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    <title>IMC Journal of Medical Science</title>
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                <title><![CDATA[Emerging bacterial resistance to antibiotics – fighting a losing battle !]]></title>

                                    <author><![CDATA[J. Ashraful Haq]]></author>
                
                <link data-url="https://imcjms.com/registration/journal_full_text/128">
    https://imcjms.com/registration/journal_full_text/128
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                <pubDate>Sun, 06 Nov 2016 10:15:20 +0000</pubDate>
                <category><![CDATA[Editorial]]></category>
                <comments><![CDATA[Ibrahim Med. Coll. J. 2009; 3(1): i-ii]]></comments>
                <description>As we
approach the end of first decade of 21st century, it is now time to seriously
reconsider the hopes and zeal that transpired in the thirties and forties of
the last century with the discovery of antimicrobials like sulfa and
penicillin. These magic bullets saved millions of lives from deadly infectious
agents. However, by the beginning of 1960s, the enthusiasm soon faded away as
many of the organisms like Staphylococcus aureus, a gram positive
bacterium, became resistant to penicillin due to its capability to produce
penicillin destroying enzymes called penicillinase or beta-lactamase. The
discovery of penicllinase or beta-lactamse resistant penicillins like
methicillin soon outwitted the smart bacteria. But this also did not last long.
Staphylococcus aureus started to become resistant to methicillin. The
resistance was due to a subtle change in its penicillin binding protein called
PBP2a. Today, methicillin resistant S. aureus (MRSA) is a leading cause
of hospital acquired infection in all countries of the world including
Bangladesh. In a multi-center study involving four divisions of Bangladesh, the
rate of isolation of MRSA from hospital patients ranged between 32-63%.1&amp;nbsp;The trend is alarming. There
are not many affordable drugs to treat simple infections with MRSA. The
emergence of antibiotic resistance is now widespread and involves both gram
positive and a wide range of gram negative organisms. One example is the spread
of antibiotic resistance in Salmonella typhi, a gram negative bacterium,
responsible for typhoid fever in Bangladesh and in many countries of the world.
Typhoid fever was treated by simple antibiotics like ampicillin, cotrimoxazole
or chloramphenicol till the mid 1980s. Since then, ciprofloxacin or third
generation cephalosporins have been increasingly used in the treatment of
typhoid fever in Bangladesh due to development of resistance to earlier drugs.2&amp;nbsp;Since 1997, treatment
failures with ciprofloxacin have slowly started to emerge in Bangladesh and
other countries due to infection with nalidixic acid resistant Salmonella
typhi or NARST.3-6&amp;nbsp;NARST
has decreased susceptibility to ciprofloxacin. A study conducted in an urban
hospital of Bangladesh noted 75% of S. typhi resistant to nalidixic acid
vis-a-vis ciprofloxacin.7&amp;nbsp;Wonder drugs for treating typhoid have now
become archaic and the list becomes ever growing. Today, many of the bacteria
which were sensitive to and treatable with cephalosporins have become resistant
due to production of extended spectrum beta-lactamases (ESBL). The enzyme
effectively inactivates all generation of cephalosporins leaving the medical
doctors with only few choices of more expensive antibiotics. A study conducted
in a referral hospital of Dhaka city has noted 43.2% and 39.5% of E. coli and
K. pneumoniae were of ESBL phenotypes respectively.8&amp;nbsp;The picture is similar in
many other countries.
Scientists are striving to develop newer drugs to combat the
emerging bacterial resistance. Exploitation of quorum sensing phenomena, use of
bacteriophage and antimicrobial peptides are few examples. Many strategies have
been taken to control the never ending challenges of resistant bacteria.
Effective infection control and antibiotic policy are few of them. We must now
cautiously prescribe antibiotics particularly, those which are considered as
reserve antibiotics for multi-resistant organisms. But the most important of
all is not the discovery of new wonder drugs but the prudent and restrained use
of antibiotics by the medical community and raising the public awareness
regarding the dangers of prolific use of new and costly antibiotics. If we wish
to live in a world where bacteria live subjugated to human beings, then we must
realize a simple fact – the war against bacteria is far from over.
References
2.&amp;nbsp; Haque Asna SMZ and Haq JA.
Decrease of antibiotic resistance in Salmonella typhi isolated from
patients attending hospitals of Dhaka City over a 3-year period. International
Journal of Antimicrobial Agents 2000; 16: 249-251.
4.&amp;nbsp; Threlfall EJ, Ward LR,
Skinner JA, et al. Ciprofloxacin-resistant Salmonella typhi and
treatment failure. Lancet 1999; 353: 1590–1.
6.&amp;nbsp; Wain J, Hoa NT, Chinh NT, et
al. Quinolone-resistant Salmonella typhi in Vietnam: molecular basis
of resistance and clinical response to treatment. Clin Infect Dis 1997; 25:
1404–10.
8.&amp;nbsp; Rahman MM, Haq JA, Hossain
MA, Sultana R, Islam F, Islam AHMS. Prevalence of extended-spectrum- b lactamase-producing Escherichia coli and Klebsiella
pneumoniae in an urban hospital in Dhaka, Bangladesh, International
Journal of Antimicrobial Agents 2004; 24:508-510.
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