Emerging antimicrobial resistance and clinical relevance of Acinetobacter isolates in a tertiary care hospital of rural area of Punjab, India

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8|P age
Emerging antimicrobial resistance and clinical relevance
of Acinetobacter isolates in a tertiary care hospital of rural area of Punjab, India
POONAM SHARMA , YOUSUF UL BASHIR , SARJIWAN
KAUR , PARMEET KAUR , ARUNA AGGARWAL
1
2
1
1
1
Department of Microbiology, Sri Guru Ram Das Institute of Medical
1
Sciences and Research (SGRDIMSAR), Amritsar, Punjab, India
Received
09 March 2015
Accepted
18May 2015
ABSTRACT
Introduction
Acinetobacter baumannii can be found in the natural microbial flora of the human skin. Members of the genus
Acinetobacter have emerged from organisms of questionable pathogenicity to multidrug-resistant nosocomial
pathogens worldwide in the past two or three decades, especially since 2005-2006 [1]. There are more than 30 genomic types of Acinetobacter identified so far, of which
more than two third of Acinetobacter infections are due to
Acinetobacter baumannii. A. baumannii colonizes healthy
humans transiently at a low density on the warm and
moist skin of axilla, groin, between toes, throat, nares and
intestinal tract but it generally does not cause infection
[2]. Its clinical significance, especially over the last 15
years, has been propelled by its remarkable ability to up-
Objective: To carry out a study on Acinetobacter isolates
from various clinical samples in a tertiary care hospital in
India. To evaluate the prevalence of A. baumannii isolates, their antibiograms and clinical significance. Their
contribution as causative agents of nosocomial infections
has also been evaluated.
Methods: The clinical specimens over a period of 12
months from January 2013 to December 2013 were analyzed and the A. baumannii isolates obtained were further
studied. Their antibiograms were studied and a clinical
correlation was made to assess their pathogenic status.
Results: A. baumannii was isolated in 417 samples out
of 2116 gram negative isolates (19.7% prevalence) from
the entire hospital. Maximum isolates were from exudates & abscesses (41.5%) followed by respiratory secretions (28%). Overall resistance of A .baumannii towards
carbapenems was 25.65% from all hospital isolates. ICU
isolates showed higher resistance (62.6%) as compared to
Inpatient Department (35.5%) and Out-patient Department (1.86%).
Conclusions: In this study, A. baumannii isolates
showed pathogenic potential, however a majority were
found to be carbapenem sensitive. There was significant
correlation between the carbapenem resistant strains isolated from the intensive care units, in-patient and outpatient departments of the hospital.
KEY WORDS:
Emerging infection,
Antimicrobial resistance
A. baumannii
regulate or acquires resistance determinants, making it one
In the hospital environment, A. baumannii can colonize
of the organisms threatening the current antibiotic era.
the respiratory, urinary, gastrointestinal tract and wounds
Acting in synergy with this emerging resistance profile is
of the patients and cause infections in burn, trauma, me-
the ability of A. baumannii to survive for prolonged peri-
chanically ventilated and immunocompromised patients. It
ods throughout a hospital environment, thus potentiating
shows a special predilection for the ICUs [3]. The epide-
its ability for nosocomial spread.
miological, clinical, prognostic, and therapeutic characteristics of A. baumannii isolated from infected patients
Correspondence to: Dr Poonam Sharma
Email: : poonam136@rediffmail.com
have been studied widely in the last decade [4]. During
this period it was noted that A. baumannii has attained
JOURNAL OF MICROBIOLOGY AND ANTIMICROBIAL AGENTS. 2015; 1(1): 8-12
9|P age
resistance to most classes of known antibiotics posing a
The Acinetobacter isolates, thus identified were studied
great threat to our containment of the infection. A. bau-
for their antibiotic sensitivity patterns as shown in table1.
mannii can rapidly modify transmembrane proteins and
The antibiotics tested against the organism were amikacin,
efflux pumps to prevent current antibiotics from penetrat-
gentamicin, netilmicin, ciprofloxacin, levofloxacin, chlo-
ing its inner membrane and executing their mechanism of
ramphenicol,
action. Furthermore, the enhanced ability of A. baumannii
ceftazidime-clavulanic
to obtain DNA from the external environment has allowed
imipenem, colistin, polymyxin B and tigecycline. Chi-
the species to obtain novel drug and heavy metal ion re-
square test was used to analyse the significance of pres-
sistance genes. With resistance documented to all known
ence of carbapenem resistant isolates in ICU, IPD and
classes of antibiotics, as well as cellular mechanisms that
OPDs of the hospital. The role of A. baumannii as a path-
prevent desiccation and the action of antimicrobials, the
ogen or a colonizer in the respective infectious cases was
world is in great need of new antimicrobials that can elim-
determined by clinical correlation involving discussion
inate this dangerous pathogen. The most active agents in
with clinicians in order to assess the pathogenic status of
vitro against the multidrug resistant A. baumannii are-
the isolate.
ceftazidime,
acid,
cefotaxime,
ceftriaxone,
piperacillin-tazobactam,
polymyxin B, polymyxin E (Colistin) and tigecycline [5].
In this study, we report the prevalence of A. baumannii
Statistical analysis
isolates, their antibiograms and their clinical significance.
Chi-square test was used to analyses the results.
P<0.05was considered to be statically significant.
Materials and methods
This retrospective study was carried out in a tertiary care
Results
hospital over a period of 12 months from Jan to Dec 2013.
The culture samples from the entire hospital processed
Informed consent was taken from the patients. Samples
during the 12 month study period from Jan to Dec 2013
collected and processed during the course of routine diag-
were 11452. The antibiotic sensitivity patterns as shown in
nostic work up from patients in the intensive care units
table1. Of the total cultures processed, the number of
(ICUs), wards and outpatient department (OPD) of the
pathogenic bacterial isolates was 2966 (25.9%) which
hospital for the identification of pathogens using routine
constituted 2116 (71.3 %) gram negative and 850 (28.6%)
microbiological techniques were analyzed and consecu-
gram positive organisms. Overall, A. baumannii isolates
tive A. baumannii isolates were picked up for further
constituted 19.7% of the total gram negative load (417 out
studies. The specimens studied were urine, respiratory
of 2116). The majority of A. baumannii isolates were from
samples (sputum, and endo-tracheal aspirate), blood, pus,
exudates & abscess (41.5%) followed by respiratory se-
body fluids (pleural fluid, peritoneal & cerebrospinal fluid
cretions (28%), 49 in blood (11.7%), 72 in urine (17.2%)
etc). Specimens were plated using appropriate culture me-
and 6 in fluids as shown in Table 2. The carbapenem re-
dia. All Gram negative were processed for identification
sistance in these A. baumannii isolates was seen the most
and antibiotic sensitivity tests were performed by standard
in respiratory isolates (35.5%, Suction tips 32/90 R to
culture methods following CLSI guidelines [6]. Inclusion
imipenem) as compared to non-respiratory isolates. Of the
criteria: All gram negative coccobacilli, strictly aerobic,
417 isolates of A. baumannii from the entire hospital, 298
non-fermenting,
non-fastidious, non-motile, catalase-
belonged to the ICU (71.5%). The inpatient department
positive, oxidase-negative bacteria were taken as Acineto-
(IPD) and the outpatient department (OPD) contributed to
bacter isolates. Exclusion criteria: Gram negative bacilli,
19.6% (82 out of 417) and 8.8% (37 out of 417) of the
facultative anaerobes, fermenters, non-fastidious, non-
total A. baumannii isolates respectively. Overall resistance
motile/motile, catalase-positive, oxidase-negative as well
of A. baumannii towards carbapenems was 25.65% from
as Gram-negative bacilli, strictly aerobic, non-fermenting,
all hospital isolates.
non-fastidious, motile, catalase-positive and oxidase-
sistance as compared to Inpatient Department and Out-
positive bacteria were excluded from the study.
patient Department as shown in Table 3.
JOURNAL OF MICROBIOLOGY AND ANTIMICROBIAL AGENTS. 2015; 1(1): 8-12
ICU isolates showed higher re-
10 | P a g e
Table 1. Percentage of Acinetobacter strains sensitive to
various antibiotics.
ANTIBIOTICS
JAN–
MAR
(75)
APRJUN
(78)
JULSEP
(160)
OCTDEC
(104)
AMIKACIN
58
57
54
31.5
GENTAMICIN
35.7
33.9
31
16.4
NETILMICIN
57.9
55
54
52
CIPROFLOXACIN
7.7
7.5
17
13.7
LEVOFLOXACIN
13
13.3
17.4
41
CEFTRIAXONE
7.2
7.5
17
12
CEFTAZIDIME
13
13.2
12
8.2
CEFTAZIDIMECLAVULANIC ACID
23
21.5
34
16.4
PIPRACILLIN/ TAZOBACTUM
70
68
48
12.3
IMIPENEM
93
87
75
67
TIGECYCLINE
100
100
99.6
98.3
COLISTIN
100
100
100
98.6
POLYMYXIN B
100
100
100
100
Table 2. Prevalence of Acinetobacter isolates in different
clinical specimens.
Specimens
To assess whether A. baumannii was actually causing clinical infection or was an innocent bystander, a clinical correlation was done in the 298 isolates of A. baumannii in
the ICU. Of the total 298 isolates of A. baumannii from
the ICU, 250 (83.8%) proved to be pathogenic. Of the 112
isolates from respiratory samples in the ICU, 18 (16.07%)
appeared to be colonizers without contributing to the signs
and symptoms of infection and 94 (83.9%) contributed to
the infection. 90 out of 112 (80.3%) were clinically proven ventilator associated pneumonia (VAP) cases and 4
were admitted with community acquired infections. Of
these 90 isolates, 53 (58.8%) were proven as having been
acquired from our tertiary care hospital and 37 (41.1%)
were brought in at the time of admission from other hospitals. Of the 41 A. baumannii isolates from the blood, 29
(70.7%) were proven for their pathogenic status and in the
remaining 12 patients who showed no symptoms of blood
stream infection (BSI), the culture positivity may have
been due to contamination with A. baumannii colonized
on skin during sample collection . Of the samples isolated
from pus and drain fluid (110 isolates), 98 (89%) isolates
were proven as pathogens and rest of the 12 (11%) were
skin colonizers. Out of the 98 pathogens, 50 were attributed to having been hospital acquired from our tertiary
care centre, and 48 were brought in from the community
or other hospitals. Of the 29 isolates from urine, 24
(82.7%) were found pathogenic. Out of 24, 17 were observed as acquired from our tertiary care hospital and the
other 7 were community acquired. There existed significant (P<0.05) correlation between the presence of carbapenem resistant strains of Acinetobacter in the ICU,
OPD and IPD.
Total iso-
Isolates from
Colonisers from
lates
ICU
ICU
PUS
173
110 (36.9%)
12 (10.9%)
RESPIRATORY
117 (28%)
(41.5%)
72 (17.2%)
112 (37.6 %)
18 (16.07%)
URINE
29 (9.7%)
05 (17.24%)
BLOOD
49 (11.7%)
41 (13.8%)
12 (29.3%)
FLUIDS
06 (1.43%)
06 (2%)
01 (16.6%)
sponds to similar study carried out by H Siau et al [7]
TOTAL
417
298 (71.5%)
48 (16.1%)
where figures of A. baumannii isolates were 11% of the
Discussion
A. baumannii was isolated in 417 consecutive samples
forming 19.7% of the total gram-negatives. This corre-
total gram negative isolates. Of the total 417 isolates of A.
baumannii, a maximum relative percentage (41.5%) was
Table 3. Prevalence of Acinetobacter isolates & carbapenem resistance at different places in hospital.
obtained in exudates & abscesses followed by respiratory
secretions (28%). However in this study the ICU showed
the maximum yield of A. baumannii from the respiratory
SITE
TION
OF ISOLA-
NUMBER
ISOLATES
OF
PERCENTAGE
OF
CARBAPENEM RESISTANT ISOLATES
samples (37.6 %) followed by pus (36.9%) & blood
(13.8%). Siau et al [7] reported in their ICU isolates that
ICU
298 (71.5%)
62.6%
respiratory tract was the most common site from which
IPD
82 (19.6%)
35.5%
Acinetobacter was isolated. Villers et al [8] have also re-
OPD
37 (8.8%)
1.86%
ported a predominance of A. baumannii in tracheobron-
TOTAL
417
25.65%
chial secretions as 24.8% to 48.8% and Suri et al [9] as
JOURNAL OF MICROBIOLOGY AND ANTIMICROBIAL AGENTS. 2015; 1(1): 8-12
11 | P a g e
45.6% respectively in their studies. An attempt was made
last 3-5 years [14]. However, lower rates of carbapenem
in this study to distinguish clinical infection from coloni-
resistance have been reported in studies carried out by
zation. Of the total 298 isolates of A. baumannii from the
Knam Soo Koo et al as 8.3%. This could be explained by
ICU, 250 proved to be pathogenic (83.8%) This was done
their stringent antibiotic policies and judicious use of car-
by correlating various clinical and lab parameters and dis-
bapenems in their countries [14]. Earlier studies in India
cussion with the clinician. An analysis was also done of
have also reported lower resistance rates (9.8-18.5%) in A.
the pathogenic potential of A. baumannii in various sam-
baumannii. This study shows the carbapenem resistant
ples like respiratory secretions, blood, pus and body fluids
isolates are circulating among ICU, OPD & IPD areas of
and urine specimens. Of the 112 isolates of A. baumannii
hospital, to prevent this there is a need of enforcing strict
from respiratory secretions, 94 (83.9%) were recognized
infection control guidelines. This study also brings up an
as pathogens and rest were colonizers. Since this organism
important aspect of increasing resistance in A. baumannii
is a fast colonizer of the respiratory tract, its percentage
towards carbapenems [15]. The antibiotic susceptibility
can increase from 7% to 45% in a healthy subject to those
patterns clearly showed the increasing resistance of A.
on ventilators respectively [10]. Of the A. baumannii iso-
baumannii to various antibiotics as compared to other
lates from blood 70.7% were found to be pathogenic and
gram negatives. Colistin (Polymyxin E) is one agent
rest were the contaminants. As Acinetobacter cannot exist
which is active against A. baumannii. In the present study,
as a colonizer in blood, it would have a higher pathogenic
colistin resistance has been reported as 1.4% but all strains
potential at this site. We did isolate A. baumannii as con-
were sensitive to Polymyxin B as shown in table1. A re-
taminants in 29.3% cases. However, Lahiri et al [11] have
cent study of clinical isolates from the Western Pacific
reported 33% of A. baumannii isolates from blood as skin
region showed 3.3% resistance of A. baumannii to colistin
contaminants. Typically, patients with A. baumannii in-
[16]. Heteroresistance to colistin among A. baumannii
fections have had prolonged ICU stays [12], sources of
isolates has also been described in earlier reports [14]. In
bloodstream infection are usually line related or attributed
a study in Korea, there was high resistance to colistin
to underlying pneumonia, UTI, or wound infection. Pus
(30.6%) and polymyxin (18.1%) [14]. However, as the
and fluids analysis showed 89% of A. baumannii as path-
resistance against colistin/polymyxin is not very high in
ogens. Sengupta et al reported a lower isolation rate of
our country, it can still be used as the drug of choice
11.5% of A. baumannii from wounds [13]. High isolation
against multidrug resistant strains of A. baumannii. A.
rate in our hospital could be because of severely ill pa-
baumannii was sensitive to tigecycline in 99.47% cases in
tients coming into a tertiary care centre. This study also
present study which correlates well with the study by
showed seasonality in the occurrence of A. baumannii
Yilmaz F. F. et al., where 3.57% isolates were resistant to
infection during the one-year period, with a significantly
tigecycline [17]. However studies by Behara B. et al., in
greater number of infections occurring from July through
India have shown only 42% susceptibility in A. baumannii
September (160) .The reason for this seasonality is un-
isolates to tigecycline [18]. Since therapeutic options are
known. The antibiograms of the isolates of A. baumannii
limited for multidrug-resistant Acinetobacter infection, the
from the entire hospital showed 25.65% carbapenem re-
development or discovery of new therapies, well-
sistance in our study. When the isolates in the ICU were
controlled clinical trials of existing antimicrobial regimens
studied, the resistance to carbapenems rose to 62.6%
and combinations, and greater emphasis on the prevention
whereas in IPD it was 35.5%. However, a comparatively
of health care-associated transmission of multidrug-
very low carbapenem resistance of 1.86% was observed in
resistant Acinetobacter infection are essential. In 2006, the
A. baumannii in the community as represented by the
CDC released a report describing guidelines to prevent the
OPD isolates. Antibiotic resistance in A. baumannii is
transmission of MDR organisms. The steps the CDC rec-
increasing at an alarming rate leading to increased mor-
ommends all health care facilities take include improve-
bidity, mortality and treatment costs in ICU settings as
ment of hand hygiene, use of contact precautions until the
revealed by surveillance studies from Europe, the Asia
patient tests culture-negative for the target organism, ac-
Pacific region, Latin America and North America over the
tive surveillance cultures, education of hospital personnel,
JOURNAL OF MICROBIOLOGY AND ANTIMICROBIAL AGENTS. 2015; 1(1): 8-12
12 | P a g e
improved environmental cleaning, and better communica-
established in health care settings. The resistance patterns
tion about patients with these infections to not just per-
detected in Acinetobacter could reflect the antibiotic mis-
sonnel within the facility but also between facilities[19].
use and lack of regulations on the over the counter sale.
While A. baumannii may not be particularly virulent, it
Our study suggested that due to the increasing resistance
can cause unnecessary disease and expense in the critical-
of A. baumannii, we should judiciously use antibiotics by
ly ill patients affected by it, and the transmission of such a
making an attempt to distinguish colonization from infec-
pathogen should be limited. Measures to prevent the inter-
tions and treatment should be only given to the clinically
and intra-hospital transmission of A. baumannii must be
confirmed Acinetobacter infections.
Conflict of Interest
We declare that we have no conflict of interest.
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