Journal of Clinical and Diagnostic Research, ISSN - 0973 - 709X

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MBBS, MD (Pathology),
Sanjay Gandhi institute of trauma and orthopedics,
Bengaluru.
On Aug 2018




Dr. Mamta Gupta,
"It gives me great pleasure to be associated with JCDR, since last 2-3 years. Since then I have authored, co-authored and reviewed about 25 articles in JCDR. I thank JCDR for giving me an opportunity to improve my own skills as an author and a reviewer.
It 's a multispecialty journal, publishing high quality articles. It gives a platform to the authors to publish their research work which can be available for everyone across the globe to read. The best thing about JCDR is that the full articles of all medical specialties are available as pdf/html for reading free of cost or without institutional subscription, which is not there for other journals. For those who have problem in writing manuscript or do statistical work, JCDR comes for their rescue.
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Reviewing articles is no less a pain staking process and requires in depth perception, knowledge about the topic for review. It requires time and concentration, yet I enjoy doing it. The JCDR website especially for the reviewers is quite user friendly. My suggestions for improving the journal is, more strict review process, so that only high quality articles are published. I find a a good number of articles in Obst. Gynae, hence, a new journal for this specialty titled JCDR-OG can be started. May be a bimonthly or quarterly publication to begin with. Only selected articles should find a place in it.
An yearly reward for the best article authored can also incentivize the authors. Though the process of finding the best article will be not be very easy. I do not know how reviewing process can be improved. If an article is being reviewed by two reviewers, then opinion of one can be communicated to the other or the final opinion of the editor can be communicated to the reviewer if requested for. This will help one’s reviewing skills.
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Dr. Mamta Gupta
Consultant
(Ex HOD Obs &Gynae, Hindu Rao Hospital and associated NDMC Medical College, Delhi)
Aug 2018




Dr. Rajendra Kumar Ghritlaharey

"I wish to thank Dr. Hemant Jain, Editor-in-Chief Journal of Clinical and Diagnostic Research (JCDR), for asking me to write up few words.
Writing is the representation of language in a textual medium i e; into the words and sentences on paper. Quality medical manuscript writing in particular, demands not only a high-quality research, but also requires accurate and concise communication of findings and conclusions, with adherence to particular journal guidelines. In medical field whether working in teaching, private, or in corporate institution, everyone wants to excel in his / her own field and get recognised by making manuscripts publication.


Authors are the souls of any journal, and deserve much respect. To publish a journal manuscripts are needed from authors. Authors have a great responsibility for producing facts of their work in terms of number and results truthfully and an individual honesty is expected from authors in this regards. Both ways its true "No authors-No manuscripts-No journals" and "No journals–No manuscripts–No authors". Reviewing a manuscript is also a very responsible and important task of any peer-reviewed journal and to be taken seriously. It needs knowledge on the subject, sincerity, honesty and determination. Although the process of reviewing a manuscript is a time consuming task butit is expected to give one's best remarks within the time frame of the journal.
Salient features of the JCDR: It is a biomedical, multidisciplinary (including all medical and dental specialities), e-journal, with wide scope and extensive author support. At the same time, a free text of manuscript is available in HTML and PDF format. There is fast growing authorship and readership with JCDR as this can be judged by the number of articles published in it i e; in Feb 2007 of its first issue, it contained 5 articles only, and now in its recent volume published in April 2011, it contained 67 manuscripts. This e-journal is fulfilling the commitments and objectives sincerely, (as stated by Editor-in-chief in his preface to first edition) i e; to encourage physicians through the internet, especially from the developing countries who witness a spectrum of disease and acquire a wealth of knowledge to publish their experiences to benefit the medical community in patients care. I also feel that many of us have work of substance, newer ideas, adequate clinical materials but poor in medical writing and hesitation to submit the work and need help. JCDR provides authors help in this regards.
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Thanking you
With sincere regards
Dr. Rajendra Kumar Ghritlaharey, M.S., M. Ch., FAIS
Associate Professor,
Department of Paediatric Surgery, Gandhi Medical College & Associated
Kamla Nehru & Hamidia Hospitals Bhopal, Madhya Pradesh 462 001 (India)
E-mail: drrajendrak1@rediffmail.com
On May 11,2011




Dr. Shankar P.R.

"On looking back through my Gmail archives after being requested by the journal to write a short editorial about my experiences of publishing with the Journal of Clinical and Diagnostic Research (JCDR), I came across an e-mail from Dr. Hemant Jain, Editor, in March 2007, which introduced the new electronic journal. The main features of the journal which were outlined in the e-mail were extensive author support, cash rewards, the peer review process, and other salient features of the journal.
Over a span of over four years, we (I and my colleagues) have published around 25 articles in the journal. In this editorial, I plan to briefly discuss my experiences of publishing with JCDR and the strengths of the journal and to finally address the areas for improvement.
My experiences of publishing with JCDR: Overall, my experiences of publishing withJCDR have been positive. The best point about the journal is that it responds to queries from the author. This may seem to be simple and not too much to ask for, but unfortunately, many journals in the subcontinent and from many developing countries do not respond or they respond with a long delay to the queries from the authors 1. The reasons could be many, including lack of optimal secretarial and other support. Another problem with many journals is the slowness of the review process. Editorial processing and peer review can take anywhere between a year to two years with some journals. Also, some journals do not keep the contributors informed about the progress of the review process. Due to the long review process, the articles can lose their relevance and topicality. A major benefit with JCDR is the timeliness and promptness of its response. In Dr Jain's e-mail which was sent to me in 2007, before the introduction of the Pre-publishing system, he had stated that he had received my submission and that he would get back to me within seven days and he did!
Most of the manuscripts are published within 3 to 4 months of their submission if they are found to be suitable after the review process. JCDR is published bimonthly and the accepted articles were usually published in the next issue. Recently, due to the increased volume of the submissions, the review process has become slower and it ?? Section can take from 4 to 6 months for the articles to be reviewed. The journal has an extensive author support system and it has recently introduced a paid expedited review process. The journal also mentions the average time for processing the manuscript under different submission systems - regular submission and expedited review.
Strengths of the journal: The journal has an online first facility in which the accepted manuscripts may be published on the website before being included in a regular issue of the journal. This cuts down the time between their acceptance and the publication. The journal is indexed in many databases, though not in PubMed. The editorial board should now take steps to index the journal in PubMed. The journal has a system of notifying readers through e-mail when a new issue is released. Also, the articles are available in both the HTML and the PDF formats. I especially like the new and colorful page format of the journal. Also, the access statistics of the articles are available. The prepublication and the manuscript tracking system are also helpful for the authors.
Areas for improvement: In certain cases, I felt that the peer review process of the manuscripts was not up to international standards and that it should be strengthened. Also, the number of manuscripts in an issue is high and it may be difficult for readers to go through all of them. The journal can consider tightening of the peer review process and increasing the quality standards for the acceptance of the manuscripts. I faced occasional problems with the online manuscript submission (Pre-publishing) system, which have to be addressed.
Overall, the publishing process with JCDR has been smooth, quick and relatively hassle free and I can recommend other authors to consider the journal as an outlet for their work."



Dr. P. Ravi Shankar
KIST Medical College, P.O. Box 14142, Kathmandu, Nepal.
E-mail: ravi.dr.shankar@gmail.com
On April 2011
Anuradha

Dear team JCDR, I would like to thank you for the very professional and polite service provided by everyone at JCDR. While i have been in the field of writing and editing for sometime, this has been my first attempt in publishing a scientific paper.Thank you for hand-holding me through the process.


Dr. Anuradha
E-mail: anuradha2nittur@gmail.com
On Jan 2020

Important Notice

Original article / research
Year : 2022 | Month : March | Volume : 16 | Issue : 3 | Page : DC06 - DC09 Full Version

Rising Minimum Inhibitory Concentration of Azithromycin: A Therapeutic Challenge in Treating Enteric Fever


Published: March 1, 2022 | DOI: https://doi.org/10.7860/JCDR/2022/51989.16059
Sandhya K Bhat, K Ravichandran, Reba Kanungo

1. Professor, Department of Microbiology, Pondicherry Institute of Medical Sciences, Puducherry, India. 2. Assistant Professor, Department of Biostatistics, Pondicherry Institute of Medical Sciences, Puducherry, India. 3. Professor Emeritus, Department of Microbiology, Pondicherry Institute of Medical Sciences, Puducherry, India.

Correspondence Address :
Dr. Sandhya K Bhat,
Professor, Department of Microbiology, Pondicherry Institute of Medical Sciences, Ganapathichettikulam, Puducherry, India.
E-mail: sandhyabhatk@gmail.com

Abstract

Introduction: Enteric fever continues to be endemic in the Indian subcontinent carrying with it significant morbidity, despite available antibiotics. With changing trends in antibiotic use, concern for emerging resistance to many common pathogens is very common. Taking enteric fever, as a case in point, there is evidence of increased use of azithromycin and third-generation cephalosporins. Documenting evidence of increasing concentrations of antibiotics, required to inhibit the organism, is necessary to alter the prescribing practice and to adopt course correction. This is required to modify antibiotic policies in health care setups both for the management of antibiotic susceptible and resistant cases of enteric fever.

Aim: To document the rising Minimum Inhibitory Concentration (MIC) of azithromycin among Salmonella isolates.

Materials and Methods: A cross-sectional study was conducted in Pondicherry Institute of Medical Sciences for a period of seven years (January 2014 to December 2020). A total of 168 clinical isolates from enteric fever cases were tested for drug resistance to azithromycin by disk diffusion as per Clinical and Laboratory Standards Institute (CLSI) guidelines. The MIC was estimated using the Epsilometer test. Results were interpreted as per CLSI 2020 guidelines. Spearman’s rank correlation coefficient (r) and two-tailed p-values were estimated to note the trend.

Results: Out of 168 Salmonella isolates, 65 were Salmonella Typhi and 103 were Salmonella Paratyphi A. The MIC of these isolates ranged from 1.5-64 μg/mL and three isolates were resistant to azithromycin with MIC ≥32 μg/mL and nine isolates had a high level of MIC of 24 μg/mL. Disc diffusion test results were consistent with MIC of azithromycin against Salmonella isolates from enteric fever. Regression coefficient for MIC for the given value of zone diameter for 65 Salmonella Typhi isolates was -0.579 (p<0.001, considered highly significant) and -0.475 (p<0.01, considered as significant) for Salmonella Paratyphi A isolates. Rising MIC to azithromycin was observed among Salmonella isolates over a period of seven years.

Conclusion: There is a need to monitor the rising trend of MIC, which may pose a therapeutic challenge for treating enteric fever cases in near future. Regular MIC estimation can pre-empt overt resistance. Hence, MIC testing should be routinely done where facilities are available than doing only disk diffusion testing for enteric fever isolates.

Keywords

Antibiotic, Rising trend, Salmonella

Enteric fever is an important public health challenge globally, with a burden of approximately 12 million cases and about 1,30,000 deaths every year (1). Mortality is as high as 30% in untreated or partially treated cases hence antibiotic therapy remains the mainstay of management; bringing down mortality to less than 1% with appropriate therapy is required (2). Appropriate and timely antimicrobial therapy is a therapeutic challenge, with reports of rising Multidrug Resistant (MDR) strains leading to treatment failures (3).

Current practice of management of enteric fever includes azithromycin and ceftriaxone as front line antibiotics. These antibiotics with spectrum of activity extending to management of various life threatening infections like meningitis, pneumonia and recently Coronavirus Disease 2019 (COVID-19) respiratory complications; in addition to the antibiotics being costly. Additionally, treatment with ceftriaxone requires hospitalisation as it is administered intravenously, with prolonged period of defervescence (4). However, use of azithromycin has increased in the recent years, as it is thought to be clinically efficacious in cases who do not respond to oral administration is an added advantage; making it a superior antibiotic for outpatient management. Recent reports of decreased susceptibility to these agents have led to the fear of re-emergence of untreatable enteric fever (5),(6),(7).

As azithromycin is a part of the regimen for treatment of enteric fever, either alone or in combination with ceftriaxone in this tertiary care hospital, continual monitoring mechanism should be in place to document emerging resistance among Salmonella isolates reported by the laboratory. Therefore, present study was done to find MIC of azithromycin among Salmonella isolates with the objective to detect discrepancy, if any between the results of azithromycin disk diffusion and MIC method for interpreting the susceptibility of the clinical isolates of Salmonella, as it would directly impact patient care.

Material and Methods

The present cross-sectional study was conducted in Pondicherry Institute of Medical Sciences, Puducherry, India, after reviewed and cleared by the Institute Ethics Committee (IEC) for a waiver of consent (IEC No- RC/14/104). Consecutive sampling method was used for the study. As the work was on archived Salmonella isolates, waiver of consent was obtained.

Inclusion criteria: All consecutive (total of 168), Salmonella isolates from positive blood cultures with clinically suspected enteric fever cases, between January 2014 to December 2020 were included. Archived Salmonella isolates had been identified by the standard biochemical tests and serotyping (8).

Exclusion criteria: Repeat Salmonella isolates from the same patients were excluded from the study.

Antibiotic Susceptibility Testing

Antimicrobial susceptibility tests of the isolates which had been determined by Kirby Bauer disc diffusion method were reconfirmed for the present analysis. The antimicrobial agents tested were ampicillin (10 μg), ciprofloxacin (5 μg), ceftriaxone (30 μg), cotrimoxazole (25 μg), chloramphenicol (30 μg) and azithromycin (15 μg). The MIC of azithromycin was determined by Epsilometer (E) strip test method (Himedia, Mumbai, India). Escherichia coli ATCC 25922 was used as control for both the disc diffusion testing and for MIC estimation. Results were interpreted as per CLSI 2020 and EUCAST 2020 guidelines (9),(10). As per CLSI 2020, the zone interpretative criteria for azithromycin susceptible isolates is ≤12 mm and resistant isolates is ≥13 mm and azithromycin MIC of ≥32 μg/mL is resistant and ≤16 μg/mL is considered as susceptible (9).

Statistical Analysis

Data analysis was undertaken using the Microsoft Excel and Statistical Package for the Social Sciences (SPSS) software version 20.0. Spearman’s rank correlation coefficient and regression coefficient (by linear regression) between disc diffusion and MIC for azithromycin was calculated, taking MIC as a dependent variable and zone diameter by disc diffusion as an independent variable. A p-value of 0.05 or below was considered significant. The p-value was calculated using Spearman’s rho test for correlation and F test for regression analysis. All the tests were two-sided.

Results

Of 168 Salmonella isolates from blood, 65 isolates (38.7%) were Salmonella Typhi and 103 were (61.3%) were Salmonella Paratyphi A. While majority of patients were males, 114 (68%), a male to female ratio of 2.1:1 was noted. Age of the patients ranged from 3-69 years, with majority of patients (76, 45.2%) of 21-30 years, followed by 47 (28%) in the age group of 31-40 years, 28 (16.6%) in 11-20 years, 6 (3.6%) each in the age group of ≤10 years and 41-50 years, 4 (2.4%) of 51-60 years and 1 (0.6%) patient of >60 years. Between 2016 to 2018; there was a surge in cases with Salmonella Paratyphi A. However, Salmonella Typhi remained the predominant isolate in rest of the years (Table/Fig 1).

All Salmonella isolates (n=168) were uniformly susceptible to ampicillin, cotrimoxazole, chloramphenicol, and ceftriaxone; whereas 38 isolates were resistant and 127 were intermediately susceptible to ciprofloxacin. Only three isolates were susceptible to ciprofloxacin by disk diffusion method. Azithromycin resistance was detected in three isolates of Salmonella Paratyphi A while remaining 165 isolates were uniformly susceptible (with varying zones of inhibition). The MIC of azithromycin among these isolates ranged from 1.5-64 μg/mL. Maximum number of isolates 125/168 (74%) had MIC ranging between 6-12 μg/mL. Three isolates were resistant to azithromycin with MIC ≥32 μg/mL and nine isolates had high level of MIC of 24 μg/mL. Disk diffusion testing (zone of inhibition-15 mm) and MIC (16 μg/mL) of azithromycin for one Salmonella Typhi isolate is shown in (Table/Fig 2). The MIC distribution of azithromycin among 168 Salmonella isolates is shown in (Table/Fig 3), (Table/Fig 4).

The MIC for azithromycin among Salmonella Typhi isolates (n=65) ranged from 1.5-24 μg/mL and corresponding zone standardised regression coefficient (Beta) for MIC for given value of zone diameter was -0.579 (p<0.001, considered significant). If zone of inhibition is reduced by 1 mm, then corresponding MIC also increases for azithromycin. However, MIC and zone diameters for azithromycin had significant negative correlation (r=-0.549; R2=0.301, p<0.01, which was significant).

The MIC for azithromycin among Salmonella Paratyphi A isolates (n=103) ranged from 1.5-64 μg/mL and corresponding zone standardised regression coefficient (Beta) for MIC for given value of zone diameter was -0.646 (p<0.001, considered significant). However, MIC and zone diameters for azithromycin had significant negative correlation (r=-0.475; p<0.01, considered as significant) in case of Salmonella Paratyphi A. Overall comparison of MIC with zone diameter by disk diffusion of azithromycin among Salmonella isolates (n=168) is shown in (Table/Fig 5).

Discussion

Antimicrobial susceptibility reports serve as a guide to clinicians for selecting most appropriate therapeutic agent. In the present study, all the Salmonella isolated over a period of seven years were found to be sensitive to chloramphenicol, cotrimoxazole, ampicillin, ceftriaxone and another welcome finding was that none were MDR. These findings were consistent with findings of Srirangaraj S et al., and Garg A et al., (4),(6). A previous study by Bhat KS et al., also correlated well the present findings (7). On the contrary a study conducted by Menezes GA et al., from Pondicherry in 2011 showed a high level (22%) of Salmonella Typhi isolates being MDR (11).

In the last two decades, emergence of MDR strains of Salmonella, worldwide has led to withdrawal of ampicillin, cotrimoxazole and chloramphenicol from the therapeutic regimen for enteric fever and has been replaced by ciprofloxacin, ceftriaxone and azithromycin. This probably has led to re-emergence of susceptibility to the earlier antibiotics, while emerging resistance with increase in the MIC of ciprofloxacin/ceftriaxone and azithromycin.

Azithromycin, till date has been an effective and suitable alternative to treat mild-to-moderate enteric fever. Due to optimum serum availability leading to high intracellular concentrations achieved by azithromycin early fever clearance, as well as lower rates of relapse has been documented following a course of 5-7 days of treatment with the drug (12). In a study conducted by Parry CM et al., Salmonella Typhi isolates with azithromycin MIC ranged between 4-16 μg/mL, showed very low clinical failure amounting to 8-11% (3). As MIC value of an antibiotic is a good predictor of in-vivo efficacy, it is thought to be a superior indicator for defervescence of fever than the disk diffusion method. A report relying on the latter may result in delayed therapeutic response probably leading to serious complications (12),(13).

The CLSI 2020 and EUCAST 2020 guidelines, give interpretation breakpoints by disk diffusion and by MIC for azithromycin susceptibility only for Salmonella Typhi but not for Salmonella Paratyphi A (9),(10). However, in present study Salmonella Typhi breakpoints was used to interpret the results for Salmonella Paratyphi A isolates also. In this study, only three isolates (Salmonella Paratyphi A) were resistant with MIC ≥32 μg/mL of azithromycin while the rest (165 isolates) were uniformly susceptible, with varying concentrations of inhibition ranging from 1.5-24 μg/mL. In the present study rising trend in the MIC distribution was observed (ranging from 1.5-24 μg/mL) over a period of first six years (from 2014 to 2019) among Salmonella isolates. Similar observations have been made by Parry CM et al., Das S et al., Bhat KS et al., and Archana M et al., (3),(5),(7),(14). However, in the year 2020, due to COVID-19 pandemic, only five Salmonella isolates were found. So rising trend in the azithromycin was not appreciated and this may expand the possible therapeutic options to treat MDR infections, eradicate the errors in forecasting therapeutic success in antibiotic susceptibility (15).

In the present study, resistance of azithromycin by disk diffusion correlated well with the MIC by E test for both the species showing significant negative correlation (r=-0.549, p<0.01 for Salmonella Typhi and r=-0.475; p<0.01 for Salmonella Paratyphi A).These results were consistent with other studies by Parry CM et al., Srirangaraj S et al., and Garg A et al., (3),(4),(16). Detecting the MIC routinely, has following advantages- first it has direct therapeutic impact, while Kirby Bauer method of reporting S, I, R may not actually reflect the exact inhibitory dose required for disease defervescence. Secondly, by mapping the MIC regularly would help in detecting rising trends through the drug concentrations creeping upwards. In the present study, as well as several others, Salmonella Paratyphi A is emerging as leading cause of enteric fever (3),(17),(18). As reported by Bhat KS et al., continuous monitoring of azithromycin MIC is important for early recognition of any emergence of resistance, and such cases can be treated by alternate options, to prevent treatment failures (7). In the absence of CLSI guidelines for cut-offs for Salmonella Paratyphi A, multicentric studies are required to establish uniform performance standards for both disk diffusion and MIC breakpoints. This will help to establish Indian standards to interpret azithromycin susceptibility against Salmonella Paratyphi A. Enteric fever continues to be a problem of the developing nations (2),(17),(18). Standards and interpretative criteria need to be formulated to suit local isolates and needs. This would help to improve consistency in reporting between laboratories in the region.

Limitation(s)

In the present study, small sample size has limited further analysis on rising trend of azithromycin MIC. There is need for more multicentric studies to establish uniform performance standards for azithromycin disk susceptibility testing and MIC estimation among Salmonella isolates, especially for Salmonella Paratyphi A. This would help to improve consistency between reporting laboratories and therapeutic utility of azithromycin for enteric fever cases.

Conclusion

Although a large proportion of Salmonella isolates from patients with enteric fever still continue to remain susceptible to azithromycin and ceftriaxone, there is a need to watch out for rising trend of MIC of azithromycin, which may pose a threat to future treatment of enteric fever. It is hoped that MIC estimation adopted as a routine antibiotic susceptibility test, will pre-empt overt resistance by implementing alternate therapeutic options. May be the time is now appropriate to recycle first-line anti-Salmonella antibiotics like ampicillin, cotrimoxazole and chloramphenicol to treat cases with enteric fever. As Salmonella Paratyphi A is emerging as a frequent cause of enteric fever, it is necessary to develop defined breakpoints for azithromycin for optimum therapeutic utility.

References

1.
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DOI and Others

DOI: 10.7860/JCDR/2022/51989.16059

Date of Submission: Aug 18, 2021
Date of Peer Review: Nov 24, 2021
Date of Acceptance: Jan 12, 2022
Date of Publishing: Mar 01, 2022

AUTHOR DECLARATION:
• Financial or Other Competing Interests: None
• Was Ethics Committee Approval obtained for this study? Yes
• Was informed consent obtained from the subjects involved in the study? No
• For any images presented appropriate consent has been obtained from the subjects. No

PLAGIARISM CHECKING METHODS:
• Plagiarism X-checker: Aug 19, 2021
• Manual Googling: Jan 11, 2022
• iThenticate Software: Jan 17, 2022 (11%)

ETYMOLOGY: Author Origin

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