• Research Article
  • |
  • Open Access

Nasal isolates of commensal Staphylococcus aureus and non-aureus species from healthy young adults in Valencia (Spain) and their resistance to chemotherapeutic agents

  • María Pilar Falomir;
    • Department of Microbiology and Ecology, University of Valencia, Spain
  • Almudena Jávega;
    • Department of Microbiology and Ecology, University of Valencia, Spain
  • Hortensia Rico;
    • Department of Microbiology and Ecology, University of Valencia, Spain
  • Daniel Gozalbo
    • Department of Microbiology and Ecology, University of Valencia, Spain

  • Corresponding Author(s): Daniel Gozalbo

  • Department of Microbiology and Ecology, Faculty of Pharmacy, University of Valencia, Avenida Vicent Andrés Estellés s/n, 46100, Burjassot, Spain

  • Daniel.gozalbo@uv.es

  • +34-963543026

  • Gozalbo D (2018).

  • This Article is distributed under the terms of Creative Commons Attribution 4.0 International License

Received : Mar 05, 2018
Accepted : May 11, 2018
Published Online : May 17, 2018
Journal : Annals of Epidemiology and Public health
Publisher : MedDocs Publishers LLC
Online edition : http://meddocsonline.org

Cite this article: Gozalbo D, Falomir MP, Jávega A, Rico H. Nasal isolates of commensal Staphylococcus aureus and non-aureus species from healthy young adults in Valencia (Spain) and their resistance to chemotherapeutic agents. A Epidemiol Public Health. 2018; 1: 1004.

Abstract

Objective: Methicillin-resistant S. aureus (MRSA) have been gradually disseminated causing serious nosocomial infections worldwide, and recently MRSA infections have emerged in healthy individuals. Besides, non-aureusstaphylococci can colonize humans and animals, and show a large proportion of methicillin resistant strains that can be transmitted between these hosts. The aim of this study was to determine the incidence of commensal Staphylococcus species in the nasal cavity of healthy young adults, and their resistance to methicillin and other antibiotics, as potential reservoirs for spreading disease and antibiotic resistance into the community.

Methods: Nasal carriage of S. aureus and other manitolfermenting non-aureus species was studied in 445 and 89 healthy volunteer university students (University of Valencia, Spain), respectively. Staphylococcus isolation, identification, and resistance tests to eight chemotherapeutic agents (ciprofloxacin, clindamycin, co-trimoxazole, erythromycin, gentamicin, mupirocin, oxacillin and vancomycin) were performed according to standard microbiological procedures.

Results: The nasal carriage rate was 22% for S. aureus (99 isolates from 445 students) and 13.5% for other manitol-fermenting non-aureus species (12 out of 89 students). Non-aureus isolates were identified as S. intermedius (7 isolates), S. saprophyticus (4 isolates), S. caprae (2 isolates), S. kloosii (1), S.warneri (1), and S. capitis (1). Interestingly, four students out of 89 (4,5%) were carriers of two Staphylococccus species. Methicillin-resistant isolates were 6% ( S. aureus ) and 25% (non-aureus species). Resistances to mupirocin and particularly to erythromycin were detected; no resistances to co-trimoxazole, ciprofloxacin, gentamicin and vancomycin were found.

Conclusion: There is a need to implement continued surveillance of MRSA dissemination within the community in order to improve MRSA prevention and control. We suggest that this surveillance should be not limited to S. aureus but extended to other Staphylococcus species to avoid the possibility of resistance transfer among non-S. aureus (most belonging to species normally found as commensals in animals) and S. aureus isolates.

Keywords: Antibiotic resistance; Nasal carriers; Commensal Staphylococcus ; University students; Young healthy adults

Introduction

      Staphylococcus aureus is a commensal bacterial species often found in skin and mucous membranes of healthy individuals; a significant percentage (20-30%) of human population are nasal carriers of S. aureus [1]. These healthy carriers constitute a reservoir of the pathogen, as most bacterial infections are caused by the patients’ own commensal microbiota. Colonization significantly increases the risk of infection in immune compromised patients which are frequently infected with the same strain they carry as a commensal. Therefore, hospitalized patients are often exposed to nosocomial infections by S. aureus , which is able to cause a plethora of diseases [2-4]. The clinical impact of S. aureus infections is enhanced by its potential to acquire antimicrobial resistance, with the development of resistance to methicillin as the most relevant concern. Over the last decades, Methicillin-resistant S. aureus (MRSA) have been gradually disseminated causing serious nosocomial infections worldwide, although it was considered as an uncommon community pathogen. However, more recently MRSA infections have emerged in healthy individuals with no obvious risk factors for its acquisition [2-6]. At present, community acquired MRSA is emerging worldwide, probably by disseminating from hospital environment, although not much is known about its transmissibility. Transmission of MRSA between companion animals and humans has been also suggested, as well as between specific livestock-associated MRSA and livestock veterinarians and farms workers [7-12]. The situation is more complex, as coagulase-positive staphylococci (CoPS) other than S. aureus , such as members of the S. intermedius group (mainly S. pseudointermedius ), show resistance to methicillin and are commensal species of companion animals that occasionally are found in human exposed to those animals [8-10,13-15]. Besides, the heterogeneous group of coagulase-negative staphylococci (CoNS), regarded as less pathogenic staphylococci , are now considered also as major nosocomial pathogens, which colonize humans and animals, show a large proportion of methicillin resistant strains, and a few studies suggest transmission between these hosts [8,10,15].

      In Spain, MRSA still continues to be an important nosocomial pathogen, although resistance to methicillin in clinical isolates appears to be stabilized both in S. aureus (25-30%) and CoNS (50-60%) [16]. However, the information concerning MRSA dissemination within the community, particularly in healthy individuals with no obvious risk factors for colonization, is still scant [17]. Similarly, there is a lack of information concerning colonization of healthy individuals by non-aureus staphylococci. Besides, in contrast to clinical isolates, antibiotic resistances of commensal isolates of S. aureus , and particularly of non-aureus isolates are largely unknown. Therefore, the aim of this study was to determine the incidence of commensal Staphylococcus species in the nasal cavity of healthy young adults (university students of the University of Valencia, Spain), and their resistance to methicillin and other antibiotics, in order to obtain relevant epidemiological data concerning the rate of healthy carriers of MRSA and other Staphylococcus species, as potential reservoirs for developing infections and spreading antibiotic resistance into the community.

Methods

      Nasal swabs were streaked on selective mannitol salt agar (Chapman mannitol) and incubated 24/48 h at 37°C for colony isolation. Manitol-fermenting isolates were routinely cultured and maintained on Tryticase Soy Agar (TSA). Staphylococcus species were identified by standard procedures: coagulase test using plasma rabbit (BioMerieux), agglutination test using the Staph plus Latex Kit (DiaMondiaL), and biochemical tests using the BBL Crystal Gram-Positive (GP) Identification (ID) system (Becton Dickinson). All isolates were identified with a confidence > 0.95. Antibiotic susceptibility was determined by disk diffusion methods according to standard microbiological procedures [18]. Disks of eight antibacterial chemotherapeutic agents commonly in clinical use against gram-positive bacteria were used (Liofilchem): ciprofloxacin 5µg, clindamycin 2µg, cotrimoxazole (trimethoprim/sulfamethoxazole) 25µg, erythromycin 15µg, gentamicin 10µg, mupirocin 200µg, oxacillin 1µg and vancomycin 30µg. The study of nasal S. aureus carriers is routinely included in the laboratory practice of the students of the Food Hygiene subject in the Nutrition and Human Dietetics degree (University of Valencia) (official teaching guide code 33954, available on line at the university website); participation in the study reported in this work was on strict volunteer basis (written consents were given) and all the personal information was kept anonymous.

Results

      A total of 99 isolates were identified as S. aureus , showing that 22% of healthy students (99 out of 445) were carriers of S. aureus as commensal bacteria in their nasal cavity. Six of these S. aureus isolates (6%) were found to be oxacillin (methicillin)- resistant.

      S. aureus isolates (n: 35, including five MRSA) from selected students (n: 89) were tested for resistance to other seven antibiotics (Table 1). Interestingly, none out of 35 isolates was resistant to ciprofloxacin, vancomycin, gentamicin, co-trimoxazole nor clindamycin. Two isolates showed resistance to mupirocin, whereas about 54% (19 isolates) were resistant to erythromycin. Only two isolates were resistant to two agents (oxacillin and erythromycin), whereas 11 isolates (31%) showed no resistances to the antibiotics tested.

table 1 Table 1

Table 1: Resistance to methicillin and other antibiotics in S. aureus and non-aureus Staphylococcus isolates from nasal cavity of selected young adults (n: 89).

      In our study, manitol-fermenting Staphylococcus isolates other than S. aureus were also identified in the above cited selected samples (n: 89). A total of 16 isolates were obtained from 12 carriers (13,5%, 12 out of 89 students). Six different species were identified: S. intermedius (7 isolates), S. saprophyticus (4 isolates), S. caprae (2 isolates), S. kloosii (1), S. warneri (1), and S. capitis (1). To gain more information about antibiotic resistances in these isolates, susceptibility tests to all eight antibiotics was assayed. Results (Table 1) showed that none out of 16 isolates was resistant to ciprofloxacin, vancomycin, gentamicin, nor co-trimoxazole; four isolates ( S. caprae , S. kloosii , S. warneri and S. intermedius ) showed resistance to methicillin (25%), whereas resistance to erythromycin was observed in nine isolates (55%: five S. intermedius , three S. saprophyticus , and one S. caprae ); three isolates ( S. intermedius ) showed resistance to mupirocin (19%), and only one isolate ( S. intermedius ) was resistant to clindamycin (6%); five isolates (31%) were resistant to two agents: erythromycin and either oxacillin (one S. caprae isolate), clindamycin (one S. intermedius isolate) or mupirocin (three S. intermedius isolates). Four isolates (25%) were susceptible to all antibiotic tested ( S. caprae, S. capitis, S. intermedius and S. saprophyticus ).

      Interestingly, four students (out of 89) were carriers of two Staphylocccus species in their nasal cavity (Table 2): S. saprophyticus and S. intermedius (one student), S. aureus and S. capitis (one student), S. aureus and S. intermedius (one student), and S. aureus and S. caprae (one students); in all cases isolates from the same individual did not share antibiotic resistance (students 1 and 4), other than erythromycin resistance (student 3) (Table 2).

table 2 Table 2

Table 2: Antibiotic resistances in Staphylococcus isolates from the same nasal cavities.

Discussion

      Our results confirm that a significant percentage (22%) of healthy young adults are nasal carriers of S. aureus , and show that 6% of the S. aureus isolates are resistant to methicillin, despite none of the volunteer students participating in the study had been exposed to risk factors for S. aureus colonization or antibiotic treatments for at least two months prior to their participation in the study. This percentage of resistance to methicillin is lower than that described for clinical isolates of S. aureus in Spain (around 28%) [16], and higher than the percentage of MRSA isolates from healthy students found in other countries (1.5-3%) [19,20] as well as to the percentage of MRSA found in individuals with no healthcare associated risks in European countries (0-2.1%) [17], whereas MRSA prevalence in community in Delhi area was found to be higher: 18.1% [21].

      Similarly, in our study resistance of S. aureus isolates to other antibiotics (clindamycin, gentamicin, and particularly ciprofloxacin) was also lower in isolates from healthy individuals (0%) than that described for clinical isolates in Spain (15%, 8% and 33%, respectively) [16]. Only resistance to erythromycin was increased in commensal isolates (about 54%) as compared to clinical isolates (28%). These observations point out that probably the relationship between S. aureus nasal isolates in the community and S. aureus from hospital environment is not obvious. Also methicillin resistance in non-aureus Staphylococcus isolates (25%) was lower than that reported in clinical isolates (51%), as well as resistances to clindamycin (6% versus 51%), gentamicin (0% versus 36%), co-trimoxazole (0% versus 23%) and ciprofloxacin (0% versus 43%), whereas resistance to erythromycin was similar in both commensal and clinical isolates [16]. Interestingly, resistance to mupirocin, the antibiotic commonly used to treat nasal carriers of S. aureus , was found both in S. aureus (6%) and non-aureus isolates (20%).

      These results suggest that the ability of S. aureus to develop resistance to methicillin (and other antibiotics) and to spread resistance within the community is limited, probably due to the absence of selective pressure to develop/select resistance outside hospital environment. In addition, as a significant percentage of individuals (13.5%) were nasal carriers of manitolfermenting non-aureus Staphylococcus species, the possibility of resistance transfer among non-S. aureus and S. aureus isolates colonizing the same individual should be considered (although in the few cases found in our study such a resistance transfer did not occur, as no common resistances were detected in these isolates). Since most non-aureus isolates belong to species normally found as commensals in animals (particularly S. intermedius in companion animals), genetic transfer of resistance determinants between animal (veterinary) and human isolates may represent a factor contributing to the spreading of methicillin resistances into the community. Therefore, due to the emergence of community acquired MRSA, there is a need to implement continued surveillance of MRSA dissemination within the community, as well as in livestock and companion animals, in order to improve MRSA prevention and control, and we suggest that this surveillance should be not limited to S. aureus but extended to other Staphylococcus species.

Acknowledgement

      Support from the University of Valencia (Research Funds) is acknowledged.

References

  1. Weidenmaier C, Goerke C, Wolz C. Staphylococcus aureus determinants for nasal colonization. Trends Microbiol. 2012; 20: 243-250.
  2. Dulon M, Haamann F, Peters C, Schablon A, Nienhaus A. MRSA prevalence in European healthcare settings: a review. BMC Infect Dis. 2011; 11: 138-151.
  3. Otto M. MRSA virulence and spread. Cell Microbiol. 2012; 14: 1513-1521.
  4. Tong SYC, Davis JS, Eichemberger E, Holland TL, Fowler VC Jr. Staphylococcus aureus infections: epidemiology, pathophysiology, clinical manifestations, and management. Clin Microbiol Rev. 2015; 28: 603-661.
  5. Chambers HF, DeLeo FR. Waves of resistance: Staphylococcus aureus in the antibiotic era. Nat Rev Microbiol. 2009; 7: 629- 641.
  6. DeLeo FR, Chambers HF. Reemergence of antibiotic-resistant Staphylococcus aureus in the genomic era. J Clin Invest. 2009; 119: 2464-2474.
  7. Couto N, Belas A, Kadlec K, Schwarz S, Pomba C. Clonal diversity, virulence patterns and antimicrobial and biocide susceptibility among human, animal and environmental MRSA in Portugal. J Antimicrob Chemother. 2015; 70: 2483-2487.
  8. Rodrigues AC, Belas A, Marques C, Cruz L, Gama LT, Pomba C. Risk factors for nasal colonization by methicillin-resistant staphylococci in healthy humans in professional daily contact with companion animals in Portugal. Microb Drug Resist. 2018: 434- 446.
  9. Gómez-Sanz E, Torres C, Ceballos S, Lozano C, Zaragaza M. Clonal dynamics of nasal Sthaphylococcus aureus and Staphylococcus pseudointermedius in dog-owning household members. Detection of MSSA ST398. PLoS ONE. 2013; 8: e69337.
  10. Pomba C, Rantala M, Greko C, Baptiste KE, Catry B, van Duijkeren E, et al. Public health risk of antimicrobial resistance transfer from companion animals. J Antimicrob Chemoter. 2017; 72: 957-968.
  11. Rinsky JL, Nadimpalli M, Wing S, Hall D, Baron D, Price LB, et al. Livestock-associated methicillin and multidrug resistant Staphylococcus aureus is present among industrial, not antibiotic-free livestock operation workers in North Carolina. PLoS ONE. 2013; 8: e67641.
  12. Schinasi L, Wing S, Augustino KL, Ramsey KM, Nobles DL, Richardson DB, et al. A case control study of environmental and occupational exposures associated with methicillin resistant Staphylococcus aureus nasal carriage in patients admitted to a rural tertiary care hospital in a high density swine region. Environ Health. 2014; 15: 54.
  13. Bond R, Loeffler A. What’s happened to Straphylococcus intermedius ? Taxonomic revision and emergence of multi-drug resistance. J Small Anim Pract. 2012; 53: 147-154.
  14. Kadlec K, Schwarz S. Antimicrobial resistance of Staphylococcus intermedius . Vet Dermatol. 2012; 23: 276-282.
  15. Becker K, Heilmann C, Peters G. Coagulase-negative staphylococci . Clin Microbiol Rev. 2014; 27: 870-926.
  16. Cercenado E. Epidemiology of the infection by resistant Grampositive microorganisms. Rev Esp Quimioter. 2016; 29(S1): 6-9.
  17. van Bijnen EME, Paget J, de Lange-de Klerk ESM, den Heijer CDJ, Versporten A, Stobberingh EE, et al. Antibiotic exposure and other risk factors for antimicrobial resistance in nasal commensal Staphylococcus aureus : an ecological study in 8 european countries. PLoS ONE. 2015; 10: e0135094.
  18. Clinical and Laboratory Standards Institute (CLSI). Detection of methicillin-resistant staphylococci . 3rd ed. Wayne, PA: CLSI. 2018.
  19. Wang HK, Huang CY, Chen CJ, Huang YC. Nasal Staphylococcus aureus carriage among college student athletes in northern Taiwan. J Microbiol Immunol Infect. 2017; 50: 537-540.
  20. Morita JE, Fujioka RS, Tice AD, Berestecky J, Sato D, Seifried SE, et al. Survey of methicillin-resistant Staphylococcus aureus (MRSA) carriage in healthy college students, Hawai’i. Hawaii Med J. 2007; 66: 213-215.
  21. Saxena S, Singh K, Talwar V. Methicillin-resistant Staphylococcus aureus prevalence in community in the east Delhi area. Jpn J Infect Dis. 2003; 56: 54-56.

MedDocs Publishers

We always work towards offering the best to you. For any queries, please feel free to get in touch with us. Also you may post your valuable feedback after reading our journals, ebooks and after visiting our conferences.

CONTACT US