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Mathematics for Biologists 19.11.99 1 Mathematics for Biologists Part Biology Morphometric - Stereologic Analyses of Lung Tissues Protocol Jan. 31st 1998 Headed by: Dr. Sänger Handed in by: Maricela Yip (Mat-#: 9424495) Salzburg, January 31st 1998 1 biophysics.sbg.ac.at/home.htm Mathematics for Biologists 19.11.99 2 Morphologic-stereologic investigation of epithelial cilia cell, macrophage cell and alveoli in human lungs: Introduction: The lung’s main function is to allow for efficient exchange of gases (O2 and CO2) between the surrounding air and the blood. For this purpose the air is led through the bronchi into a large volume made up of many small chambers, the alveoli. Similarly blood flows through arteries into a dense capillary network which is contained in the alveolar walls and is then collected and conducted back to the heart by veins. Respiratory passages: When a mammal breaths in, air enters the respiratory system through the mouth or nose. The air is warmed and humidified by the moist mouth or the nasal cavity which are located posteriorly to the pharynx. The pharynx branches into a pair of tubes; one the esophagus, leads to the stomach, while the other, the wind pipe, or trachea, is the air-way leading to the lungs. At the anterior end of the trachea, lies the larynx, housing the vocal cords. Just above the opening to the larynx, is a flap of tissues called the epiglottis, which normally closes off the larynx during swallowing and thus prevents food from accidentally entering the lungs. Ventilation of lungs is brought about passively by the intercostal muscle of the ribcage, which is connected via the pleura and pleural cavity and the diaphragm. Lungs: The trachea branches into two hollow passage ways called bronchi, each of which enters a lung. Finer and finer branchings of these tubes create an inverted tree, with thousands of narrow airways, or bronchioles, that eventually leads to millions of tiny, bubble-shaped, sacs, called alveoli. It is in the alveoli, that gas-exchange takes place. The terminal bronchioles, the respiratory bronchioles, the alveolar ducts, and the alveolar sacs, constitute the respiratory portion of the lungs. Many of the cells that line the larger airways produce a sticky mucus ideally suited to the capturing inhaled dirt-particles or microorganisms. This mucus is continuously cleared from the bronchi by the beating of cilia, which sweep the mucus and any trapped debris up toward the pharynx, where they can be swallowed or expelled. 2 Mathematics for Biologists 19.11.99 3 Alveolus: (L. small cavity) Gases are transferred across the thin-walled alveoli found in the region distal to the terminal bronchioles, termed acini. The airways leading to the terminal bronchiole constitute the non-respiratory portion of the lungs. Alveoli in a joining acini are interconnected by a series of holes, the pores of kohn, allowing the collateral movement of air, which may be a significant factor in gas distribution during lung ventilation. Each alveolus is surrounded by blood capillaries, and the inside of each tiny pouch is lined with a moist layer or epithelial cells. At those places where the wall of a capillary lies near the outer wall of an alveolus, O2 easily diffuses out of the alveolus and into red blood cells squeezing down the center of the narrow capillary. Meanwhile, CO2 leaves the blood, diffusing out of the capillary and entering the alveolus. From the alveolus, it is expelled to the outside with the next exhalation. The lung-wall tension depends on the properties of the alveolar wall and the surface tension at the liquid-air interface. The explanation for the relatively low surface tension of the liquid lining the lungs is the presence of surfactant, lipo-protein complexes that bestow a very low surface tension in the liquid-air interface. Lung surfactant not only reduce the effort associated with breathing but also help prevent alveoli from collapsing. Finally a few words about the tabacco plant itself: Tobacco (Nicotiana tabacum) is a hardy C3 plant that grows up to 2m tall and produces very large leaves and spikes of pretty, usually pink, flowers. As a natural defense, tobacco leaves and stems produce various compounds that discourage insects and other predators. Among them is a bitter-tasting nitrogen-containing compound, an alkaloid called nicotine. The cigarettes, cigars, pipe and chewing tobacco made from the tobacco plant seem to be addictive. This is because the nicotine in tobacco leaves causes a strong psychologically dependence on the taste and feel of tobacco. Besides that, analysis of smoke from burning tobacco has shown to contain over 4000 separate compounds, including DDT, arsenic, nitrosamines, and formaldehyde, all known carcinogens. Similar tests of chewing tobacco reveals traces of three additional carcinogens: cadmium, uranium, polonium. One of the most damaging compounds in tobacco smoke remains as the poisonous gas carbon monoxide (CO). 3 Mathematics for Biologists 19.11.99 4 Effects of tabacco smoke in human cells: Paralyzed Cilia: Tobacco smoke can paralyze the cilia, the microscopic hairlike projections from cells lining the airways of the human respiratory tract. Without these continuously beating cilia, germs and particles of foreign matter can enter the lungs and cause irritation and infection. The lungs of a smoker and his respiratory passageways compensate by producing more mucus, which is expelled in a cough. Perennial coughing can weaken the lungs and lead to chronic bronchitis. Lung Cell Changes: Cadmium, nitrogen dioxide, and other substances in cigarette smoke can rupture cells in the lungs' tiny, ballonlike air sacs, or alveoli. They can also prevent a cell's smooth endoplasmic reticulum from producing normal amounts of surfactant. Both of these changes can contribute to permanent shortness of breath and to lung diseases such as emphysema. Disturbed Mitochondria: Smoke destroys the mitochondria's normal internal structure, and with it, their ability to carry out the reactions of the Krebs cycle (an elementary process in cell respiration) and the electron transport chain. Thus the cell is starved for ATP (energy carrier within the cell) energy and eventually dies. DNA Damage: Many of the toxic compounds in tobacco can attack and damage DNA. Repair enzymes in the nucleus attempt to fix these broken strands, and correct mismatched base pairs. However, continual exposure to the toxins can lead to an accumulation of errors, which are implicated in the formation of cancerous tumors. Nicotine and the Cell: Certain cells in the nervous and muscular system have receptor proteins in their membranes that bind with nicotine, causing a different cell response to normal nerve signals, explaining how nicotine acts as a stimulant. Increased Carbon Monoxide: Smokers have elevated CO levels in their bloodstream. When CO combines with hemoglobin, the pigment delivers less oxygen to the body's tissues, including the brain, and the person's ability to think clearly is reduced. 4 Mathematics for Biologists 19.11.99 5 Immune Cell Changes: Researchers studying the white blood cells (macrophages) that patrol and protect the airways and lungs have found an increase in the size and numbers of lysosomes within the cells and a decrease in protein synthesis. The cells are apparently so busy ingesting foreign particles and the debris of damaged cells that they can't grow and function properly. Immune cell disruption helps explain why smokers catch colds, flu, and pneumonia more easily than nonsmokers, as well as experience increased cancer rates. Further Consequences of tobacco use: Tobacco users have lowered resistance to colds and flu, and slower healing of broken bones and other wounds. Female smokers tend to have more miscarriages and babies of lower birth weight. Even in their teens and twenties, tobacco users tend to develop periodontal (gum) disease four times as often as nonsmokers. A smoker’s lungs A non-smoker’s lungs 5 Mathematics for Biologists 19.11.99 6 1. Working Hypothesis: Statistical evidence show that smokers are more likely to suffer from respiratory diseases and premature death than nonsmokers. Morphologic-stereological approach should help to determine the following effects: Hair-like cilia: In a Nonsmokers lungs, the cilia protrude from the cells that line the trachea and bronchioles sweep mucus and debris from the respiratory passageways. In a smokers lungs, the cilia are paralyzed or broken by cigarette smoke. Debris can reach the lungs and accumulate, blackening and clogging the delicate tissues lining the alveoli. Stereological methods should show how the all over cilial-surface area is lower in smokers. Lung Cell Changes: Cadmium, nitrogen dioxide, and other substances in cigarette smoke can rupture cells in the lungs' tiny, ballonlike air sacs, or alveoli. They can also prevent a cell's smooth endoplasmic reticulum from producing normal amounts of surfactants which further deteriorates the alveolar walls. These changes can contribute to permanent shortness of breath and to lung diseases such as emphysema. Stereology will help us to show the loss of alveolar surface area of a smoker lungs versus a nonsmoker. Macrophage Cells: in white blood cells, lysosomes enlarge after smoking. Macrophages exposed to cigarette smoke do show significant changes, lysosomes of these immunodefencee cells can be used to show the modifications under stressed conditions; therefore, morphologic-stereological techniques can be used to prove this correlation? 2. Components of the Structures, needed for stereologic investigation The different components must be clearly separated and identifiable. Each parameter is obtained as the ratio of two measurements, one estimating the size of the objects of interest (phase), the other the size of the space in which they are contained (reference). Structure Ciliated epithelial cell vs Cilia Macrophage vs Lysosome Alveolar ducts vs alveolus Objects Reference: A ciliated epithelial cell represents a structural unit. Phase: Cilia, part of this structure, are the site of interest on which debris and smoked gas affects them, here as the phase. Reference: Macrophage is the direct immune defense organelle that ingest and digest undesired material and debris that enters along with air into the lungs, therefore considered to be the reference unit. Phase: Lysosome are contained in the macrophage, are small membrane bounded structures that contain a set of powerful hydrolytic enzymes, which are capable of breaking down most organic materials, so that the foreign body is quickly disassembled; i.e.: the phase. Reference: Alveolar ducts as the pulmonary gas exchanger consist of at least two alveoli of the same air duct system, hence, the reference. Phase: Alveolus is a thin-walled, sacklike chamber in the vertebrate lung where gas exchange takes place, the single structure within the unit. 6 Mathematics for Biologists 19.11.99 7 2.1. Determination of Parameters The quantitative description of the structure is the density of the various components within the structure (the quantity per unit volume). Structure: surface density X Hair cilia: in a 2-D, SEM picture, comparison of the size of the surface between a nonsmoker hair cilia with a smoker hair cilia reveals that a smoker’s epithelial cell is severely damaged compared to a nonsmoker’s cilial epithelium; i.e.: ”surface” is the criteria to look for. Lysosome: the size of the lysosome of a smoker is significantly larger than the nonsmoker’s; i.e.: the ”volumetric” content determines the effect. X Alveolus: in a smoker’s, the alveolar walls are almost lost, resulting in shortness of breath and death; i.e.: all over surface area determines efficiency in gas exchange. volume density X 2.2. Measuring Methods Since 2-D cuts obtained by a series of microtomial cuts do not reveal the actual 3-D structure, indirect census techniques like point, intersection, or number counting are used to rebuild the original structure (the parameter of interest). Structure: Hair cilia: irregular patches of surface area of the epithelial cell are better determined by counting the number of intersecting lines that falls into the irregular patches. Lysosome: the sizes of the lysosomes of the nonsmoker’s and the smoker’s can be easily determined by this method. Alveolus: the surface of alveolar walls can be easily determined by counting the intersections that fall into the air sacs of an alveolus. surface density intersection counting volume density point counting intersection counting 2.4. Testgrid The spatial distances between testlines should not exceed dimensions of objects of interest; i.e.: • Cilium: spatial distance between testlines should be the size of average cilial length; • Lysosome: spatial distance between testlines should be the average lysosomal size; • Alveolus: spatial distance between testlines should be the distance of alveolar walls. Structure Hair cilia: Damaged cilia are better determined with a finer testgrid, whereas intact cilia, with the coarse one; so that, we can see the difference between the two SEM pictures. Lysosome: Enlarged lysosomes in macrophages of smokers are determined by a coarse testgrid, whereas the finer is more suitable for the census of a non-smoker’s tissue. Alveolus: A short-lined testgrid is probably best to use because nonsmoker’s alveoli are far smaller (more walls in between them) than of a smoker’s (increase surface area per alveolus) due to the loss of alveolar walls. 7 Testgrid double square lattice double square lattice short-lined multipurpose testsystem (M168) Mathematics for Biologists 19.11.99 8 Healthy epithelial cilia Damaged epithelial cilia 8 Mathematics for Biologists 19.11.99 9 Loss of alveolar walls Normal alveolar walls References: • Stereological Methods Vol. 1, Ewald. R. Weibel, Academic Press London 1979, UK • Animal Physiology 4th ed., Eckert, W.H. Freeman and Company New York 1997, USA • The Nature of Life. 3rd ed., Postlethwait J.H., Hopson J.L, McGraw Hill, New York 1995, USA • Zoology, Robert L. Dorit, Warren F. Walker, Robert D. Barnes, Saunders College Publishing, Orlando 1991, USA • Medical Physiology, Ninth Edition, Arthur C. Guyton, John E. Hall, W.B.Saunders Company 1996, USA • Cell and Tissue Ultrastructure, Patricia C. Cross, K. Lynne Mercer, W.H.Freeman and Company 1993, USA • The pathway for oxygen, E. R. Weibel, Harvard University Press, 1984, USA 9