Monday, June 3, 2019
Rotating Wall Vessel Bioreactor
Rotating W squ be Vessel BioreactorAbstractRecently there be signifi finisht step of research work undergoing about compel from raw stuff engineering science science and bioreactor designing. Therefore, there argon so may research paper published around the world. It may enjoyment embryonic base of operations cubicle, mesenchymal bag cubicle, meander graft or other animal spaces tissues or carrel for civilizement of human and animal medicine treatment. In that case there should be any(prenominal) ethics and laws to control the usage of the tissue or stall in the medical treatment. Some government organizations and hole-and-corner(a) sector by independently or by joining do some research work about the tissue engineering and bioreactor designing. The cardiovascular constitution is the major disease problem in the human and animal medicine treatment. In recent decade there are cellphone and tissue engineering and the bioreactor designing involving treating the car diovascular disease educate. Researchers may try to develop marrow valve, wall and blood vas etc. Hole in the warmheartedness is labyrinthian congenital heart diseases, in new born babies and leading causes of mortality. The treatment of this kind of the cardiovascular disease yet performed surgery correction, the real painful by and by the surgery at tolerate by baby. When correcting the hole, that must(prenominal) draw closed priggishly otherwise it lead to another problem to the young one, but amount of the diameter of the hole is very(prenominal) difficult and correction also very difficult. In the recent decade there is stem cell therapy and the tissue engineering has rapidly demonstrable. By utilize stem cell and tissue finishing there are so m both researches and development of the treatment about cardiovascular system. Myocardial tissue engineering actual the heart tissue by using the stem cells in trey-dimensional matrices of biodegradable polymers sustai n is the innovation of the myocardial constructs and cardiovascular treatment.IntroductionThe heart is the most important organs in the human body. It transports blood to the organs, tissues, and cells of the body. Blood delivers oxygen and nutritiouss to every cell and removes the carbon dioxide and negate crossings excreted by those cells. A Holes in the Heart is an opening in the septum amid atria or ventricles of heart, this is congenital condition. 8-10/1000 live born babies has congenital defects in the heart. This condition occurred during the babys heart does not develop inside the womb no specific cause for this condition, but some increase risk of being born. If mother had German measles or toxoplasmosis during pregnancy, or if she has diabetes, or if someone else in her family was born with a heart complaint. A hole in the heart may be give awayd in the first few months of life or even before the baby is born, sometimes a hole is not found until a person is much old er. This often happens when the hole is between the upper chambers of heart. It may notice person are feeling a bit short- channel of breath and dont know why. But sometimes there are no complaints at all. Because of the hole, the lead of blood through the heart is abnormal. This crystallises noises in the heart, so a bear on can find the hole by listening to the heart with a stethoscope. If the doctor hears a murmur, this tells the doctor there could be a hole. If the doctor thinks there is a hole, person exit need an echocardiogram ultrasound test of heart. Sometimes the hole isnt found until a person is much older when they notice they are feeling tired and breathless and cant find a reason for it. Some holes are so small that they cause no problem and are left altogether. Some holes in small babies may close by themselves if the heart surgeon thinks this is wish wellly, he al junior-gradeer-ranking not close it immediately, but arrest for some time to see if it has c losed by itself, by repeating an echo. Other holes must be closed, either because they are already a problem, or because they leave alone cause a problem in the future.There are three different typesAtrial Septal Defect (ASD) this is a hole in the wall between the atria (interatrial septum). This causes more blood to flow to the lungs and may not have any symptoms the excess flow can damage the lungs. If the hole is small, and doesnt presume the function of heart, theres no need to reinstate it.Ventricular Septal Defect (VSD) this is a hole in the interventricular septum or wall between two reject chambers (RV and LV). If its large, can change the mechanics in heart. This makes the heart work harder than it should and can enlarge it. If the hole is small, and doesnt affect the function of heart, theres no need to fix it.Atrioventricular Septal Defect this is a large hole in the middle of heart between the atria and ventricles. Some people with this condition only have one valve between the atria and ventricles instead of two. This defect can also damage the lungs by allowing too much blood to flow to the lungs. Although this condition is uncommon, t can be found in babies born with Downs syndrome.VSDs are the commonest lesion about 25-30% of all congenital heart defects whereas ASD are about 5-8% of them. Another point to remember is that all of us are born with small ASD. However, VSD is never found in normal heart. The only treatment availablewas surgical closure. Though the ultimate out off tick was good, these children had to inevitably suffer the pain, scar and long hospital stay. There are two ways to do this. The first way is via an operation called catheterisation. This is when a cardiologist puts a tube into leg that goes up towards heart. Then put a device through that tube so that it fits into the hole. When its in the right place, the device opens equal a little umbrella, and blocks the hole. The device stays inside forever. This is not poss ible, because of the size, shape or position of the hole. In these more complicated situations, a surgeon will perform an operation where he puts a patch over the hole directly. If holes have between the two pump chambers of the heart that stay open, will need antibiotic treatment at certain times. This might be before having other operations or serious treatment at the dentist. some perseverings who have ASD/VSD corrections go on to lead perfectly normal lives. Person will be followed-up for a short period, but if everythings OK after a year, wont need to worry about it ever again. It also doesnt increase the chances of having any other heart-related issues in the future but should take secureness exercise and aim for a healthy diet. After correction of the hole in the heart there are low risk for structural degeneration, thrombo-embolism and endocarditis and growth latent for paediatric patient. From 1970s onwards, a group of cardiologists started thinking differently. They exp erimented on animals by creating holes in their hearts and then tried closing them without surgery. Gradually they replicated the whole procedure on humans. For the last twenty years, nonsurgical closure or device closure has been the normal.Adult life heart muscle cells do not proliferate, if there is damage or injuries happened to the heart, functional tissue try to form the non-functional scar tissue. In 1996, 98 Klug et al. Suggest that development of human Embryonic stem cell derived cardiomyocytes help for therapy of cardiac disease.There are some experiments done by using stem cells. Stem cells are the cell ability for self-renewal and the potential for differentiating into senesce cell types. The embryonic stem cells can give rise to almost every mature cell type, while adult stem cells are classified as restricted to differentiation into only few types of mature cells. The mesenchymal stem cell can only differentiate to one specific mature cell type, are referred to as pre cursor cells. First clinical applications of stem cells for cardiac regeneration comprised cell transplantation trials. These trials were less successful than promising preclinical studies these efforts initiated intense research activities providing new insight into the mechanisms of tissue growth and differentiation. Cardiac tissue engineering is focused on three different organ subunits the myocardium, valves, and vessels. These three compounds of the heart can already be replaced by artificial or biological transplant constructs with their respective limitations, like assist devices, commercial heart valves, autologous coronary bypasses, etc. When growing the heart tissue must contemplate produced cardiomyocytes, vascular endothelial cell and the smooth muscles cell. Engineering these tissues must compete with the durability, expertness and safety of existing substitutes and be affordable at the same time. Tissue engineering is the development of biological substitutes that restore, maintain, or improve tissue function or a whole organ, includes an in vitro.During designing of bioreactor, physiochemical environs maintain is very impotent, that will help to kept high school quality of the stem cells and high percentage point of reproducibility of the cells. But must make sure cell culture has developed under sterile environment and sufficient nutrition and waste product exchange throughout the medium and clean and maintain the medium. After that, design some mechanical and hydrodynamic force to compression or expansion of the developing tissue, like rob stress to the tissue. Then maintain steady flow of media in pulsatile manner and reduce the excessive turbulence in the fluid flow rate. Other than that, must provide the low volume capacity for effective use for growth factors and medium, also select the fabricate material compatible with the heart tissue or stem cell. The bioreactor designing for heart tissue development must determine some specifi c design and functional requirement. Both biomechanical and biochemical factors affect the growth of the cell therefore essential to create some control mechanism by stimulate the physiological environment for heart cell growth, like pulsatile forces, pressure, flow rate, compression, expansion, shear stress, frequency, stroke rate and stroke volume. Other than that, when creating heart tissue must consider cardiac flow rate and pressure. When consider the design the bioreactor, there are nutrition, oxygen, carbon dioxide, waste product, pH, temperature and humidity are main important biochemical controls affect the growth of the cell. There than the flow rate, volume, shear stress, pressure, resistance and compliance like biomechanical controls also involved in the cell growth. Therefore, specific bioreactors are need for the growth of the stem cell. Because inside the body, cells are incessantly stimulated by mechanical, electrical and chemical signals, these influencing their be haviour. In fact, biological tissues adapt their structure and composition to surrounding specific and functional demands. By putting cells alone or only in contact with materials in culture medium is not enough to obtain a functional tissue. In vivo, the heart valves are subject to a unique combination of mechanical stimuli, including flexure, shear stress, and tension (Vesely and Boughner 1989). In growth of the embryonic stem cells require temperature, partial(p) pressure of oxygen, partial pressure of carbon dioxide, pH, and shear force and biochemical conditions of their micro- and macro-environment. Then try to find homogeneous and changeless conditions for micro- and macro-environment for the entire cells population. By uneven cell distribution, leave out of nutrition and oxygen and insufficient extracellular matrix production cause some limitation to bioreactor scaffold in stem cell culture. Therefore, get unloosen of those must make to stem cell onto polymers, which wil l increase the mechanical strength of the heart tissue construction and develop subsequent tissue formation.To develop a bioreactor to provide cyclic flexural stimulation, to demonstrate the operation of the bioreactor and sterility maintenance and to evaluate the effects of unidirectional flexure on the effective stiffness of bioresorbable polymeric scaffolds which have been used extensively in the tissue engineering of the heart tissue. Therefore, must design the devices for closed controlled environment in which biological and/or biochemical attendes are developed maintained pH, temperature, pressure, nutrient supply and waste removal, with high degree of reproducibility of the heart valve. Therefore, bioreactors are particularly crucial for the regeneration of intricate 3D tissues. The bioreactor was designed using 3D software. The structural element of the device was machined from polysulfone chosen for its excellent thermal and chemical stability and abrasion-resistant acry lic which provides good opthalmic transparency. Culture medium was Dulbeccos Modified Eagles Medium with 4.5 g/L glucose and L-glutamine supplemented with 10% fetal bovine serum. Antibiotics were excluded to assess the intrinsic ability of the bioreactor to maintain sterility. When developing scaffold use the degradable material and permanent materials as in artificial implants and in use of cells. Then preparing scaffold must test in vitro and in vivo how they hypotheses of scaffold and cell interaction, scaffold effect on tissue growth and 3D environment effect on stem cell differentiation. Scaffold materials consisted of a non-woven profits of polyglycolic acid(PGA) fibers dip-coated with poly-4-hydroxybutyrate (P4HB), and a non- woven, 5050 blend, mesh of PGA and poly-L-lactic acid (PLLA) fibers dip-coated with P4HB. The PGA and PGA/PLLa scaffold had an approximate fiber diameter of 0.012-0.015 mm and density of 69mg/ml. Rectangular scaffold sample were delete to size (approxi mately 257.5x2mm) and dipped briefly into a solution of P4HB in tetrahydrofuran (1% wt/vol), resulting in a P4HB coating following solvent evaporation. P4HB is a bioresorbable thermoplastic that allows for scaffold to be moulded into any shape. Scaffold were cold gas sterilized with ethylene oxide prior to use.The use of bioreactors, chambers which provide the flow of nutrient media for the development and culture of heart valves construct, to provide an environment which as closely as possible mimics the natural in vivo conditions. These bioreactors have been designed for pulsatile flow, driven by a pulsatile pump, which leads to the exertion of only a positive pressure. This is not the case in vivo, as during the cardiac cycle the positive pressure exerted by fluid force is slightly counterbalanced by a little vacuum. Stem cells grow in vitro under bioreactor conditions must provide the nutrient and they produced the nitrogen contain waste product, but they refined to the nitroge nated waste product. This will be varying with the tissue and that will change the shear stresses effecting on the tissue. The oxygen pressure is maintained at set unending value with calculated volume of solution added every time to the medium. Other way round maintained the carbon dioxide pressure at set constant value with calculated volume of waste product upstage from the medium. Oxygen is most important nutrients for cells in all aerobic metabolic cycles. It is the limiting nutrient in successful tissue growth in vitro, sufficient amounts of oxygen to the surface of the cells mainly because of the poor solubility of oxygen in culture media. In that case hypo-oxygen or hyper-oxygen stresses will be concern the stem cell culture causes of programmed cell death or apoptosis. Therefore, coordinate the stem cell for the anaerobiotic cell metabolism with low oxygen tension (40 mmHg) and low pH or for aerobic cell metabolism with higher oxygen tension (80mmHg) and high pH. Then li ving tissue is sensitive to pH changes in the medium, during maintain of the oxygen level must maintain the pH also. Other than that glucose and lactate are providing to cell metabolic process. Therefore, they act as the indicator for cells activity.In the bioreactor environment stem cell proliferates and increased the mass that leads the limitation of the final size of the tissue grow. Other than that, there are spaces to pass oxygen and nutrient throughout the scaffold otherwise this also leads to limitation of the tissue growth. Therefore, bioreactor must design to proper diffusion of oxygen and the nutrient and mass proliferation cell will survive and proliferate within 150-200m distance.Shear stress will affect the tissue culture growth, most of the stem cell responds to it. They are proliferating according the orientation of the flow direction. In that case stem cell can aggregates by using higher shear stress that can be used for tissue function and viability. If design the r otating bioreactor that can decrease the shear stress and avoids the contact between the cells and the wall of the bioreactor, chamber must permanently rotate with one direction and control to forming uniformed growth of the tissue. But if design the non-rotating bioreactor then must create the specific mechanical stress applied on the cell culture, by perfusion solution can passed through the cell tissues by flow through the culture chamber. Some experiments were demonstrated that the shears stress 0.1 dyn/cm2 was ideal for stem cell to growth. If that exceeds the shears stress 1 dyn/cm2 were damaged the cells and the shears 0.01 dyn/cm2 were insufficient to promote the growth.Bioreactors have developed functional heart tissue in vitro environment over specific biochemical and physical signals known to regulate cell differentiation, by up(p) the formation of the heart tissue by proving uniformed mixing pattern, transported the nutrient to enhance the cell growth and hydrodynamic or mechanical stimulation for stem cell to develop. Simple passive flasks or a magnetically stirred flask is not suitable environment for 3-dimensional heart tissue scaffolds to develop. To develop the terminal possible homogeneous cell number for heart tissue, must grow the cell with uniform and efficient of porous scaffolds. When compare the cells seeding into mixed petri dishes yield with the static loading of the cell into the scaffolds has thicker constructs and more spatially uniformed distribution of cells. By seeding in rotating vessels or mixed flask must maintain a uniformed suspension of isolated cells and provide a relative velocity between cells and the scaffold during seeding. Dynamic seeding using mixed flasks will show to achieve seeding efficiencies draw near 100% but led to cell densities higher at the scaffold periphery. Therefore, when design bioreactor must provide the scaffold perfusion with a cell suspension in alternate directions, which lead to the more h omogenous seeding on a variety of scaffold with potential yield. Once the cells are associated with the scaffold, cell-polymer constructs can be cultured in bioreactors applying specific regimes of fluid flow.Selecting rotation wall vessels bioreactorThe bioreactors are used for proliferation of cells on a small or large scale, to generate 3D tissue constructs, a certain process must occur. That case the cells are proliferated in a bioreactor to provide the quantity of cells needed. The cell loses their specialized characteristics during the process of proliferation is the problem. Therefore, microcarrier culture used for improves cell expansion significantly and that mixed the bioreactor system well. After the cell proliferation they must associate with enhanced heart tissue formation. In above process cells must receive proper nutrition and a stable environment. There for controlled the temperature, optimum pH, sufficient substrate, water, salts, vitamins, and oxygen. The Rotating -wall vessel culture is the best bioreactor for culturing constructs stained intensely, and homogeneously for scaffold for their cross-section(a) area. Inside the bioreactor a dynamic flow generated by a rotating fluid environment is an alternative and efficient way to reduce diffusion limitations of nutrients and wastes. The rotation produced the low level of the shear stress to the cells, creating mechanical stimulation. Other than that, there are other mechanical forces that affect the cells during growth, like mechanical compression, hydrodynamic pressure, and fluid flow. They will affect the magnitude, frequency, and duty of the bioreactor cycle.To control the free-falling state adjusted the rotation speed, it protects the fragile tissue by decreasing the shear stress and avoiding the contact between cells and the walls of the bioreactor. During nineties NASA scientist did some research about the microgravity involved in to the cell tissue of the mammals. They used the closed tubular cylinder forms the systems cell culture chamber, which filled with a liquid medium where the cell grows on micron-size beads. The chamber has rotated along the horizontal axis in that case they allowed the cell to develop in an environment like the free fall of microgravity. They supply oxygen and nutrition through a porous wall in the chamber, as same way they removed the waste product and the carbon dioxide. The rotating wall vessel bioreactor is providing the conditions of weightlessness for microbes by growing them inside of a slow downly rotating liquid-filled chamber. The process of the rotation liquid has counteracted with slow sedimentation of the cell by creating a constant free fall of the cells through the culture medium. While rotation cell gets a slight issue stress from liquid, lead to avoid the flattened on the bottom of the container. The scientist used the clear shell for allowed to check growth and cylindrical filter holds on the reduce for supply the ox ygen and nutrition and removed the carbon dioxide and waste products. And, they insure the fluid rotation without shear stress would leads to destroy the cells. They noticed rotation vessels did not cancelled the gravity, but that maintain the cells in continual free fall environment inside the shell.Bioreactors for the application of physical forces to engineered cartilage tissues. In the rotating wall vessel system (A), the rotational speed is adjusted so that the drag force of the medium (Fd) is balanced by the centrifugal (Fc) and gravitational (Fg) forces. The constructs are thus maintained in a tumble-slide regime and the resulting dynamic laminar flow enhances the production and accumulation of cartilaginous extracellular matrix. Specific culture chambers (B) have been developed for the application of direct deformation to engineered constructs. Chambers include wells to allocate tissue constructs (I), a magnetic bar for medium stirring (II), an inlet/ takings port for medium change (III), a cover lid to maintain sterility (IV), and micrometer screws to accurately establish the contact position between the plungers and from each one specimen (V).The cell seeding is effects of shaking speed and initial cell concentration in suspension on cell culture medium, therefore cell seeding must do in efficiency. In that case initial seeding density and cell distribution within the scaffolds must understand. Initially cell concentration is low, in that time seeding efficiency and initial density will decreased with increasing shaking speed. But high initial cell concentration that will end the result. All the different cell concentration uniformity of the cell distribution decreased with increased shaking speed. But under the same shaking volume were observed with on significant differences in uniformity between cells with different initial concentration. In vitro the tissue engineering of heart tissue structures is to develop combine cell seeding and perfusio n system. Cell seeding is consisting of whole system, that incorporated into the perfusion system and air-driven respirator pump connected to the bioreactor. Therefore, cell culture medium is closed-loop system that will continuously circulate. Therefore, scientist developed a cell seeding device for static and dynamic seeding of vascular cells onto a polymeric vascular scaffold and a closed-loop perfuse bioreactor for long term vascular conditioning. By using cell seeding chamber can be easily connected to the bioreactor, which have combines continuous pulsatile perfusion and mechanical stimulation to the tissue -engineered conduct. In that scientist adjust the stroke volume, the stroke rate, and inspiration/ expiration time of the ventilator allow various pulstile flows and different levels of pressure.DiscussionWhen selecting of the scaffold consider the biocompatibility, reproducibility, biodegradability, ability to be refined to complex shapes, ability to support cell growth an d proliferation and mechanical properties of materials. Other than that, scaffolds must have similar electrical and functional activity with create systolic force. The limited availability of the incubator space the place where the multiple bioreactors place, in this space multiple bioreactors must be places. Development of the stem cell is temperature depended process, any cells grow at body temperature in optimal level therefore temperature must maintain in that level as possible. The bioreactor design must set the temperature parameter to monitor the temperature. If inside temperature changes by increased or decreased then that must alarm on, then it can adjust manually.Sterility is very important throughout the development of the heart tissue. We used flask and glass vessels with threaded fitting, which is cheap and proved to maintain perfect sterility. To reduce the risk of contamination, make sure all connections before sterilisation and sterilize bottles with correction solut ions connected to the vessel, by using either alcohol or stem. The tubing can be placed into the pump head easily after the sterilization. Because contamination of the medium lead to the growth of the heart tissue. Therefore, bioreactor must develop as a semi-closed system. book the small cell culture medium all the time, easy replace the balance amount of the cell culture medium for requirement created by cell seeded as soon as possible. If require in addition to that easy seeding of the additional cells. Maintain the oxygen level in the medium is very essential therefore, reassure the amount of the oxygen in the medium is enough for the development of the stem cells. When we maintain the pH level in the medium that passively adjust oxygen level in the medium, by enrich the medium with CO2 level up to 5%. The biocompatible substances must use when the designing process of the bioreactor, those substance will not kill the stem cell during the tissue growth. There are many analytic p arameters, those must monitor regularly with some sensory methods to alarm if there are any changes occur in the media and correct it manually. Any design bioreactor can have ability to experiment several(prenominal) times with longer period. If there are any alternations, like change the cell culture medium with ingredients needed or changer scaffold materials change those and can perform the process easily. By using roller pump can sucks the cell culture medium from the bioreactor, which leads to stress of the scaffold. This help to stem cell growth towards the heart tissue.This bioreactor must use inside the hospital, for treat each of the hole in the heart patient therefore this must produce low cost heart tissue for the patient. Other than that, there should be very low laboratory involvement and convince for patient and the surgeon. When using this kind of tissue engineering think some social highlight that affect the both quality and quantity of the life. Some religious backg round this technology is some pitiful for the life, ethical concern there are some extent to do those kinds of experiment. But medical point of view this is the good solution for treatment of the patient without suffering. In that case be careful of handling with stem cell and other, that will lead to caused critical threat to handler.ConclusionsThe developed bioreactor has set sterility at least week, with working tool for conducting experiments regarding heart tissue growth. The growth of the heart tissue helps to develop entire heart, which can helpful to many heart diseases. pabulum concentration must keep in mind when performing the bioreactor process. When the time of the replacing the medium nutrition concentration must maintain, also try to asperse the number of time replacement the medium.AcknowledgmentI would like to thank Professor Alicia El Haj, Dr. Nicholas R. Forsyth and Dr. Ying Yang for their support and guidance in completing this study.I would like to special th ank Dr. Sun Tao for his support and guidance in completing this study.
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