Antibiotics.
Publié le 11/05/2013
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In some species of bacteria the cell wall consists primarily of a thick layer of peptidoglycan.
Other species have a much thinner layer of peptidoglycan and an outer aswell as an inner membrane.
When bacteria are subjected to Gram's stain, these differences in structure affect the differential staining of the bacteria with a dye calledgentian violet.
The differences in staining coloration (gram-positive bacteria appear purple and gram-negative bacteria appear colorless or reddish, depending on theprocess used) are the basis of the classification of bacteria into gram-positive (those with thick peptidoglycan) and gram-negative (those with thin peptidoglycan and anouter membrane), because the staining properties correlate with many other bacterial properties.
Antibacterials can be further subdivided into narrow-spectrum andbroad-spectrum agents.
The narrow-spectrum penicillins act against many gram-positive bacteria.
Aminoglycosides, also narrow-spectrum, act against many gram-negative as well as some gram-positive bacteria.
The tetracyclines and chloramphenicols are both broad-spectrum drugs because they are effective against both gram-positive and gram-negative bacteria.
C Cell Death and Growth Suppression
Antibiotics may also be classed as bactericidal (killing bacteria) or bacteriostatic (stopping bacterial growth and multiplication).
Bacteriostatic drugs are nonethelesseffective because bacteria that are prevented from growing will die off after a time or be killed by the defense mechanisms of the host.
The tetracyclines and thesulfonamides are among the bacteriostatic antiobiotics.
Antibiotics that damage the cell membrane cause the cell's metabolites to leak out, thus killing the organism.Such compounds, including penicillins and cephalosporins, are therefore classed as bactericidal.
IV TYPES OF ANTIBIOTICS
Following is a list of some of the more common antibiotics and examples of some of their clinical uses.
This section does not include all antibiotics nor all of their clinicalapplications.
A Penicillins
Penicillins are bactericidal, inhibiting formation of the cell wall.
There are four types of penicillins: the narrow-spectrum penicillin-G types, ampicillin and its relatives, thepenicillinase-resistants, and the extended spectrum penicillins that are active against pseudomonas.
Penicillin-G types are effective against gram-positive strains ofstreptococci, staphylococci, and some gram-negative bacteria such as meningococcus.
Penicillin-G is used to treat such diseases as syphilis, gonorrhea, meningitis,anthrax, and yaws.
The related penicillin V has a similar range of action but is less effective.
Ampicillin and amoxicillin have a range of effectiveness similar to that ofpenicillin-G, with a slightly broader spectrum, including some gram-negative bacteria.
The penicillinase-resistants are penicillins that combat bacteria that havedeveloped resistance to penicillin-G.
The antipseudomonal penicillins are used against infections caused by gram-negative Pseudomonas bacteria, a particular problem in hospitals.
They may be administered as a prophylactic in patients with compromised immune systems, who are at risk from gram-negative infections.
Side effects of the penicillins, while relatively rare, can include immediate and delayed allergic reactions—specifically, skin rashes, fever, and anaphylactic shock, whichcan be fatal.
B Cephalosporin
Like the penicillins, cephalosporins have a Β-lactam ring structure that interferes with synthesis of the bacterial cell wall and so are bactericidal.
Cephalosporins are moreeffective than penicillin against gram-negative bacilli and equally effective against gram-positive cocci.
Cephalosporins may be used to treat strains of meningitis and asa prophylactic for orthopedic, abdominal, and pelvic surgery.
Rare hypersensitive reactions from the cephalosporins include skin rash and, less frequently, anaphylacticshock.
C Aminoglycosides
Streptomycin is the oldest of the aminoglycosides.
The aminoglycosides inhibit bacterial protein synthesis in many gram-negative and some gram-positive organisms.They are sometimes used in combination with penicillin.
The members of this group tend to be more toxic than other antibiotics.
Rare adverse effects associated withprolonged use of aminoglycosides include damage to the vestibular region of the ear, hearing loss, and kidney damage.
D Tetracyclines
Tetracyclines are bacteriostatic, inhibiting bacterial protein synthesis.
They are broad-spectrum antibiotics effective against strains of streptococci, gram-negative bacilli,rickettsia (the bacteria that causes typhoid fever), and spirochetes (the bacteria that causes syphilis).
They are also used to treat urinary-tract infections and bronchitis.Because of their wide range of effectiveness, tetracyclines can sometimes upset the balance of resident bacteria that are normally held in check by the body's immunesystem, leading to secondary infections in the gastrointestinal tract and vagina, for example.
Tetracycline use is now limited because of the increase of resistantbacterial strains.
E Macrolides
The macrolides are bacteriostatic, binding with bacterial ribosomes to inhibit protein synthesis.
Erythromycin, one of the macrolides, is effective against gram-positivecocci and is often used as a substitute for penicillin against streptococcal and pneumococcal infections.
Other uses for macrolides include diphtheria and bacteremia.
Sideeffects may include nausea, vomiting, and diarrhea; infrequently, there may be temporary auditory impairment.
F Sulfonamides
The sulfonamides are synthetic bacteriostatic, broad-spectrum antibiotics, effective against most gram-positive and many gram-negative bacteria.
However, becausemany gram-negative bacteria have developed resistance to the sulfonamides, these antibiotics are now used only in very specific situations, including treatment ofurinary-tract infection, against meningococcal strains, and as a prophylactic for rheumatic fever.
Side effects may include disruption of the gastrointestinal tract andhypersensitivity.
V PRODUCTION
The production of a new antibiotic is lengthy and costly.
First, the organism that makes the antibiotic must be identified and the antibiotic tested against a wide varietyof bacterial species.
Then the organism must be grown on a scale large enough to allow the purification and chemical analysis of the antibiotic and to demonstrate that itis unique.
This is a complex procedure because there are several thousand compounds with antibiotic activity that have already been discovered, and these compounds.
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