Ciprofloxacin Multiple Dose for Adult Cholera
Mo kle
Abstrè
Deskripsyon
Cholera is caused by infection of the human intestine with Vibrio cholerae O1 or V. cholerae O139. It is a major health problem in many developing countries including Bangladesh.1 The importance of cholera as a worldwide public health problem is evident from the large number of countries affected by cholera epidemics.2 Data of the Diarrhoeal Disease Surveillance system of the Dhaka Hospital demonstrated that V. cholera O1 was the most frequently isolated pathogens (617/2,068 i.e. 30%) in patients attending the hospital with diarrhoeal illnesses in 2006. By extrapolating the number of patients enrolled in the surveillance system we estimate that over 30,000 out of the total 106,531 patients attending the hospital in 2006 had cholera- a huge number of patients indeed.
Like other diarrhoeal illnesses, prevention and management of dehydration using appropriate oral and/or intravenous fluids is the mainstay in the management of cholera, irrespective of severity. However, appropriate antimicrobial therapy is a very useful adjunct therapy that reduces the duration of diarrhoea, the volume of diarrhoeal stools (thus the amount of oral and intravenous fluids), and also the duration of faecal excretion of the pathogen, V. cholerae O1 and O139 by about 50%. 3-6 Based on these observations made in numerous clinical trials, routine use of an appropriate antimicrobial therapy is recommended in the management of severe cholera, both in adults and children. All three benefits, as described above, are very important in resources-constraint settings where cholera is endemic and also during epidemic outbreaks.
Nosocomial transmission of cholera has also been increasingly recognized as an important problem,7 and reducing the duration of excretion of Vibrio cholerae in the stool associated with appropriate antimicrobial therapy will presumably decrease the rate of nosocomial infection. Lastly, by shortening the course of illness, patients and their families' can more quickly return to their normal life, lessening their financial burden, which is of particular relevance to socio-economically disadvantaged population who disproportionately share the most of the disease burden from cholera.
From the time of the initial controlled trials of antimicrobial therapy for cholera, almost four decades ago,3 a number of antimicrobial agents have been evaluated to be useful in the treatment of cholera. Tetracycline, chloramphenicol, doxycycline, furazolidone and trimethoprim-sulfamethoxazole have all been found to be effective in the treatment of cholera when given in multiple doses for 3 days.8-14 Tetracycline and it's long-acting congener doxycycline are also effective when administered in a single 1 or 2 g and 200 or 300 mg oral doses respectively in adults.13, 14 Vomiting is a common problem in association with doxycycline therapy and the problem is greater when doxycycline is used in 300 mg dose (39%) compared to when 200 mg dose is used (30%); however, the therapeutic efficacy is better with the higher dose (mean duration of diarrhoea were 32h vs. 40h respectively.14
Antimicrobial resistance has now become an important problem in the clinical management of cholera. For example, in 2006 virtually all of the 683 clinical strains of V. cholerae O1 isolated from patients attending the Dhaka Hospital were multiply drug resistant with 100% resistance to ampicillin, furazolidone and co-trimoxazole, 83% to erythromycin and 85% to tetracycline.15 All V. cholerae strains remained susceptible to ciprofloxacin by disc-diffusion testing, but in E-test their MIC were noted to have increased from 0.002 µg/ml during 1993-2003 to 0.250-0.380 µg/ml in 2006
Resistance of V. cholerae to commonly used drugs such as tetracycline, doxycycline, furazolidone and trimethoprim-sulfamethoxazole have also been reported from Asia, Africa and Latin America,17-20 In the early 1990's increasing prevalence of V. cholerae resistant to antimicrobials commonly used in the treatment of cholera (tetracycline, ampicillin, co-trimoxazole) prompted our group and others to conduct series of trials to identify newer affective agents for treatment of cholera. We evaluated ciprofloxacin in both adult and children infected with V. cholerae O1 and O139, and observed very good rates of both clinical and bacteriological response when used in multiple doses or in a single dose administered only once.11, 21, 22
Ciprofloxacin, is a member of the class of drugs called fluoroquinolones, which act by blocking the action of bacterial DNA gyrase.23 This enzyme, which is not present in human cells, is responsible for supercoiling of bacterial DNA, an essential element for DNA functions.24 Without the three-dimensional DNA structure the cell is unable to replicate, and thus bacterial growth is rapidly halted. Ciprofloxacin is the most active of the fluorinated 4-quinolones (ciprofloxacin, norfloxacin, ofloxacin) against bacterial diarrhoea pathogens in-vitro as assessed by MIC. It has a relatively long serum half-life.25 Due to its multiple mechanisms of excretion toxic levels of quinolones do not usually accumulate in the body. Experience suggests that resistance against ciprofloxacin develops much more slowly than against the older quinolone agent such as nalidixic acid, as the rate of spontaneous mutation is much lower and multiple mutations are required to confer frank resistance.26, 27 Increases in the MIC, however, can occur with single mutation, and this is the likely sequence that has occurred among currently circulating V. cholerae isolates in Bangladesh.
Because of resistance to other agents and susceptibility of the isolates to ciprofloxacin in-vitro, disc diffusion tests, Dhaka and Matlab Hospitals of ICDDR, B changed their treatment policy (early 2005) to single-dose ciprofloxacin therapy for treatment of cholera irrespective of patients' age, except for cholera in pregnant women. However, experienced physicians at the Dhaka Hospital quickly noted sub-optimal clinical response to ciprofloxacin therapy- higher stool output and longer hospitalisation. A quick review of the clinical study that we recently published in the New England Journal of Medicine confirmed these findings.28 In that study only 26 (27%) of 98 patients who were infected with V. cholerae O1 experienced an optimal clinical response to single-dose ciprofloxacin, while only 10 (10%) of the 98 patients had a bacteriologic cure, as defined in the protocol. Eventual determination of MICs of the V. cholerae strains from that study revealed that the inferior clinical and bacteriological response to ciprofloxacin was associated with an increase in MIC values.29 Table 1 below shows the increase in ciprofloxacin MIC values that were observed during 1993-1994 when we first conducted clinical trials with ciprofloxacin to subsequent years including in 2005 when ciprofloxacin was first introduced for routine use in the treatment of cholera at the Dhaka Hospital. We can see, the median MICs has increased approximately one hundred folds between 1993 and 2006.
Dat
Dènye verifye: | 07/31/2008 |
Premye Soumèt: | 08/03/2008 |
Enskripsyon Estimasyon Soumèt: | 08/24/2008 |
Premye afiche: | 08/25/2008 |
Dènye Mizajou Soumèt: | 07/10/2011 |
Dènye Mizajou afiche: | 07/11/2011 |
Dat aktyèl kòmanse etid la: | 06/30/2007 |
Dat Estimasyon Prensipal Estimasyon an: | 09/30/2008 |
Dat estime fini etid la: | 05/31/2010 |
Kondisyon oswa maladi
Entèvansyon / tretman
Drug: 1
Drug: 2
Faz
Gwoup bra
Bra | Entèvansyon / tretman |
---|---|
Experimental: 1 Ciprofloxacin | Drug: 1 12 hourly oral dose of ciprofloxacin for 3 days |
Active Comparator: 2 Azithromycin | Drug: 2 1 gm Azithromycin single dose |
Kritè kalifikasyon yo
Laj ki kalifye pou etid | 18 Years Pou 18 Years |
Sèks ki kalifye pou etid | Male |
Aksepte Volontè Healthy | Wi |
Kritè | Inclusion Criteria: - Age: 18 - 60 years. - Gender: Male - Duration of diarrhoea: Not exceeding 24 hours - Written informed consent for participation. - Dehydration status: Severe dehydration. - Positive stool dark-field microscopic examination for V. cholerae & culture positive for V cholerae - For patients assigned to receive ciprofloxacin, an MIC of the V. cholerae isolates to ciprofloxacin of > 0.190 µg/ml and to azithromycin of ≤ 0.125 µg/ml. Exclusion Criteria: - History of receiving an antimicrobial agent known to be effective in cholera in adults. - Concomitant infection requiring antimicrobial therapy other than the study drugs. - Chronic illness. |
Rezilta
Mezi Rezilta Prensipal yo
1. To determine whether clinical success of therapy in the two treatment regimens are comparable. [48 hours]
Mezi Rezilta Segondè
1. Compare the rates of bacteriological success. Compare the diarrhea duration. Compare stool volume of patients. Measure stool concentrations of the two drugs and compare them with MICs of V. cholerae. Record and compare adverse events. [48 hours]