NURS N111F Week 2 Microbiology & Pharmacology (PDF)
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This document is a week 2 lecture from a microbiology and pharmacology course at Hong Kong Metropolitan University. It covers topics such as bacterial growth curve, factors affecting microbial growth, and methods of microbial control.
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NURS N111F Fundamentals of Microbiology and Pharmacology WEEK 2 Interaction between Microbes and Host Learning Outcomes for Week 2 On completion of this lecture, you will be able to: 1. Describe the bacterial growth curve; 2. Explain factors affecting bacterial gr...
NURS N111F Fundamentals of Microbiology and Pharmacology WEEK 2 Interaction between Microbes and Host Learning Outcomes for Week 2 On completion of this lecture, you will be able to: 1. Describe the bacterial growth curve; 2. Explain factors affecting bacterial growth; 3. Describe the terminology of controlling microbial growth; 4. Describe methods for controlling microbial growth; 5. Describe the interactions between microorganisms and human; and 6. Describe the mechanism of pathogenicity. 2 Interaction between Microbes & Host Part 1: Microbial Growth How microbes grow Methods measuring bacterial growth Factors affecting microbial growth [Factors favouring infection] Part 2: Control of microbial growth Terminologies Physical methods Chemical methods Part 3: Interactions between microbes & human Normal microbiota Pathogenic microbes Mechanism of pathogenicity [How bacteria (and other microorganisms) cause diseases] 3 PART 1: Microbial Growth https://www.youtube.com/watch?v=GX55_-IlfyI How microbes grow Methods measuring bacterial growth Factors affecting microbial growth 4 BINARY FISSION IN BACTERIA Bacterial Growth Bacterial growth = increase in number of cell NOT size Growth by: Under favourable environmental conditions Mcstrother, CC BY 3.0 https://creativecommons.org/licenses/by/3.0 Binary fission via Wikimedia Commons [bacteria] Budding [e.g. yeast, less common in bacteria] Under unfavourable environmental conditions Sporulation [Forming spores] Created with BioRender.com 5 Binary Fission Process by which 1 cell divides into 2 cells Grow exponentially 1 20 2 21 4 22 8 23 16 24 … … Generation time Duration required for doubling a population (~10 min to 48 hours) Different bacteria grow at different rates 6 Steps for Binary Fission English Wikipedia user ZabMilenko, CC BY-SA 3.0 http://creativecommons.org/licenses/by-sa/3.0/, via Wikimedia Commons 1. Cell elongates & DNA is replicated 2. Plasma membrane begins to constrict & new wall is made 3. Cross-wall forms, completely separating the 2 DNA copies 4. Cells separate Created with BioRender.com 7 Bacterial Growth Curve Noexchauge rf mateunals wren N suwnawings Bacterial growth in a close system (e.g. a culture flask) by binary fission follows the bacterial growth curve 1. Lag phase 2. Log phase (Exponential growth phase) 3. Stationary phase cronet ) increase 4. Death phase (Decline phase) Created with BioRender.com 8 Bacterial Growth Curve (cont’d) 1. Lag phase ( prebavation prase ) No obvious increase in population size (cell number) Bacteria are undergoing a period of intense metabolic activity Synthesize enzyme to prepare for cell division 2. Log phase (Exponential growth phase) Exponential increase in population size Number of newly divided cell > Number of dying cell veny Plenty of nutrient support, with relatively less competition steady Generation time can be calculated in this phase Fast grower has a steeper slope 3. Stationary phase 𝐺𝑟𝑜𝑤𝑡ℎ 𝑟𝑎𝑡𝑒 4. Death phase (Decline phase) 𝐶𝑒𝑙𝑙 𝑛𝑢𝑚𝑏𝑒𝑟 = 𝑇𝑖𝑚𝑒 9 「 Bacterial Growth Curve (cont’d) 1. Lag phase 2. Log phase (Exponential growth phase) competefor 3. Stationary phase space nutrents , Flat portion of the curve No net increase in cell number, but cells are still growing Number of newly divided cell = Number of dying cell metabolzc A period of equilibrium waste Approach the carrying capacity with accumulation of waste & space 4. Death phase (Decline phase) The population drops, with decrease in the number of living cells Number of newly divided cell < Number of dying cell Lack of nutrient support & accumulation of waste products 10 cunfovonroble condneion ) Bacteria -- Endospores [Sporulation] Usually in Gram +ve bacteria Form under adverse environmental condition (sporogenesis) e.g. Nutrient depletion, Bacterial Spore Formation Animation Video extreme temperature or pH https://www.youtube.com/watch?v=NAcowliknPs Can survive under extreme heat, lack of water, exposure to chemical and radiation Dormant state for bacteria Can re-grow under favourable conditions (germination) 11 Created with BioRender.com Method Measuring Bacterial Growth Ho m e Se a rc h Bo oks he lf Se tti Eb ook Cen tr al A. Direct measurement methods Counting the number of actual bacteria cells physically 1. Direct microscopic count (DMC) Counts bacterial cell number under microscope using cell counter ⑦ Textbook: Microbiology Fig. 6.20 2. Serial dilution and plate count method Counts the number of bacterial colony grown on agar plate (pronne nuynents) Calculate the bacterial number by multiplying with dilution factor B. Indirect measurement methods 성 췄쏟 밌포포니 Textbook: Microbiology Fig. 6.16 12 Method Measuring Bacterial Growth (cont’d) Turbrd clear A. Direct measurement methods tzbacterra B. Indirect measurement methods Not counting the actual number of bacteria, but the effect of bacteria cells on the physical properties of the culture medium (e.g. turbidity) Turbidity estimation of bacteria number Bacterial growth in liquid culture broth turns the solution turbid (cloudy) 며 없 □ Textbook: Microbiology Fig. 6.21 Bacteria (live or dead) in the liquid scatter the light passing through ^ A spectrophotometer is an instrument for measuring turbidity (spectrophotometry) ) Turbidity is measured in terms of absorbance (A) or optical density (OD) measures laght More cells More scattering pass through the Less light being transmitted High Absorbance specimen 13 Factor Affecting Microbial Growth Physical Requirements: Temperature pH Osmotic pressure Chemical Requirements: Carbon Nitrogen Phosphorus Sulphur Trace elements Oxygen ) fon bacterra togrow Toxncsusstanceinher bacternal groamen 14 Physical Requirement -- Temperature bulish cow meta. Different microorganisms have different requirement for corspeea Minimum temperature Tnautve o Bortern Growth no longer occurs below this temperature [min. temp. for bacterial growth] Optimum temperature The most rapid growth occurs [bacteria grow best] Maximum temperature Growth is not possible above this temperature [kill the bacteria when over the max. temp.] Denatured Lower uppev Temp https://ucanr.edu/blogs/blogcore/postdetail.cfm?postnum=26278 ↓ repyratoy H, w ghe. Bactev 개 Temp resnroty il 15 、 」 Physical Requirement -- Temperature (cont’d) Classification according to temperature requirement: Low temperature/cold Psychrophiles W Can grow at 0 – 10oC, optimum temp. at ~10oC Psychrotrophs Optimum temp at ~20oC Mesophiles Middle range Can grow at 25 – 40oC, optimum temp. at 37oC Textbook: Microbiology Fig. 6.2 Thermophile Hot temperature Optimum temp. at ~50-60oC Hyperthermophiles Super hot temperature Optimum temp. at >80oC Toxin that releases by some toxic bacteria cannot be removed even the toxic bacteria is killed by high temperature Textbook: Microbiology Fig. 6.1 16 Physical Requirement -- pH Different microbes have different requirement for minimal, optimal & maximal pH to grow Grow better in acidic ph Acidophiles Grow best at low pH (acidic environment) Alkaliphiles Grow best at high pH (alkaline environment) Extreme pH can kill the microbes by Inactivating (Denaturing) proteins Disrupting transport in the plasma membrane Destroying enzymes in the cytoplasm Bacteria usually grow best at neutral (~pH 6.5 – 7.5) In general, pathogens do not grow, or grow very slowly, at < pH 4 Molds & yeasts will grow over a greater pH range than bacteria 17 Physical Requirement -- Osmotic Pressure Salt (as solute) osmolarity of surrounding environment Microorganisms require water for growth Water account for 80 – 90% of their composition High osmotic pressure has the effect of removing necessary water from a cell (water move out of the cell) [Salt] in solution > [Salt] in cell (hypertonic solution) Water moves out Osmotic loss of water causes plasmolysis or shrinkage of the cell’s cytoplasm Must t sa Obligate halophiles Grow well in high salt concentration e.g. Microbes found in Dead Sea Both Textbook: Microbiology Fig. 6.4 1 Facultative halophiles Do not require high salt concentration, but can grow at moderate salt level (~2%) 18 Chemical Requirement Carbon Universal source of energy needed by all living organisms For synthesis of all organic molecules to build cell structures Carbohydrates (e.g. glucose, starch) are the major energy source Nitrogen For synthesis of DNA, RNA, proteins, etc. Phosphorous For synthesis of DNA, RNA, ATP, membrane phospholipids Sulphur For synthesis of proteins Trace elements Needed in small amounts As enzyme cofactors, growth factors Important for cellular functions, e.g. energy production, metabolism 19 Chemical Requirement (cont’d) Oxygen Aerobes Require O2 to grow a. Obligate aerobes O2 must present ratmosphernclevel b. Microaerophiles Require O2, but lower than atmospheric level Anaerobes Growth is inhibited by O2 c. Facultative anaerobes Can grow with / without O2 (grow better with O2) d. Aerotolerant anaerobes Cannot use O2, but tolerate the presence of O2 e. Obligate anaerobes Poisoned by O2 (O2 is toxic) 20 PART 2: Control of Microbial Growth Terminologies Physical methods Chemical methods 21 Purpose to Control Microorganism Growth To kill, control, slow down the growth of microorganisms To prevent infections To reduce transmission of diseases To maintain a good health / hygiene To achieve an aseptic environment for clinical / surgical / laboratory practices 22 Terminology for Controlling Microorganism Growth -cide / -cidal (suffix) Methods = To kill e.g. Bactericidal = kill bacteria :햇업 Sterilization -static / -stasis (suffix) Reduction in microbes MOsT tA 에 = To stop or steady *311 , ; 로걸 시브 … , , Stop the growth of microorganisms, Disinfection NOT kill : FXP 묻 XAIl tRemwreae lowlevel Growth might resume Sanitization e.g. Bacteriostatic Cleaning 23 Terminology for Controlling Microorganism Growth (cont’d) Control Method Reduction Level Methods Examples Sterilization o Destruction or elimination o Heat sterilization o Autoclave of ALL living o Using chemical - High temperature microorganisms, sterilizer (121oC) + High pressure incl. endospores (15psi) for 15 minutes Disinfection o Elimination MOST of o Chemical o Using disinfectant to / Antisepsis vegetative microorganisms, disinfection perform decontamination EXCEPT endospores o Bleach vs o Using antiseptic to perform o ≠ Complete sterility 70% Alcohol antisepsis o Disinfection kills microbes on non-living things o Antisepsis kills microbes on living object (non-toxic) Sanitization o Reduce bacteria number o Chemical o Using sanitizer to reduce to a safe level microbial number o Using soap to wash hands 24 「 Methods for Controlling Microbial Growth A. Physical Methods B. Chemical Methods 1. Heat sterilization 1. Low antimicrobial power by thermal destruction a. Soap and detergent Moist heat b. Heavy metal a. Autoclave b. Pasteurization 2. Intermediate antimicrobial power c. Boiling c. Phenolic compounds Dry heat d. Halogen d. Direct flame e. Alcohol e. Hot-air oven 3. High antimicrobial power 2. Irradiation f. Oxidizing agents a. X-ray / Gamma ray radiation g. Aldehyde b. UV-light radiation >- Damuye BwA mutation 25 Physical Methods -- Heat Sterilization Heating A universally well-accepted, cheap & easy method to control microorganism High temperature can denature protein -cidal effect cess cess Time I Temp ) less Efforts Moist heat is more effective than dry heat ∵ Penetrates materials much more rapidly than air + Water molecules conduct heat better than air Moist heat sterilization requires relatively lower temperatures & shorter exposure time when compared to dry heat sterilization 26 」 ^ Moist Heat -- Boiling 4 Stevy inme hetwod. Boil object in boiling water at 98 – 100 oC Heat inactivates microorganisms by denaturing protein 10 minutes can inactivate most vegetative cells, but NOT heat-resistant forms e.g. endospores Some fungal spores & viruses may require up to 30 minutes Bacterial spores often require > 2 hours Common method to “sterilize” drinking water 27 、 Moist Heat -- Autoclave t Autoclave " ☆ 평했습 Global standard for absolute control of microbial growth 니도 Steam under pressure (use moist heat + pressure) 15 pounds / square inch (psi) (~1.1 kg/cm2) At 121oC for 15 mins Most common sterilization method for materials not damaged by heat Examples Use in hospital Instruments, glassware, intravenous solutions Textbook: Microbiology Fig. 7.2 Use in laboratories Instruments, culture medium 28 「 Moist Heat -- Pasteurization Named after the great microbiologist Louise Pasteur Reduce the number of non-spore forming bacteria & heat-sensitive microbes in milk & juice Does NOT kill all microorganisms Only disinfection (not sterilization) Can keeps quality of the milk and juice, retains flavor Used to control pathogenic bacteria in milk or juice e.g. Prevent food spoilage caused by Salmonella spp., E. coli O157:H7 High-temperature short-time (HTST) pasteurization 72oC for 15 sec [milk sold at 4oC] Ultra-high-temperature (UHT) pasteurization 135oC for 2-5 sec [milk sold at 25oC] 29 Dry heat -- Direct Flame Kill by burning Oxidation e.g. To sterilize inoculating loops & the opening of test tube during bacterial culture [Try it in the lab session] Dry heat -- Hot-air Oven Very high dry temperature e.g. 171 oC for 1 hour or 160oC for >2 hours Used for sterilizing metal instruments, powders materials Moisture is undesirable 30 Physical Methods -- Irradiation Radiation kills microorganisms by damaging DNA & protein Strength depends on its Wavelength Intensity Duration Textbook: Microbiology Fig. 7.5 31 Physical Methods -- Irradiation (cont’d) mutation i X-ray / Gamma Ray Radiation A T UV-light Radiation X - Higher energy ray Cu kF Lower energy ray Stronger effect Weaker effect Ionizing radiation Cause DNA breakage 졌챠 to cause microorganism death Non-ionizing radiation Cause DNA mutation to cause microorganism death t , High penetration power Poor penetration power 어깝 e e. on surface Only microorganisms on the surface are susceptible to destruction Only useful for controlling surface contaminants Sterilization of interior structure of Commonly used in instruments, e.g. needles hospital operating rooms & sinks, aseptic filling rooms of pharmaceutical companies, laboratory culture chamber 32 Chemical Methods -- Low Antimicrobial Power Pw Soap & detergent sauntukator phinc , uphobc Common sanitizer to reduce number of microbes Physical rubbing off the bacteria 9 999. Heavy metal Otuna nembrane Interfere with microbial metabolism Q 우 o to inhibit growth & kill microbes e.g. Sliver, mercury, copper ¢ ㆀ Textbook: Microbiology Fig. 7.8 33 」 Chemical Methods -- Intermediate Antimicrobial Power Phenolic compounds 몹 Disrupt plasma membrane & denature protein to kill microbes With odour smell Examples Hexachlorophene: hand washing agent for surgical uses Triclosan: active ingredient in toothpaste rNot sood freeradzal Halogen fm크본 Forming radial that can oxidize microbes Examples Chlorine (e.g. hypochlorite ion CIO-) in bleach Iodine as antiseptics for wound cleaning Fluorine as antiseptics in toothpaste & drinking water 34 Chemical Methods -- Intermediate Antimicrobial Power (cont’d) Alcohol Disrupt plasma membrane & denature protein to kill microbes Effective concentration: 60% - 95% Most effective concentration: 70% 70% alcohol can penetrate bacterial cell wall Denature proteins & enzymes inside the cell Ifry 100% alcohol has poor penetrating power Can only denature proteins ¤ on cell wall surface frxny baltenn -cidal activity will be lost once evaporated Textbook: Microbiology Table 7.6 35 」 B3. High Antimicrobial Power Oxidizing agents Denature protein by oxidization Examples Hydrogen peroxide H2O2 Ozone O3 Aldehyde 쁩 Very high power Fix protein & nucleic acid Used in preserving biological specimen, preparing vaccine & histological specimen for medical examination e.g. 2% - 8% formaldehyde (formalin) [carcinogenic] 36 PART 3: Interactions between Microbes & Human Normal microbiota Pathogenic microbes Mechanism of pathogenicity 37 Relationship between Normal Microbiota & the Host * Microbiota or normal flora (microflora) Ithaseunes Human body is inhabited by many different bacteria benesthaal Relationship between normal microbiota & the host illustrates symbiosis One organism is dependent on the other Colonization 춤 Pb Presence of bacteria on body surface without causing disease Either Externally on skin surface; or Internally on mucosal surface Examples of Microbiota on Human ⑦☆ Skin: S. epidermidis Eye, mouth, nose: S. epidermidis, S. aureus Gastrointestinal tract: Various gut microbiota for fermentation e.g. E.coli Urogenital tract: Lactobacillus (maintain low pH in the vagina) L, sevetl And - cowply s 38 에 Textbook: Microbiology Table 14.1 39 Beneficial Effects of Microbiota 1. As a barrier to inhibit pathogenic bacteria A phenomenon called competitive exclusion By pathogen displacement, nutrient and oxygen competition, altering pH Microbiota secrete harmful substances against the invading microbes 2. Stimulates immune response t 9. Furg ' ? sewets Induce production of immunoglobulins (Ig) (antibodies) peneuhn Enhance immune system development in newborn 3. Improves digestion (in gut only) Gut microbiota acts as probiotics Bacterial fermentation of plant carbohydrates facilitates digestion, stimulates peristalsis, prevents constipation Fermentation also produces nutrients e.g. Short chain fatty acid (SCFA), vitamins B2, B9 (folic acid), B12, K 40 Interaction between Pathogens & Human Pathogens Microorganisms that can cause diseases in human Infection The entry & development or multiplication of an infectious agent in the body that causes disease Levels of infection Subclinical / inapparent infection (asymptomatic) i 뛰 : Latent infection (inactive active & produce symptoms) Clinical infection (symptomatic) 41 “Harmfulness” of a Pathogen Pathogenicity 도 춰가는 The inherent ability of a microorganism to cause disease to its host during the host-pathogen interaction e.g. Normal E.coli without causing diarrhoea vs highly pathogenic O157 E.coli that can cause diarrhoea Virulence 빽 Degree of pathogenicity (disease-producing power) of a microorganism e.g. Viruses that cause common cold with less severe symptoms vs influenza A with severe symptoms uthe β ) A pathogenic microorganism can be of high or low virulence nfmenra A non-pathogenic microorganism can never be of high virulence 42 Mechanism of Pathogenicity How is a disease / infection being developed? 1. Portal of entry 2. Adhere 3. Defense / survive in host 4. Invade 5. Damage 6. Portal of exit 43 Textbook: Microbiology Fig. 15.9 Microbial Mechanism of Pathogenicity (cont’d) 1. Portal of entry Pathogens usually entry host through Skin Contact with the Mucosal membrane environment on urogenital tract, digestive tract, respiratory tract, conjunctiva Different pathogens have different preferred portal of entry e.g. COVID-19 – respiratory mucosal membrane 2. Adhere After getting into the host The pathogen should get adhere onto the cell / tissue Recall: Bacteria: pili, capsule Virus: viral spike, surface protein Fungi: surface protein Parasite: hook, sucker 44 고답석[A Textbook: Microbiology Table 15.1 45 Mechanism of Pathogenicity (cont’d) 3. Defense / survive in host Ability of the pathogen to defense the host’s immune system, & being survived within the host by Avoiding phagocytosis (chemical nature of the capsule) Producing pathogen’s molecules to interfere / suppress the host’s immune responses (e.g. Ig A protease – digests the antibody) 4. Invade Ability of the pathogen to penetrate the tissue & spread in host’s body by Producing enzymes to break down the integrity of supporting tissues to help pathogen spread e.g. Invasins – cause rearrangement of nearby cytoskeleton 46 Mechanism of Pathogenicity (cont’d) 5. Damage Cause damage to the host’s tissue by Using the host’s nutrient Helminths absorb host nutrient for survival Causing direct damage ∞ Virus can kill the host cells or transform normal cells into malignant cells Produce toxins Bacteria produce exotoxin & endotoxin ^ … Inducing hypersensitive reaction ☆면 고 모구종 47 Exotoxin vs Endotoxin abie tosecrete eθ Exotoxin Endotoxin From both gram +ve (more common) LPS on the cell wall of & –ve bacteria gram –ve bacteria Protein produced inside pathogenic bacteria Being secreted out through Released into the host after exocytosis / after cell lysis bacterial cell lysis Can cause serious disease & death Effects Fever, hypotension, thrombosis, septic shock, etc. Most of them can be inactivated by heat Examples 좁어* 부에를 Diphtheria toxin, botulism toxin, 함 tetanus toxin, various food poisoning toxins (cholera toxin, Shiga toxin, Staphylococcus enterotoxin, etc.) 48 Textbook: Microbiology Table 15.3 49 Microbial Mechanism of Pathogenicity (cont’d) f t×75t ) 6. Portal of Exit Ways by which bacteria leave the host Allow pathogen to spread in a population Usually same portal of entry & exit Examples Respiratory tract: droplet, expelled during coughing or sneezing GI tract: Faeces Chicken pox: discharge from blister 50 「 Recap Part 1: Microbial Growth How microbes grow Methods measuring bacterial growth Factors affecting microbial growth Part 2: Control of microbial growth Terminologies Physical methods Chemical methods Part 3: Interactions between microbes & human Normal microbiota Pathogenic microbes Mechanism of pathogenicity 51 Reference Tortora, G.J., Funke, B.R., & Case, C.L. (2018). Microbiology: An Introduction (13th ed.). Pearson. Chapter 3 Observing Microorganisms Through a Microscope Chapter 4 Functional Anatomy of Prokaryotic and Eukaryotic Cells Chapter 6 Microbial Growth Chapter 7 The Control of Microbial Growth Chapter 14 Principles of Disease and Epidemiology Chapter 15 Microbial Mechanisms of Pathogenicity 52