HCV is not uncommon in geographic areas where a high endemic level of both infections is reported such as Southeast-Asia and the Mediterranean. In general, the prevalence is around 10-20% in patients with chronic HBV infection, and 2- 10% of anti-HCV-positive patients have markers of HBV infection. Co-infection of HBV and HCV was found to be high in HIV-infected people (66%), particularly in HIV infected drug users (84%). Syphilis is a systemic disease caused by Treponema Pallidum. The signs and symptoms of syphilis vary depending in which of the four stages it presents (primary, secondary, latent, and tertiary). Treponema Pallidum (TP) is the causative agent of the venereal disease Syphilis. TP is a spirochete bacterium with an outer envelope and a cytoplasmic membrane. One study reported a substantial epidemiological correlation between the acquisition and transmission of the HIV virus and Syphilis. Multiple clinical stages and long periods of latent, asymptomatic infection are characteristic of Syphilis. Primary Syphilis is defined by the presence of a chancre at the site of inoculation. The antibodies response to the TP bacterium can be detected within 4 to 7 days after the chancre appears. The infection remains detectable until the patient receives adequate treatment. The Multi Infectious Disease Combo Rapid Test utilizes recombinant HIV antigen coated particle and recombinant HIV antigen immobilized on a membrane to detect HIV type 1 and/or HIV type 2 antibody, anti-HBsAg antibodies to detect elevated levels of HBsAg, recombinant HCV core and non-structure antigens to detect anti-HCV antibodies, and a double antigen combination of a Syphilis antigen coated particle and Syphilis antigen immobilized on membrane to detect anti-TP antibodies (IgG and IgM) qualitatively and selectively in human whole blood, serum, or plasma specimens. This assay can be performed to get test result at 15-20 minutes by minimally trained personnel and without cumbersome laboratory equipment.

Specification packaging

20 Tests/Kit.

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About Kangte

Zhejiang Kangte Biotechnology Co., Ltd

Zhejiang Kangte Biotechnology Co., Ltd. was established in 2001 and is located in Zhejiang Xinchang Provincial High-tech Industrial Park. It is a national high-tech enterprise integrating R&D, production and sales of in vitro diagnostic reagents. Relying on the pioneering team spirit and scientific management, the company has repeatedly won the national advanced production unit in the in vitro diagnostic industry. 

The company has GMP standard workshops, clean workshops, R&D laboratories, equipped with high-precision testing equipment and fully automatic production equipment. In order to enhance the company's overall R&D strength, it has established a good "production-study-research" cooperative relationship with many colleges and universities. The company has obtained a number of invention patents and utility model patents and has passed ISO9001, ISO14001, ISO13485, and other system certifications. The company currently has more than 100 registered products, covering biochemical, immunological, and other fields, and many of the products have reached the leading domestic level in technology. 

The company adheres to the concept of "integrity, professionalism, efficiency and innovation" to serve customers, and constantly introduces products with higher technological content to provide customers. The company will, as always, position itself in "service technology, professionalism and efficiency, and achieve customers", and work hard to jointly shape the IVD industry and continuously improve the level of human health.

 

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