Difference between revisions of "Team:Wageningen UR/Background"

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<p>Especially in developing countries, infectious diseases are the major cause of death and account for more than half of all deaths in children [3] and many young adults [4]. Loss of so many potentially healthy and productive years greatly affects the economy [4] and society as a whole. Examples such as the SARS epidemic of 2002, the influenza A pandemic of 2006 or the more recent Ebola epidemic of 2014 have shown that outbreaks can happen unexpectedly and quickly. Other examples are Zika virus, a viral disease causing major outbreaks in South and Central America, or African Sleeping Sickness, which is caused by Human African Trypanosomiasis (HAT) and has been endemic in African countries for many decades. These facts underline the necessity of proper surveillance and global communication for fast responses against possible threats.
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<p>Especially in developing countries, infectious diseases are the major cause of death and account for more than half of all deaths in children [3] and many young adults [4]. Loss of so many potentially healthy and productive years greatly affects the economy [4] and society as a whole. Examples such as the SARS epidemic of 2002, the influenza A pandemic of 2006 or the more recent Ebola epidemic of 2014 have shown that outbreaks can happen unexpectedly and quickly. Other examples are Zika virus, a viral disease causing major outbreaks in South and Central America, and African Sleeping Sickness, which is caused by Human African Trypanosomiasis (HAT) and has been endemic in African countries for many decades. These facts underline the necessity of proper surveillance and global communication for fast responses against possible threats.
 
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<p>When such an epidemic emerges, the main priority is curing patients of their infection. Diagnosis is critical here, as in order to cure a person one should first know which disease the patient is infected with. Moreover, diagnosis of potential patients is important as well, as this allows for proper treatment, limitation of further spread (e.g. quarantine) and monitoring the disease impact over time [4,5]. This is especially important when there are no vaccines available.
 
<p>When such an epidemic emerges, the main priority is curing patients of their infection. Diagnosis is critical here, as in order to cure a person one should first know which disease the patient is infected with. Moreover, diagnosis of potential patients is important as well, as this allows for proper treatment, limitation of further spread (e.g. quarantine) and monitoring the disease impact over time [4,5]. This is especially important when there are no vaccines available.
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     <h3>The development of a new diagnostic test  </h3> </div>
 
     <h3>The development of a new diagnostic test  </h3> </div>
 
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                             <p>The development of an adequate diagnostic can be challenging as many aspects are required. This is especially difficult for point-of-care diagnostic tests. These tests are used in low resource areas such as tropical areas. As a guideline, the WHO has postulated the ASSURED criteria, highlighting the most important aspects. A diagnostic test should be Affordable, Sensitive, Specific, User-friendly, Rapid and robust, Equipment-free, and Deliverable to end-users [4].
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                             <p>The development of an adequate diagnostic can be challenging as many aspects are required. This is especially difficult for point-of-care diagnostic tests. These tests are used in low resource areas such as tropical areas. As a guideline, the WHO has postulated the ASSURED criteria, highlighting the most important aspects. A diagnostic test should be Affordable, Sensitive, Specific, User-friendly, Rapid and Robust, Equipment-free, and Deliverable to end-users [4].
 
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     <h4>Current diagnostics: Antibody detection tests  </h4> </div>
 
     <h4>Current diagnostics: Antibody detection tests  </h4> </div>
 
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                           <p>Diagnostic tests that detect antibodies against diseases in blood samples are widely used in the field as point-of-care diagnostics. These include antibody dipsticks and agglutination tests. These tests are easy to handle and fast but have several drawbacks. Since antibodies are present in the body even after an infection has been fend off, these tests cannot distinguish between current and past infections. Moreover, due to cross-reactivity (antibodies that can bind to multiple diseases), false-positive results are periodically observed [6]. For example, the Card Agglutination Test (CATT) for HAT. This test is small, fast and high throughput, but it needs refrigeration, electricity and it lacks specificity. Moreover, these serological screening tests yield 99 false positives for every true positive, meaning many people are unnecessarily sent to the hospital for further investigation [7]. In dipstick tests, there is no positive control available. A negative result might mean no infection or an incorrectly working test. We learned this from dr. Philippe Büscher, HAT expert at the Institute of Tropical Medicine of Antwerp.
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                           <p>Diagnostic tests that detect antibodies against diseases in blood samples are widely used in the field as point-of-care diagnostics. These include antibody dipsticks and agglutination tests. These tests are easy to handle and fast but have several drawbacks. Since antibodies are present in the body even after an infection has been fended off, these tests cannot distinguish between current and past infections. Moreover, due to cross-reactivity (antibodies that can bind to multiple disease markers), false-positive results are periodically observed [6]. For example, the Card Agglutination Test (CATT) for HAT. This test is small, fast and high throughput, but it needs refrigeration, electricity and it lacks specificity. Moreover, these serological screening tests yield 99 false positives for every true positive, meaning many people are unnecessarily sent to the hospital for further investigation [7]. In dipstick tests, there is no positive control available. A negative result might mean no infection or an incorrectly working test. We learned this from dr. Philippe Büscher, HAT expert at the Institute of Tropical Medicine of Antwerp.
 
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<p>We use synthetic biology to create Mantis: a point-of-care diagnostic device that can detect disease antigens in blood samples. This whole-cell system can detect the pathogen, after which it emits a fluorescent signal. Below we discuss how Mantis improves upon current diagnostics. By providing a better ASSURED diagnostic, we not only help the population by lowering casualties and economic losses, but also enable the local community to protect themselves from infectious diseases, without being dependent on the help of foreign countries or institutes.
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<p>We use synthetic biology to create Mantis: a point-of-care diagnostic device that can detect disease antigens in blood samples. This whole-cell system can detect the pathogen, after which it emits a fluorescent signal. Below we discuss how Mantis improves upon current diagnostics. By providing a better ASSURED diagnostic, we do not only help the population by lowering casualties and economic losses, but also enable the local community to protect themselves from infectious diseases, without being dependent on the help of foreign countries or institutes.
 
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     <h4>Surveillance of current outbreaks  </h4> </div>
 
     <h4>Surveillance of current outbreaks  </h4> </div>
 
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                           <p>Human African Trypanosomisis (HAT) is an infectious diseases caused by the parasitic protozoan <i>Trypanosoma brucei</i> and is transferred via the bite of the Tsetse fly [9]. It is one of many neglected tropical diseases; a disease common in (sub)tropical third world countries with a lack of funding to control the epidemics [10]. HAT is, and has been, endemic in many African countries since the beginning of the 20th century. Although great efforts have been taken to contain the disease, resulting in a decline of new cases in the last decade, it was estimated that currently still over 70 million people in the sub-Saharan region in Africa are at risk of getting the disease [11]. The symptoms start with general infection symptoms, like headaches, fever and pain, but progress further to neurological disorders like a sleeping disorder, sensory disturbances and ultimately seizures, coma and death [10].
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                           <p>Human African Trypanosomisis (HAT) is an infectious diseases caused by the parasitic protozoan <i>Trypanosoma brucei</i> and is transferred via the bite of the tsetse fly [9]. It is one of many neglected tropical diseases; a disease common in (sub)tropical third world countries with a lack of funding to control the epidemics [10]. HAT is, and has been, endemic in many African countries since the beginning of the 20th century. Although great efforts have been taken to contain the disease, resulting in a decline of new cases in the last decade, it was estimated that currently still over 70 million people in the sub-Saharan region in Africa are at risk of getting the disease [11]. The symptoms start with general infection symptoms, like headaches, fever and pain, but progress further to neurological disorders like a sleeping disorder, sensory disturbances and ultimately seizures, coma and death [10].
 
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<p>While the WHO targets HAT for elimination by 2020, there is still a great need for the development of a new, point-of-care test for both screening and surveillance [10, 12, 13, 14]. Since HAT is a neglected tropical infectious disease with a long history, we take it as a proof-of-principle for our diagnostic device to be applied to parasitic infections.</p>
 
<p>While the WHO targets HAT for elimination by 2020, there is still a great need for the development of a new, point-of-care test for both screening and surveillance [10, 12, 13, 14]. Since HAT is a neglected tropical infectious disease with a long history, we take it as a proof-of-principle for our diagnostic device to be applied to parasitic infections.</p>
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                           <p>HAT is transmitted by the Tsetse fly. In order to reduce the spread of the disease, surveillance of vector populations can be valuable. Moreover, the other form of HAT, caused by <i>Trypanosoma brucei rhodesiense</i>, is difficult to eliminate not only by the lack of available screening kits, but even more by the vast amount of animal reservoirs which serve as an intermediate for disease transmission. A key part to control <i>T. b. rhodesiense</i> HAT is the monitoring of the domestic reservoirs infected by the parasite, as well as reduction of the Tsetse fly population [17]. For viral diseases, like Zika and chikungunya, vector control is also a very important factor, since these diseases are transmitted by mosquitoes. Since the Mantis device is equipped with GPS data storage, it would be suitable for vector monitoring and spread. However, we found out that a modular tool like Mantis is not the top priority within vector control, hence we decided to focus our project on human screening. You can read why on our <a href="https://2017.igem.org/Team:Wageningen_UR/HP/Gold_Integrated" target="_blank"> Integrated Human Practices page</a>.</p>
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                           <p>HAT is transmitted by the tsetse fly. In order to reduce the spread of the disease, surveillance of vector populations can be valuable. Moreover, the other form of HAT, caused by <i>Trypanosoma brucei rhodesiense</i>, is difficult to eliminate not only by the lack of available screening kits, but even more by the vast amount of animal reservoirs which serve as an intermediate for disease transmission. A key part to control <i>T. b. rhodesiense</i> HAT is the monitoring of the domestic reservoirs infected by the parasite, as well as reduction of the tsetse fly population [17]. For viral diseases, like Zika and chikungunya, vector control is also a very important factor, since these diseases are transmitted by mosquitoes. Since the Mantis device is equipped with GPS data storage, it would be suitable for vector monitoring and spread. However, we found out that a modular tool like Mantis is not the top priority within vector control, hence we decided to focus our project on human screening. You can read why on our <a href="https://2017.igem.org/Team:Wageningen_UR/HP/Gold_Integrated" target="_blank"> Integrated Human Practices page</a>.</p>
 
   
 
   
 
 
 
 

Revision as of 17:49, 30 October 2017