Antibiotics and Antibiotic Resistance PDF

Summary

This document provides an overview of antibiotics and their resistance mechanisms. It discusses the characteristics of antibiotics, different types based on their mechanism of action, and the development of antibiotic resistance. The document is likely part of a larger work on medicine or microbiology.

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ANTIBIOTICS AND ANTIBIOTIC RESISTANCE

Antibiotics – biochemical substances produced by microorganisms that inhibit
the growth of, or kill, other microorganisms.

Many drugs are now completely synthetic or the natural drug is manipulated to
change its structure called semi synthetics.

There is a large number of antimicrobial agents available for treating diseases
caused by microorganisms. Such drugs are now an essential part of modern
medical practice.

The antimicrobial agents used in medical practice are aimed at eliminating the
infecting microorganisms or at preventing the establishment of an infection.

To be of therapeutic use, an antimicrobial agent must exhibit selective toxicity;
it must exhibit greater toxicity to the infecting pathogens than to the host
organism

Characteristics of an antibiotic

It should be toxic to the infecting organism while harmless to the host cells
and the microbiota of the host.

It should stay in toxic form for a sufficient amount of time to affect the
infecting microorganism. If it changes to another form or is broken down in the
body, it may not be useful.

Sufficient amounts of it should reach the site of infection to kill the infecting
agent.

The infecting agent should be sensitive to it.

Broad-spectrum antibiotics are active against several types of microorganisms
(e.g., tetracyclines are active against gram-negative rickettsiae. mycoplasma and
chlamydia) while narrow-spectrum antibiotics act against only one type of
microorganism (eg, vancomycin is active against gram-positive staphylococcus
only).

Antibiotics may be bactericidal, that is, they kill the bacteria, or may be
bacteriostatic, that is, they inhibit the growth of bacteria but do not kill them. In
the latter type, the bacteria can grow when the drug is withdrawn.

TYPES OF ANTIBIOTICS BASED ON MECHANISM OF ACTION
Inhibition of cell wall synthesis : Antibiotics such as Penicillins and
cephalosporins act by inhibiting transpeptidase and hence inhibit cell wall
synthesis. They bind to the penicillin-binding proteins (PBP) which are
cell surface receptors. Due to the absence of a rigid cell wall. the bacterial
cell cannot withstand the osmotic pressure and hence ruptures.
Inhibition of protein synthesis : Bacteria have 30S and 50S ribosomes
which differ from host cell ribosomes. Protein synthesis inhibitors take
advantage of this difference. They act by misreading messenger RNA and
inhibiting the formation of the initiation complex.
Drugs that act on 30S ribosomes are:
Aminoglycosides (gentamicin, amikacin)
Tetracycline (blocks the aminoacyl transfer RNA (RNA)
Drugs that act on 50S ribosomes are:
Chloramphenicol, which blocks the action of peptidyl transferase,
thereby preventing the formation of new peptides
Macrolides (erythromycin, clarithromycin and azithromycin), which
bind to the 50S ribosome. thereby preventing translocation
Other antibiotics with similar action-clindamycin. streptogramin and
linezolid
Inhibition of nucleic acid synthesis : This may take place in three ways.
1. Inhibition of precursor synthesis:
Sulphonamides These are structural analogues to para-amino benzoic acid
(PABA) required for folic acid synthesis.
Trimethoprim This inhibits dihydrofolate reductase.
2. Inhibition of DNA synthesis:
Fluoroquinolones They inhibit the DNA gyrase (topoisomerase) enzyme.
3 Inhibition of mRNA synthesis:
Rifampicin acts by blocking RNA polymerase and thereby, mRNA synthesis.
 Action on bacterial cell membrane: 1.Polymyxin destroys the
phospholipid component of the cell membrane and acts on Pseudomonas
and Acinetobacter.

2.Daptomycin disrupts the cell membrane of gram- positive cocci and
acts against staphylococci and enterococci.
ANTIBIOTIC RESISTANCE
Antimicrobial resistance refers to development of resistance to an antimicrobial
agent by a microorganism. It can be of two types
acquired
intrinsic

Acquired Resistance
this refers to the emergence of resistance in bacteria that are ordinarily
susceptible to antimicrobial agents, by acquiring
the genes coding for resistance. Most of the antimicrobial resistance shown by
bacteria belong to this category.
The emergence of resistance is a major problem worldwide in antimicrobial
therapy. Infections caused by resistant microorganisms often fail to respond to
the standard treatment l, resulting in prolonged illness, higher healthcare
expenditures, and a greater risk of death.
 Overuse and misuse of antimicrobial agents is the single most important cause
of developmental og acquired resistance.
The evolution of resistant strains is a natural phenomenon, which can occur
among bacteria especially when an antibiotic is overused.
Use of the particular antibiotic poses selective pressure in a population of
bacteria which in turn promotes
resistant bacteria to thrive and the susceptible bacteria to die off.
thus the resistant bacterial populations flourish in areas of high antimicrobial
use, where they enjoy a selective advantage over susceptible populations.
The resistant strains spread in the environment and transfer the genes coding
for resistance to other unrelated bacteria.

Other factors favouring the spread of antimicrobial resistance include-

Poor infection control practices in hospitals- e.g. poor hand hygiene practices
can facilitate transmission of
resistant strains.
inadequate sanitary conditions.
inappropriate food-handling.
irrational use of antibiotics by doctors, not following antimicrobial
susceptibility report.
Uncontrolled sale of antibiotics over the counters without a prescription.

Intrinsic Resistance

It refers to the innate ability of a bacterium to resist a class of antimicrobial
agents due to its inherent structural or
functional characteristics, (e.g. gram-negative bacteria are
resistant to vancomycin). this imposes only little threat to the world as very few
organisms show intrinsic resistance

Mutational and Transferable Drug Resistance
In presence of selective antibiotic pressure, bacteria
acquire new genes mainly by two broad methods:
Mutational Resistance

Resistance can develop due to mutation of the resident genes.
It is typically seen in Mycobacterium tuberculosis, developing resistance to
anti-tubercular drugs.
Mutational drug resistance differs from transferable drug resistance
Usually, it is a low level resistance, developed to one drug at a time; which can
be overcome by using combination of different classes of drugs.
That is why multidrug therapy is used in tuberculosis using 4-5 different
classes of drugs, such as isoniazid, rifampicin, pyrazinamide, ethambutol and
streptomycin.

Transferable Drug Resistance
In contrast, transferable drug resistance is plasmid coded and usually transferred
by conjugation or rarely by transduction, or transformation
The resistance coded plasmid ( called R plasmid) can carry multiple genes,
each coding for resistance to one class of antibiotic.
thus, it results in a high degree of resistance to multiple drugs, which cannot
be overcome by using combination of drugs.

Mechanism of Antimicrobial Resistance

Bacteria develop antimicrobial resistance by several mechanisms.
1. Decreased Permeability across the Cell Wall
Certain bacteria modify their cell membrane porin channels; either in their
frequency, size, or selectivity;
thereby preventing the antimicrobials from entering into the cell. This strategy
has been observed in many gram-negative bacteria, such as Pseudomonas,
Enterobacter and Klebsiella species against drugs, such as imipenem,
aminoglycosides and quinolones.
2. Efflux Pumps
Certain bacteria possess efflux pumps which mediate expulsion of the drug(s)
from the cell, soon after their entry; thereby preventing the intracellular
accumulation of drugs. This strategy has been observed in:
Escherichia coli and other Enterobacteriaceae against
tetracyclines, chloramphenicol.
Staphylococci against macrolides and streptogramins.
Staphylococcus aureus and Streptococcus pneumoniae
against fluoroquinolones.
3. By Enzymatic Inactivation
Certain bacteria can inactivate the antimicrobial agents by
producing various enzymes, such as:
Beta lactamase enzyme production (observed in both gram-positive and
gram-negative bacteria): It breaks down the beta lactam rings, there by
inactivating the Beta lactam antibiotics
Aminoglycoside modifying enzymes like (acetyltransferases,
adenylyltransferase, and phosphotransferases, produced by both
gram-negative and gram-positive bacteria)-they destroy the structure of
aminoglycosides.
Chloramphenicol acetyltransferase: It is produced by members of
Enterobacteriaceae; it destroys the structure of chloramphenicol.

4.By Modifying the Target Sites
Modification of the target sites of antimicrobial agents (which are within the
bacteria) is a very important mechanism. It is observed in:
MRSA (Methicillin-resistant Staphylococcus aureus): ln
these strains, the target site of penicillin i.e. penicillin binding protein(PBP)gets
altered toPBP-2a. The altered
PBP do not sufficient to bind beta-lactam antibiotics and therefore prevent them
from inhibiting the cell wall
synthesis.
Streptomycin resistance in Mycobacterium tuberculosis:
It is due to modification of ribosomal proteins or 16S rRNA.
Rifampicin resistance in Mycobacterium tuberculosis due to mutations in
RNA polymerase.
Quinolone resistance seen in many gram-positive bacteria, particularly S.
aureus and S. pneumoniae
due to mutations in DNAgyrase enzyme.
Vancomycin resistance in enterococci (VRE): These strains have a change in
the target site of vancomycin(i.e. D-alanine
D-alanine side chain peptidoglycan)