In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates

Introduction: Acute respiratory infections (ARI) contribute to more than 75% of health care seeking in primary health care facilities in India. Respiratory tract infections (RTIs) are managed frequently by β-lactam, macrolide and fluroquinolone class of antibiotics. However, these recommended cl...

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Main Authors: Saiprasad Vilas Patil, Anoop Laxminarayan Hajare, Manjusha Patankar, K Krishnaprasad
Format: Article
Language:English
Published: JCDR Research and Publications Private Limited 2015-02-01
Series:Journal of Clinical and Diagnostic Research
Subjects:
Online Access:https://jcdr.net/articles/PDF/5560/12092_CE[Ra]_F(P)_PF1(NJAK)_PFA(AK)_PF2(PAK)_PF2(PAG)_u.pdf
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spelling doaj-ab2339ec9d1441c9bb2d5c334f874acc2020-11-25T03:24:36ZengJCDR Research and Publications Private LimitedJournal of Clinical and Diagnostic Research2249-782X0973-709X2015-02-0192DC13DC1510.7860/JCDR/2015/12092.5560In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical IsolatesSaiprasad Vilas Patil0Anoop Laxminarayan Hajare1Manjusha Patankar2K Krishnaprasad3Assistant Manager, Medical Services, Glenmark Pharmaceuticals Ltd, Andheri(E). Mumbai, India. Assistant Manager, Medical Services, Glenmark Pharmaceuticals Ltd, Andheri(E). Mumbai, India. Lecturer, Department of Pharmacology, D.Y. Patil Medical College, Navi Mumbai, India.Deputy General Manager, Medical Services, Glenmark Pharmaceuticals Ltd, Andheri(E). Mumbai, India. Introduction: Acute respiratory infections (ARI) contribute to more than 75% of health care seeking in primary health care facilities in India. Respiratory tract infections (RTIs) are managed frequently by β-lactam, macrolide and fluroquinolone class of antibiotics. However, these recommended classes of antibiotic have shown resistance in community settings. Antibiotic combinations may provide broader spectrum not only in terms of coverage but also to overcome multiple resistance mechanisms overcoming individual class limitations. Aim: The study aimed to determine In vitro interactions interpreted according to calculated fractional inhibitory concentration (FIC) index between cefixime and azithromycin against common respiratory clinical isolates. Materials and Methods: Forty four bacterial respiratory clinical isolates from microbiology department of tertiary care hospital from Mumbai were used to determine the minimum inhibitory concentration (MIC) values of cefixime and azithromycin. Synergy testing of cefixime combination with azithromycin was performed by checkerboard method. Interaction was determined according to calculated FIC index. Results: MIC values were ranging from 2–128 µg/ml and 0.24– 128 µg/ml for cefixime and azithromycin respectively against K.pneumoniae, M.catarrhalis, S.pneumoniae and H.influenzae isolates. All the tested isolates were resistant to cefixime. Azithromycin resistance was noted in all the isolates except six M. catarrhalis isolates. FIC index showed synergy and additive effect in 66% (29/44) and 34% (15/44) all bacterial clinical isolates. Maximum synergy between cefixime and azithromycin was observed against K. pneumoniae in 91% isolates. Conclusion: This is one of the first attempts to check the rationality of fixed dose antibiotic combination of cefixime and azithromycin in India market. Though results of this study cannot be generalized considering the limitations of low sample size and in vitro model, our data provides stepping stone for further validation of cefixime and azithromycin fixed dose combinations (FDCs) in clinical setting by conducting randomized controlled trials. We think that judicious and rational use of FDCs may help to reduce the risk of selection of further drug resistance along with better clinical outcome.https://jcdr.net/articles/PDF/5560/12092_CE[Ra]_F(P)_PF1(NJAK)_PFA(AK)_PF2(PAK)_PF2(PAG)_u.pdfacute respiratory infectionsfixed dose combinationfractional inhibitory concentration indexminimum inhibitory concentrationsynergy
collection DOAJ
language English
format Article
sources DOAJ
author Saiprasad Vilas Patil
Anoop Laxminarayan Hajare
Manjusha Patankar
K Krishnaprasad
spellingShingle Saiprasad Vilas Patil
Anoop Laxminarayan Hajare
Manjusha Patankar
K Krishnaprasad
In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
Journal of Clinical and Diagnostic Research
acute respiratory infections
fixed dose combination
fractional inhibitory concentration index
minimum inhibitory concentration
synergy
author_facet Saiprasad Vilas Patil
Anoop Laxminarayan Hajare
Manjusha Patankar
K Krishnaprasad
author_sort Saiprasad Vilas Patil
title In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
title_short In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
title_full In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
title_fullStr In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
title_full_unstemmed In Vitro Fractional Inhibitory Concentration (FIC) Study of Cefixime and Azithromycin Fixed Dose Combination (FDC) Against Respiratory Clinical Isolates
title_sort in vitro fractional inhibitory concentration (fic) study of cefixime and azithromycin fixed dose combination (fdc) against respiratory clinical isolates
publisher JCDR Research and Publications Private Limited
series Journal of Clinical and Diagnostic Research
issn 2249-782X
0973-709X
publishDate 2015-02-01
description Introduction: Acute respiratory infections (ARI) contribute to more than 75% of health care seeking in primary health care facilities in India. Respiratory tract infections (RTIs) are managed frequently by β-lactam, macrolide and fluroquinolone class of antibiotics. However, these recommended classes of antibiotic have shown resistance in community settings. Antibiotic combinations may provide broader spectrum not only in terms of coverage but also to overcome multiple resistance mechanisms overcoming individual class limitations. Aim: The study aimed to determine In vitro interactions interpreted according to calculated fractional inhibitory concentration (FIC) index between cefixime and azithromycin against common respiratory clinical isolates. Materials and Methods: Forty four bacterial respiratory clinical isolates from microbiology department of tertiary care hospital from Mumbai were used to determine the minimum inhibitory concentration (MIC) values of cefixime and azithromycin. Synergy testing of cefixime combination with azithromycin was performed by checkerboard method. Interaction was determined according to calculated FIC index. Results: MIC values were ranging from 2–128 µg/ml and 0.24– 128 µg/ml for cefixime and azithromycin respectively against K.pneumoniae, M.catarrhalis, S.pneumoniae and H.influenzae isolates. All the tested isolates were resistant to cefixime. Azithromycin resistance was noted in all the isolates except six M. catarrhalis isolates. FIC index showed synergy and additive effect in 66% (29/44) and 34% (15/44) all bacterial clinical isolates. Maximum synergy between cefixime and azithromycin was observed against K. pneumoniae in 91% isolates. Conclusion: This is one of the first attempts to check the rationality of fixed dose antibiotic combination of cefixime and azithromycin in India market. Though results of this study cannot be generalized considering the limitations of low sample size and in vitro model, our data provides stepping stone for further validation of cefixime and azithromycin fixed dose combinations (FDCs) in clinical setting by conducting randomized controlled trials. We think that judicious and rational use of FDCs may help to reduce the risk of selection of further drug resistance along with better clinical outcome.
topic acute respiratory infections
fixed dose combination
fractional inhibitory concentration index
minimum inhibitory concentration
synergy
url https://jcdr.net/articles/PDF/5560/12092_CE[Ra]_F(P)_PF1(NJAK)_PFA(AK)_PF2(PAK)_PF2(PAG)_u.pdf
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