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BACTERIAL INFECTIONS
What are bacterial infections?
Bacteria are microscopic organisms of many different types with
a chemically distinctive cell wall. This gives each type a particular
shape - spherical, rod-shaped or spiral. They multiply by cell
division - a process that can occur every 20-30 minutes. A single
bacterium entering the body and multiplying at this rate could give
rise to over 30 billion new cells within 12 hours. Fortunately, most
bacteria are harmless and some are even essential, such as those in
the intestine which aid digestion. But a minority, called pathogens,
cause disease (Figure 1 and Table 1). These may be localised near
the surface of the skin, as in laryngitis, boils and abscesses, or
invade internal organs and cause, for example, infections of the
digestive or urinary tract, brain (meningitis), lung (pneumonia),
heart (endocarditis), or the bloodstream (sepsis), which can be
serious or life-threatening.
Who do bacterial infections affect?
Everyone experiences bacterial infections from time to time, but
most infections heal by themselves or are readily treated with
antibiotics. However, resistance to antibiotics is an ever-growing
problem and infections that were easily treatable a decade ago are
now staging a come-back in deadlier form.
Examples of bacteria and some related illnesses* |
GRAM-POSITIVE |
GRAM-NEGATIVE |
| Staphylococcus aureus |
MRSA blood poisoning |
Neisseria meningitidis |
Meningitis |
| Streptococcus pneumoniae |
Pneumonia |
Moraxella catarrhalis |
Sinusitis, bronchitis |
| Streptococcus pyogenes |
Necrotising fasciitis |
Bordetella pertussis |
Whooping-cough |
| Enterococcus spp |
Bacteraemia |
Escherichia coli |
Peritonitis, sepsis |
| Clostridium difficile |
Diarrhoea |
Klebsiella pneumoniae |
Pneumonia, urinary-tract infections |
| Bacillus anthracis |
Anthrax |
Salmonella typhi |
Typhoid fever |
| Listeria monocytogenes |
Listeriosis |
Pseudomonas aeruginosa |
Burn/wound infections |
NOT RELIABLY STAINED BY GRAM’S METHOD |
| |
Borrellia burgdorferi |
Lyme disease |
|
| |
Legionella pneumophila |
Legionnaires' disease |
|
| |
Mycobacterium tuberculosis |
Tuberculosis |
|
| |
Mycobacterium leprae |
Leprosy |
|
| |
Treponema pallidum |
Syphilis |
|
| |
Rickettsia rickettsii |
Rocky Mountain spotted fever |
|
| * Note:This listing of bacteria and diseases is not exhaustive |
Table 1: Bacteria are often distinguished according to whether they are stained by a method first described in 1884 by the Danish
bacteriologist Hans Christian Gram.
People whose immunity is depressed by other illnesses such as
cancer, or by immunosuppressive treatments, as in transplant surgery, are at greater risk of serious infection. Hospital-acquired
infections are becoming increasingly frequent. If an infection
(sepsis) develops, it may lead to septic shock - a cascade of
inflammation, blood clotting and low blood pressure that often
results in death through multiple organ failure. In 2004, people
with sepsis required over 270,000 bed-days of inpatient care in
hospitals in England and sepsis was recorded as the underlying
cause of more than 2,000 deaths in England and Wales, 87 per
cent of them in people aged 60 and over. During the same period
there were more than 7,000 cases of bacteria in the blood due to
methicillin-resistant Staphylococcus aureus (MRSA) in England and
more than 44,000 infections due to Clostridium difficile, with over
1,200 deaths due to this organism. A study has shown that the cost
of treating patients who develop sepsis after admission to an
intensive care unit exceeded £10,000 per patient (in 1999).
Their average stay in the unit was 16 days, compared with 2 days
for those without sepsis, and their death rate 50-60 per cent
(versus 20 per cent).
| Class |
Mode of action |
Examples |
| Beta-lactams |
Inhibit bacterial cell wall synthesis |
Penicillins |
Penicillin G
Amoxicillin
Piperacillin |
| Cephalosporins |
Cefalexin
Cefuroxime
Ceftazidime
Ceftriaxone |
| Carbapenems |
Ertapenem
Meropenem |
| Glycopeptides |
Inhibit cell wall synthesis & assembly |
Vancomycin
Teicoplanin |
| Quinolones |
Inhibit bacterial DNA replication |
Ciprofloxacin
Norfloxacin
Moxifloxacin |
| Aminoglycosides |
Inhibit bacterial protein synthesis by
binding to 30S ribosomal subunit |
Amikacin
Gentamicin
Netilmicin
Tobramycin |
| Macrolides |
Inhibit bacterial protein synthesis by
binding to 50S ribosomal subunit |
Erythromycin
Azithromycin
Clarithromycin |
| Ketolides |
Inhibit bacterial protein synthesis |
Telithromycin |
Tetracyclines and
derivatives |
Inhibit bacterial protein synthesis by
blocking tRNA binding to ribosomes |
Doxycycline
Chlortetracycline
Tigecycline |
| Oxazolidinones |
Inhibit bacterial protein synthesis |
Linezolid |
| Streptogramins |
Inhibit bacterial protein synthesis |
Synercid |
| Sulphonamides |
Inhibit folate synthesis |
Sulfamethoxazole
Trimethoprim |
| Others |
Various |
Chloramphenicol
Metronidazole
Aztreonam
Clindamycin
Rifampicin |
Table 2: Some major types of antibiotics currently available and their mechanisms of action.
Present treatments and shortcomings
Many antibiotics have been discovered over the last fifty years,
including the penicillins and cephalosporins, tetracyclines,
macrolides, aminoglycosides (streptomycin group) and quinolones.
(Table 2) Despite this range of medicines, the emergence of
resistant organisms such as MRSA and vancomycin-resistant
enterococci (VRE) is creating widespread concern.
A variety of antibiotics have been introduced in recent years, in an
attempt to keep ahead of growing resistance. Synercid
(quinupristin/dalfopristin, sanofi-aventis), the first of the
streptogramin group, combines two components that together kill a
wide range of bacteria, including MRSA strains. Linezolid (Zyvox,
Pfizer) is an oxazolidinone which is used in hospital for treating
pneumonia and skin and soft tissue infections due to resistant
strains of Gram-positive bacteria. Another new class of antibiotic
(ketolides), is represented by telithromycin (Ketek, sanofi-aventis).
It is used to treat community-acquired respiratory tract infections,
including those caused by resistant strains of Streptococcus
pneumoniae. More recently, tigecycline (Tygacil, Wyeth) has
become available for the treatment of complicated skin, soft tissue
and intra-abdominal infections and Novartis has daptomycin
(Cubicin) for the first two of these uses.
NEW SINCE 2000 |
| 2001 - |
Linezolid (Zyvox, Pfizer) |
| 2001 - |
Telithromycin (Ketek,
sanofi-aventis) |
| 2002 - |
Ertapenem (Invanz,
Merck Sharp & Dohme) |
| 2002 - |
Drotrecogin (Xigris, Lilly) |
| 2003 - |
Moxifloxacin (Avelox, Bayer) |
2006 -
|
Tigecycline (Tigacyl,Wyeth)
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What's in the development pipeline?
The search continues for antibiotics that work in new ways, and so
might be active against bacteria that have developed resistance to
other medicines. GlaxoSmithKline has completed Phase 3 trials for
retapamulin, the first in the class of pleuromutilin antibiotics, and
two further members of this class (GSK 565154 and 742510) are in
Phase 1 development. Retapamulin is applied to the skin (a topical
medicine) in skin and soft tissue infections. Merck Sharp &
Dohme's platensimycin blocks enzymes involved in fatty acid
production that are used by bacteria to make their cell walls. It is
still in early development, but pre-clinical experiments have shown
it to be effective against MRSA and vancomycin-resistant
enterococci, two key types of antibiotic-resistant bacteria.
Many new members of existing classes of antibiotics are also in
development:
- A second ketolide antibiotic (cethromycin, Advanced Life
Sciences) is in Phase 3 study for community-acquired
pneumonia.
- Replidyne is developing the oral penem (faropenem
medoxomil, Orapem) and Johnson & Johnson is
conducting Phase 3 trials of doripenem in urinary tract
infections, intra-abdominal infections and hospitalacquired
pneumonia. Roche is also developing a new
carbapenem - R1558, which has reached Phase 2 trials.
- Pfizer is investigating dalbavancin (Zeven), a
lipoglycopeptide in the same class as vancomycin.
Dalbavancin can be given once weekly, and is active
against Gram-positive but not Gram-negative bacteria.
Another lipoglycopeptide in development is telavancin
(Theravance), which has reached Phase 3 trials in
hospital-acquired pneumonia and complicated skin and
skin structure infections.
- Other new antibiotics under development for skin
infections include Arpida's Iclaprim, a dihydrofolate
reductase inhibitor in the trimethoprim class, which is in
Phase 3 trials as an injectable and at Phase 1 in
oral form.
- Two new cephalosporins are under investigation:
ceftobiprole (Basilea, Phase 3) and ceftaroline acetate
(Cerexa, Phase 2).
- In addition, Enanta is investigating a new macrolide (EDP-420) in Phase 2 trials for community acquired
pneumonia.
- Sanofi-aventis has a new oral streptogramin (XRP 2868)
at Phase 1, as has Novexel (NXL 103).
- New quinolone antibiotics are also still being developed.
Oscient Pharmaceuticals has gemifloxacin (Factive) in
Phase 3 trial for bacterial sinusitis, while Schering-Plough
has the broad-spectrum agent garenoxacin. Daiichi-
Sankyo has the injected fluoroquinolone DU-6859a
(sitafloxacin) in Phase 2 trials and is preparing Phase 3
trials for the oral form of this medicine. The company also
has the quinolone DX 619 in Phase 1 trial.
Of particular interest are new treatments for the serious problem of
C. difficile diarrhoea, for which metronidazole and vancomycin are
the only currently available antibiotics. Two new antibiotics under
development are ramoplanin, a lipoglycopeptide being studied by
Oscient that acts to kill the bacteria in the intestine, and
Tiacumicin B, being tested by Par Pharmaceuticals. Both have
reached Phase 2 trials. Genzyme is working on a new approach
that uses a non-absorbed polymer (tolevamer) to bind the toxins
released by this organism and hence control the diarrhoea
associated with its uncontrolled growth in the intestine. Tolevamer
is now in Phase 3 trials. Another toxin-binding approach is being
explored by Medarex in Phase 2 trials of MDX-066, a monoclonal
antibody against C. difficile.
The remaining big problem in bacterial infection, apart from
antibiotic resistance, is the lack of effective medicines for treating
severe sepsis, which still causes a lot of deaths. Drotrecogin alfa
activated (Xigris, Lilly), a version of the naturally occurring
activated Protein C, has been introduced, but the reduction in
death rate it brings is relatively modest and new alternatives are
urgently needed. A major challenge to developing effective
therapies is the great complexity of inflammatory and
blood-clotting pathways that are activated in sepsis, making it
difficult to find an agent that can shut down the cascade of events
that lead to circulatory collapse and organ failure.
Eisai has a compound (E5564, eritoran) in Phase 3 trial that may
offer an alternative, as it inhibits an early step in the events leading
to the rapid production of inflammatory cytokines involved in
sepsis. A Phase 3 study of this compound has now started to
evaluate whether eritoran can significantly lower the death rate
from severe sepsis. Takeda also has a TLR-4 inhibitor (TAK-242)
under investigation and Novartis is investigating TFP 561 (tifacogin,
Phase 3) in severe community acquired pneumonia, which may
precede sepsis. Meanwhile, AstraZeneca is preparing a Phase 3
trial of the antibody CytoFab which is directed against TNF-α (one
of the key inflammatory cytokines). If any of these compounds can
be shown to produce a substantial decrease in sepsis-associated
deaths, that will be a very welcome development for those
clinicians and patients facing the most dramatic forms of bacterial
infection.
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