SlideShare a Scribd company logo

Chemistry of gram negative cell wall with reference to antibiotics

Download as PPTX, PDF
The University of the Punjab, Lahore, Punjab, Pakistan
The University of the Punjab, Lahore, Punjab, Pakistan

The document summarizes the chemistry of the gram-negative cell wall and the effects of various antibiotics. It describes the general structure of the gram-negative cell wall, which has an outer membrane, peptidoglycan layer, and periplasmic space. The peptidoglycan is composed of sugars and amino acids that form a mesh-like polymer. The outer membrane contains lipopolysaccharides that protect the cell from host defenses. Several classes of antibiotics target aspects of cell wall synthesis, such as penicillins and cephalosporins which inhibit peptidoglycan cross-linking, and vancomycin which blocks transpeptidation.

Education
1 of 17
Chemistry of Gram negative cell wall with reference to antibiotics
Contents • Chemistry of cell wall • Effects of antibiotics
Chemistry of gram negative cell wall
Cell wall: • Layer, usually fairly rigid, that lies just outside the plasma membrane. • Helps determine the shape of the cell • Helps protect the cell from osmotic lysis • Can protect the cell from toxic substances; and in pathogens General structure: • It has a 2 to 7 nm peptidoglycan layer covered by a 7 to 8 nm thick outer membrane. • One important feature is a space that is frequently seen between the plasma membrane and the outer membrane called as periplasmic space. (ranges in size from 1 nm to as great as 71 nm). • The space filled with a metrial called as periplasm. • The most outer membrane is also an important constituent plays an important role in defence against antibiotics.
Chemistry of cell wall Two constituents are important to understand the basic chemistry: •Peptidoglycan • Outer membrane Peptidoglycan structure: • Also known as murein, is an enormous mesh like polymer composed of many identical subunits. • Polymer contains: oTwo sugar derivatives  N-acetylglucosamine  N-acetylmuramic acid o Several different amino acids (D-glutamic acid, D-alanine, and mesodiamino pimelic acid)
Composition of peptidoglycan polymer • Backbone is composed of alternating N-acetylglucosamine and N-acetylmuramic acid residues. • A peptide chain of four alternating D- and L-amino acids is connected to the carboxyl group of N-acetylmuramic acid. • In order to make a strong, meshlike polymer, chains of linked peptidoglycan subunits must be joined by cross-links between the peptides. Often the carboxyl group of the terminal D-alanine is connected directly to the amino group of diaminopimelic acid. • Periplasmic proteins are involved in peptidoglycan synthesis and the modification of toxic compounds that could harm the cell.
Outer Membrane • Lies outside the thin peptidoglycan layer and is linked to the cell in two ways.  The first is by Braun’s lipoprotein, the most abundant protein in the outer membrane.  Covalently joined to the underlying peptidoglycan  Embedded in the outer membrane by its hydrophobic end  Involves many adhesion sites joining the outer membrane and the plasma membrane. • The two membranes appear to be in direct contact at these sites. • The most unusual constituents of the outer membrane are its lipopolysaccharides (LPSs): These large, complex molecules contain both lipid and carbohydrate, and consist of three parts:  Lipid A  The core polysaccharide  The O side chain.
The lipid A region: Contains two glucosamine sugar derivatives, each with three fatty acids and phosphate or pyrophosphate attached. • Fatty acids attach the lipid A to the outer membrane • Remainder of the LPS molecule projects from the surface The core polysaccharide is joined to lipid A O side chain or O antigen: Polysaccharide chain extending outward from the core. Function of LPS: • Protects pathogenic gram-negative bacteria from host defenses. • O antigen elicits an immune response by producing some peculiar proteins. • Many gram negative bacteria are able to rapidly change the antigenic nature of their O side chains, thus thwarting host defenses. • Lipid A portion of LPS often is toxic, hence forming endotoxins, inducing septic shocks in their hosts.
Effects of Antibiotics
Antibiotics: • Antibiotic [anti, against, and bios, life] • Microbial products or their derivatives that can kill susceptible microorganisms or inhibit their growth. • Special kind of chemotherapeutic agents usually obtained from living organisms.
There are total 4 antibiotics vulnerable to the gram negative cell wall. • Penicillin • Cephalosporin • Vancomycin & Teicoplanin • Cycloserine
Penicillin • Most are derivatives of 6-aminopenicillanic acid and differ from one another with respect to the side chain attached to its amino group • The most crucial feature of the molecule is the β-lactam ring, which is essential for bioactivity Mechanism of action: There are several proposed mechanisms: • It is said that penicillins resemble the terminal D-alanyl-D-alanine found on the peptide side chain of the peptidoglycan subunit • They block the linkage between the peptidoglycans (transpeptidation) thereby blocking cross links, leading to osmotic lysis. • Penicillins may also bind to several periplasmic proteins (penicillin-binding proteins, or PBPs) and destroy bacteria by activating their own autolytic enzymes. β-lactam ring
•Penicillin may stimulate special proteins called bacterial holins to form holes or lesions in the plasma membrane, leading directly to membrane leakage and death. • Many penicillin-resistant bacteria produce penicillinase (also called β- lactamase), making penicillins unable to work. Attack site • Other penicillin derivatives are made by physicians in which bacteria cannot destroy β-lactame ring.
Cephalosporins • Isolated from the fungus Cephalosporium. • They contain a β-lactam structure that is very similar to that of the penicillins, so they also inhibit transpeptidation. • Given to those patients who are having penicillin allergy. • Four generations are made of cephalosporins  First generation is more effective against gram positive and less against negative  Second had improved effects against gram negative, with some anaerobe range.  Third generation was particularly developed against gram negative bacteria, but some of them cross blood brain barrier and cause harm.  Fourth generation is broad spectrum with excellent gram-positive and gram-negative coverage. They, inhibit the growth of the difficult opportunistic pathogen Pseudomonas aeruginosa.
Vancomycin and Teicoplanin • Vancomycin is a glycopeptide antibiotic produced by Streptomyces oreintalis. • Blocks the transpeptidation reaction. • Bactericidal for Staphylococcus and some members of the genera Clostridium, Bacillus, Streptococcus, and Enterococcus. • It is given both orally and intravenously. • Particularly important in the treatment of antibiotic resistant staphylococcal and enterococcal infections. • Staphylococcus has become resistant to Vancomycin so, threatning health. New generations of vancomycin must be made. • Teicoplanin is a glycopeptide obtained from Actinoplanes teichomyceticus. • Similar in structure and mechanism of action to vancomycin. • Active against staphylococci, enterococci, streptococci, clostridia, Listeria, and many other gram-positive pathogens.
Cycloserine • Relatively simpler compound. • Was originally discovered as an antibiotic produced by streptomycs and is now manufactured through chemical synthesis. • Main use is tuberculosis therapy. • Due to potential undesirable side effects, its utilization is limited. • Prevents the formation of peptide moeity • Inhibits both alanine racemase and D-alanyl-D-alanine synthetase, the enzymes involved in the synthesis of peptide side chains.
Questions & Answers

Recommended

MECHANISMS OF ANTIBACTERIAL ACTION.
MECHANISMS OF ANTIBACTERIAL ACTION.MECHANISMS OF ANTIBACTERIAL ACTION.
MECHANISMS OF ANTIBACTERIAL ACTION.
Dr. Ravi Sankar
 
Cell Wall Inhibitors
Cell Wall InhibitorsCell Wall Inhibitors
Cell Wall Inhibitors
shabeel pn
 
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
Saminathan Kayarohanam
 
Antibiotic Mechanisms
Antibiotic MechanismsAntibiotic Mechanisms
Antibiotic Mechanisms
Kimberly Treier
 
Meningitis antibiotics mechanism of action
Meningitis antibiotics mechanism of actionMeningitis antibiotics mechanism of action
Meningitis antibiotics mechanism of action
Mario Wilmath
 
Antimicrobials 1 Lec
Antimicrobials 1 LecAntimicrobials 1 Lec
Antimicrobials 1 Lec
MD Specialclass
 
Antibiotic Mechanisms of Action
Antibiotic Mechanisms of ActionAntibiotic Mechanisms of Action
Antibiotic Mechanisms of Action
Yazan Kherallah
 
Antibiotics
AntibioticsAntibiotics
Antibiotics
Ashiq Toor
 

Recommended

MECHANISMS OF ANTIBACTERIAL ACTION.
MECHANISMS OF ANTIBACTERIAL ACTION.MECHANISMS OF ANTIBACTERIAL ACTION.
MECHANISMS OF ANTIBACTERIAL ACTION.
Dr. Ravi Sankar
 
Cell Wall Inhibitors
Cell Wall InhibitorsCell Wall Inhibitors
Cell Wall Inhibitors
shabeel pn
 
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
3. ANTIBIOTIC (PROTEIN SYNTHESIS INHIBITORS)
Saminathan Kayarohanam
 
Antibiotic Mechanisms
Antibiotic MechanismsAntibiotic Mechanisms
Antibiotic Mechanisms
Kimberly Treier
 
Meningitis antibiotics mechanism of action
Meningitis antibiotics mechanism of actionMeningitis antibiotics mechanism of action
Meningitis antibiotics mechanism of action
Mario Wilmath
 
Antimicrobials 1 Lec
Antimicrobials 1 LecAntimicrobials 1 Lec
Antimicrobials 1 Lec
MD Specialclass
 
Antibiotic Mechanisms of Action
Antibiotic Mechanisms of ActionAntibiotic Mechanisms of Action
Antibiotic Mechanisms of Action
Yazan Kherallah
 
Antibiotics
AntibioticsAntibiotics
Antibiotics
Ashiq Toor
 
Antibiotics and their mode of action ankush (2019 a109m)
Antibiotics and their mode of action ankush (2019 a109m)Antibiotics and their mode of action ankush (2019 a109m)
Antibiotics and their mode of action ankush (2019 a109m)
ankushkanger1
 
Antibiotics introduction to classification
Antibiotics introduction to classificationAntibiotics introduction to classification
Antibiotics introduction to classification
NAGA PRASHANT KOPPURAVURI
 
Usmleantibiotics3028
Usmleantibiotics3028Usmleantibiotics3028
Usmleantibiotics3028
sarosem
 
Antibiotics and their mode of action
Antibiotics and their mode of actionAntibiotics and their mode of action
Antibiotics and their mode of action
Ajayprakashuniyal
 
Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2
Bruno Mmassy
 
Antibacterial chemotherapy
Antibacterial chemotherapyAntibacterial chemotherapy
Antibacterial chemotherapy
Sarath Thulaseedharan
 
Alkylating agents
Alkylating agentsAlkylating agents
Alkylating agents
Money Kalash
 
Antibiotics
AntibioticsAntibiotics
Antibiotics
SANDEEP MEWADA
 
Bacteria
BacteriaBacteria
Bacteria
kharatearun
 
Drug resistance
Drug resistanceDrug resistance
Drug resistance
Rinshana Fathima
 
Macrolides
MacrolidesMacrolides
Macrolides
Gourango Kumar
 
Tetracyclines, glycicyclines, macrolides and ketolides Drugs
Tetracyclines, glycicyclines, macrolides and ketolides DrugsTetracyclines, glycicyclines, macrolides and ketolides Drugs
Tetracyclines, glycicyclines, macrolides and ketolides Drugs
Areej Abu Hanieh
 
Chemotheray (Antibiotics) general cosideratons
Chemotheray (Antibiotics) general cosideratonsChemotheray (Antibiotics) general cosideratons
Chemotheray (Antibiotics) general cosideratons
kavya m
 
medicines used to treat bacterial infections
medicines used to treat bacterial infectionsmedicines used to treat bacterial infections
medicines used to treat bacterial infections
bahati_jr
 
Mode of action of penicillin
Mode of action of penicillin Mode of action of penicillin
Mode of action of penicillin
ShubhamDubey217
 
1. INTRODUCTION OF CHEMOTHERAPY
1. INTRODUCTION OF CHEMOTHERAPY1. INTRODUCTION OF CHEMOTHERAPY
1. INTRODUCTION OF CHEMOTHERAPY
Saminathan Kayarohanam
 
Class introduction to chemoTHERAPY
Class introduction to chemoTHERAPYClass introduction to chemoTHERAPY
Class introduction to chemoTHERAPY
Raghu Prasada
 
Medicinal chemistry-Anticancer agents
Medicinal chemistry-Anticancer agentsMedicinal chemistry-Anticancer agents
Medicinal chemistry-Anticancer agents
DHARMENDRA BARIA
 
vsv5
vsv5vsv5
vsv5
Hiệp Lê Bá
 
Emb +pasa
Emb +pasaEmb +pasa
Emb +pasa
Khalid Hussain
 
Bacterial cell wall
Bacterial cell wallBacterial cell wall
Bacterial cell wall
Ashfaq Ahmad
 
Bacterialcellwall 161031150608
Bacterialcellwall 161031150608Bacterialcellwall 161031150608
Bacterialcellwall 161031150608
NucmaanCqadir
 

More Related Content

What's hot

Usmleantibiotics3028
Usmleantibiotics3028Usmleantibiotics3028
Usmleantibiotics3028
sarosem
 
Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2
Bruno Mmassy
 
Mode of action of penicillin
Mode of action of penicillin Mode of action of penicillin
Mode of action of penicillin
ShubhamDubey217
 

What's hot (20)

Antibiotics and their mode of action ankush (2019 a109m)
Antibiotics and their mode of action ankush (2019 a109m)Antibiotics and their mode of action ankush (2019 a109m)
Antibiotics and their mode of action ankush (2019 a109m)
 
Antibiotics introduction to classification
Antibiotics introduction to classificationAntibiotics introduction to classification
Antibiotics introduction to classification
 
Usmleantibiotics3028
Usmleantibiotics3028Usmleantibiotics3028
Usmleantibiotics3028
 
Antibiotics and their mode of action
Antibiotics and their mode of actionAntibiotics and their mode of action
Antibiotics and their mode of action
 
Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2Antimicrobial agents and mechanisms of action 2
Antimicrobial agents and mechanisms of action 2
 
Antibacterial chemotherapy
Antibacterial chemotherapyAntibacterial chemotherapy
Antibacterial chemotherapy
 
Alkylating agents
Alkylating agentsAlkylating agents
Alkylating agents
 
Antibiotics
AntibioticsAntibiotics
Antibiotics
 
Bacteria
BacteriaBacteria
Bacteria
 
Drug resistance
Drug resistanceDrug resistance
Drug resistance
 
Macrolides
MacrolidesMacrolides
Macrolides
 
Tetracyclines, glycicyclines, macrolides and ketolides Drugs
Tetracyclines, glycicyclines, macrolides and ketolides DrugsTetracyclines, glycicyclines, macrolides and ketolides Drugs
Tetracyclines, glycicyclines, macrolides and ketolides Drugs
 
Chemotheray (Antibiotics) general cosideratons
Chemotheray (Antibiotics) general cosideratonsChemotheray (Antibiotics) general cosideratons
Chemotheray (Antibiotics) general cosideratons
 
medicines used to treat bacterial infections
medicines used to treat bacterial infectionsmedicines used to treat bacterial infections
medicines used to treat bacterial infections
 
Mode of action of penicillin
Mode of action of penicillin Mode of action of penicillin
Mode of action of penicillin
 
1. INTRODUCTION OF CHEMOTHERAPY
1. INTRODUCTION OF CHEMOTHERAPY1. INTRODUCTION OF CHEMOTHERAPY
1. INTRODUCTION OF CHEMOTHERAPY
 
Class introduction to chemoTHERAPY
Class introduction to chemoTHERAPYClass introduction to chemoTHERAPY
Class introduction to chemoTHERAPY
 
Medicinal chemistry-Anticancer agents
Medicinal chemistry-Anticancer agentsMedicinal chemistry-Anticancer agents
Medicinal chemistry-Anticancer agents
 
vsv5
vsv5vsv5
vsv5
 
Emb +pasa
Emb +pasaEmb +pasa
Emb +pasa
 

Similar to Chemistry of gram negative cell wall with reference to antibiotics

BACTERIA pdf.pdf
BACTERIA pdf.pdfBACTERIA pdf.pdf
BACTERIA pdf.pdf
DeeptiNegi13
 
Bacterial structure
Bacterial structureBacterial structure
Bacterial structure
Bruno Mmassy
 

Similar to Chemistry of gram negative cell wall with reference to antibiotics (20)

Bacterial cell wall
Bacterial cell wallBacterial cell wall
Bacterial cell wall
 
Bacterialcellwall 161031150608
Bacterialcellwall 161031150608Bacterialcellwall 161031150608
Bacterialcellwall 161031150608
 
Understanding the Potency of β-Lactam Antibiotics
Understanding the Potency of β-Lactam AntibioticsUnderstanding the Potency of β-Lactam Antibiotics
Understanding the Potency of β-Lactam Antibiotics
 
biosynthesis of the cell wall and antibiotics
biosynthesis of the cell wall and antibioticsbiosynthesis of the cell wall and antibiotics
biosynthesis of the cell wall and antibiotics
 
antimicrobialchemotherapy- Mode of action of antibiotics
antimicrobialchemotherapy- Mode of action of antibioticsantimicrobialchemotherapy- Mode of action of antibiotics
antimicrobialchemotherapy- Mode of action of antibiotics
 
Bacteria Structure.pptx
Bacteria Structure.pptxBacteria Structure.pptx
Bacteria Structure.pptx
 
Bacteria structure.pptx
Bacteria structure.pptxBacteria structure.pptx
Bacteria structure.pptx
 
Antimicrobial chemotherapy
Antimicrobial chemotherapyAntimicrobial chemotherapy
Antimicrobial chemotherapy
 
Chemotherapy
ChemotherapyChemotherapy
Chemotherapy
 
Beta Lactams.pptx
Beta Lactams.pptxBeta Lactams.pptx
Beta Lactams.pptx
 
Antibiotics
AntibioticsAntibiotics
Antibiotics
 
Lecture 5- antibiotics.ppt
Lecture 5- antibiotics.pptLecture 5- antibiotics.ppt
Lecture 5- antibiotics.ppt
 
lecture-5-antibiotics.PowerPoint Presentation
lecture-5-antibiotics.PowerPoint Presentationlecture-5-antibiotics.PowerPoint Presentation
lecture-5-antibiotics.PowerPoint Presentation
 
fundamentals of microbiology- bacterial membrane
fundamentals of microbiology- bacterial membranefundamentals of microbiology- bacterial membrane
fundamentals of microbiology- bacterial membrane
 
B.Sc. Microbiology II Bacteriology Unit II Morphology of Bacterial Cell
B.Sc. Microbiology II Bacteriology Unit II Morphology of Bacterial CellB.Sc. Microbiology II Bacteriology Unit II Morphology of Bacterial Cell
B.Sc. Microbiology II Bacteriology Unit II Morphology of Bacterial Cell
 
B.sc. microbiology II Bacteriology Unit II Morphology of Bacterial Cell
B.sc. microbiology II Bacteriology Unit II Morphology of Bacterial CellB.sc. microbiology II Bacteriology Unit II Morphology of Bacterial Cell
B.sc. microbiology II Bacteriology Unit II Morphology of Bacterial Cell
 
BACTERIA pdf.pdf
BACTERIA pdf.pdfBACTERIA pdf.pdf
BACTERIA pdf.pdf
 
Ultra structure of bateria
Ultra structure of bateriaUltra structure of bateria
Ultra structure of bateria
 
Bacterial Morphology.ppt
Bacterial Morphology.pptBacterial Morphology.ppt
Bacterial Morphology.ppt
 
Bacterial structure
Bacterial structureBacterial structure
Bacterial structure
 

Recently uploaded

Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
ZurliaSoop
 

Recently uploaded (20)

Sociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning ExhibitSociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning Exhibit
 
Food safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdfFood safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdf
 
How to Create and Manage Wizard in Odoo 17
How to Create and Manage Wizard in Odoo 17How to Create and Manage Wizard in Odoo 17
How to Create and Manage Wizard in Odoo 17
 
Google Gemini An AI Revolution in Education.pptx
Google Gemini An AI Revolution in Education.pptxGoogle Gemini An AI Revolution in Education.pptx
Google Gemini An AI Revolution in Education.pptx
 
Micro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdfMicro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdf
 
Towards a code of practice for AI in AT.pptx
Towards a code of practice for AI in AT.pptxTowards a code of practice for AI in AT.pptx
Towards a code of practice for AI in AT.pptx
 
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
 
SOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning PresentationSOC 101 Demonstration of Learning Presentation
SOC 101 Demonstration of Learning Presentation
 
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
 
Mehran University Newsletter Vol-X, Issue-I, 2024
Mehran University Newsletter Vol-X, Issue-I, 2024Mehran University Newsletter Vol-X, Issue-I, 2024
Mehran University Newsletter Vol-X, Issue-I, 2024
 
This PowerPoint helps students to consider the concept of infinity.
This PowerPoint helps students to consider the concept of infinity.This PowerPoint helps students to consider the concept of infinity.
This PowerPoint helps students to consider the concept of infinity.
 
General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...
 
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptxHMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
HMCS Max Bernays Pre-Deployment Brief (May 2024).pptx
 
Application orientated numerical on hev.ppt
Application orientated numerical on hev.pptApplication orientated numerical on hev.ppt
Application orientated numerical on hev.ppt
 
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
 
Holdier Curriculum Vitae (April 2024).pdf
Holdier Curriculum Vitae (April 2024).pdfHoldier Curriculum Vitae (April 2024).pdf
Holdier Curriculum Vitae (April 2024).pdf
 
80 ĐỀ THI THỬ TUYỂN SINH TIẾNG ANH VÀO 10 SỞ GD – ĐT THÀNH PHỐ HỒ CHÍ MINH NĂ...
80 ĐỀ THI THỬ TUYỂN SINH TIẾNG ANH VÀO 10 SỞ GD – ĐT THÀNH PHỐ HỒ CHÍ MINH NĂ...80 ĐỀ THI THỬ TUYỂN SINH TIẾNG ANH VÀO 10 SỞ GD – ĐT THÀNH PHỐ HỒ CHÍ MINH NĂ...
80 ĐỀ THI THỬ TUYỂN SINH TIẾNG ANH VÀO 10 SỞ GD – ĐT THÀNH PHỐ HỒ CHÍ MINH NĂ...
 
How to setup Pycharm environment for Odoo 17.pptx
How to setup Pycharm environment for Odoo 17.pptxHow to setup Pycharm environment for Odoo 17.pptx
How to setup Pycharm environment for Odoo 17.pptx
 
Python Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docxPython Notes for mca i year students osmania university.docx
Python Notes for mca i year students osmania university.docx
 
SKILL OF INTRODUCING THE LESSON MICRO SKILLS.pptx
SKILL OF INTRODUCING THE LESSON MICRO SKILLS.pptxSKILL OF INTRODUCING THE LESSON MICRO SKILLS.pptx
SKILL OF INTRODUCING THE LESSON MICRO SKILLS.pptx
 

Chemistry of gram negative cell wall with reference to antibiotics

  • 1. Chemistry of Gram negative cell wall with reference to antibiotics
  • 2. Contents • Chemistry of cell wall • Effects of antibiotics
  • 3. Chemistry of gram negative cell wall
  • 4. Cell wall: • Layer, usually fairly rigid, that lies just outside the plasma membrane. • Helps determine the shape of the cell • Helps protect the cell from osmotic lysis • Can protect the cell from toxic substances; and in pathogens General structure: • It has a 2 to 7 nm peptidoglycan layer covered by a 7 to 8 nm thick outer membrane. • One important feature is a space that is frequently seen between the plasma membrane and the outer membrane called as periplasmic space. (ranges in size from 1 nm to as great as 71 nm). • The space filled with a metrial called as periplasm. • The most outer membrane is also an important constituent plays an important role in defence against antibiotics.
  • 5. Chemistry of cell wall Two constituents are important to understand the basic chemistry: •Peptidoglycan • Outer membrane Peptidoglycan structure: • Also known as murein, is an enormous mesh like polymer composed of many identical subunits. • Polymer contains: oTwo sugar derivatives  N-acetylglucosamine  N-acetylmuramic acid o Several different amino acids (D-glutamic acid, D-alanine, and mesodiamino pimelic acid)
  • 6. Composition of peptidoglycan polymer • Backbone is composed of alternating N-acetylglucosamine and N-acetylmuramic acid residues. • A peptide chain of four alternating D- and L-amino acids is connected to the carboxyl group of N-acetylmuramic acid. • In order to make a strong, meshlike polymer, chains of linked peptidoglycan subunits must be joined by cross-links between the peptides. Often the carboxyl group of the terminal D-alanine is connected directly to the amino group of diaminopimelic acid. • Periplasmic proteins are involved in peptidoglycan synthesis and the modification of toxic compounds that could harm the cell.
  • 7. Outer Membrane • Lies outside the thin peptidoglycan layer and is linked to the cell in two ways.  The first is by Braun’s lipoprotein, the most abundant protein in the outer membrane.  Covalently joined to the underlying peptidoglycan  Embedded in the outer membrane by its hydrophobic end  Involves many adhesion sites joining the outer membrane and the plasma membrane. • The two membranes appear to be in direct contact at these sites. • The most unusual constituents of the outer membrane are its lipopolysaccharides (LPSs): These large, complex molecules contain both lipid and carbohydrate, and consist of three parts:  Lipid A  The core polysaccharide  The O side chain.
  • 8. The lipid A region: Contains two glucosamine sugar derivatives, each with three fatty acids and phosphate or pyrophosphate attached. • Fatty acids attach the lipid A to the outer membrane • Remainder of the LPS molecule projects from the surface The core polysaccharide is joined to lipid A O side chain or O antigen: Polysaccharide chain extending outward from the core. Function of LPS: • Protects pathogenic gram-negative bacteria from host defenses. • O antigen elicits an immune response by producing some peculiar proteins. • Many gram negative bacteria are able to rapidly change the antigenic nature of their O side chains, thus thwarting host defenses. • Lipid A portion of LPS often is toxic, hence forming endotoxins, inducing septic shocks in their hosts.
  • 10. Antibiotics: • Antibiotic [anti, against, and bios, life] • Microbial products or their derivatives that can kill susceptible microorganisms or inhibit their growth. • Special kind of chemotherapeutic agents usually obtained from living organisms.
  • 11. There are total 4 antibiotics vulnerable to the gram negative cell wall. • Penicillin • Cephalosporin • Vancomycin & Teicoplanin • Cycloserine
  • 12. Penicillin • Most are derivatives of 6-aminopenicillanic acid and differ from one another with respect to the side chain attached to its amino group • The most crucial feature of the molecule is the β-lactam ring, which is essential for bioactivity Mechanism of action: There are several proposed mechanisms: • It is said that penicillins resemble the terminal D-alanyl-D-alanine found on the peptide side chain of the peptidoglycan subunit • They block the linkage between the peptidoglycans (transpeptidation) thereby blocking cross links, leading to osmotic lysis. • Penicillins may also bind to several periplasmic proteins (penicillin-binding proteins, or PBPs) and destroy bacteria by activating their own autolytic enzymes. β-lactam ring
  • 13. •Penicillin may stimulate special proteins called bacterial holins to form holes or lesions in the plasma membrane, leading directly to membrane leakage and death. • Many penicillin-resistant bacteria produce penicillinase (also called β- lactamase), making penicillins unable to work. Attack site • Other penicillin derivatives are made by physicians in which bacteria cannot destroy β-lactame ring.
  • 14. Cephalosporins • Isolated from the fungus Cephalosporium. • They contain a β-lactam structure that is very similar to that of the penicillins, so they also inhibit transpeptidation. • Given to those patients who are having penicillin allergy. • Four generations are made of cephalosporins  First generation is more effective against gram positive and less against negative  Second had improved effects against gram negative, with some anaerobe range.  Third generation was particularly developed against gram negative bacteria, but some of them cross blood brain barrier and cause harm.  Fourth generation is broad spectrum with excellent gram-positive and gram-negative coverage. They, inhibit the growth of the difficult opportunistic pathogen Pseudomonas aeruginosa.
  • 15. Vancomycin and Teicoplanin • Vancomycin is a glycopeptide antibiotic produced by Streptomyces oreintalis. • Blocks the transpeptidation reaction. • Bactericidal for Staphylococcus and some members of the genera Clostridium, Bacillus, Streptococcus, and Enterococcus. • It is given both orally and intravenously. • Particularly important in the treatment of antibiotic resistant staphylococcal and enterococcal infections. • Staphylococcus has become resistant to Vancomycin so, threatning health. New generations of vancomycin must be made. • Teicoplanin is a glycopeptide obtained from Actinoplanes teichomyceticus. • Similar in structure and mechanism of action to vancomycin. • Active against staphylococci, enterococci, streptococci, clostridia, Listeria, and many other gram-positive pathogens.
  • 16. Cycloserine • Relatively simpler compound. • Was originally discovered as an antibiotic produced by streptomycs and is now manufactured through chemical synthesis. • Main use is tuberculosis therapy. • Due to potential undesirable side effects, its utilization is limited. • Prevents the formation of peptide moeity • Inhibits both alanine racemase and D-alanyl-D-alanine synthetase, the enzymes involved in the synthesis of peptide side chains.