Characterisation of S. aureus/MRSA CC1153 and review of mobile genetic elements carrying the fusidic acid resistance gene fusC

Stefan Monecke,Mayada Gwida,Rania Nassar,Sascha D Braun,Annett Reissig,Darius Gawlik,Antje Ruppelt-Lorz,Ali M Somily,Marc Armengol-Porta,Ines Engelmann,Elke Müller,Edet E Udo,Ralf Ehricht,Michèle Bes,Helmut Hotzel,Samar Boswihi,Abiola Senok,Maged El-Ashker

doi:10.1038/s41598-021-86273-4

Abstract

While many data on molecular epidemiology of MRSA are available for North America, Western Europe and Australia, much less is known on the distribution of MRSA clones elsewhere. Here, we describe a poorly known lineage from the Middle East, CC1153, to which several strains from humans and livestock belong. Isolates were characterised using DNA microarrays and one isolate from the United Arab Emirates was sequenced using Nanopore technology. CC1153 carries agr II and capsule type 5 genes. Enterotoxin genes are rarely present, but PVL is common. Associated spa types include t504, t903 and t13507. PVL-positive CC1153-MSSA were found in Egyptian cattle suffering from mastitis. It was also identified among humans with skin and soft tissue infections in Saudi Arabia, France and Germany. CC1153-MRSA were mainly observed in Arabian Gulf countries. Some isolates presented with a previously unknown SCCmec/SCCfus chimeric element in which a mec B complex was found together with the fusidic acid resistance gene fusC and accompanying genes including ccrA/B-1 recombinase genes. Other isolates carried SCCmec V elements that usually also included fusC. Distribution and emergence of CC1153-MRSA show the necessity of molecular characterization of MRSA that are resistant to fusidic acid. These strains pose a public health threat as they combine resistance to beta-lactams used in hospitals as well as to fusidic acid used in the community. Because of the high prevalence of fusC-positive MRSA in the Middle East, sequences and descriptions of SCC elements harbouring fusC and/or mecA are reviewed. When comparing fusC and its surrounding regions from the CC1153 strain to available published sequences, it became obvious that there are four fusC alleles and five distinct types of fusC gene complexes reminiscent to the mec complexes in SCCmec elements. Likewise, they are associated with different sets of ccrA/B recombinase genes and additional payload that might include entire mec complexes or SCCmec elements.

Highlights

Staphylococcus aureus (S. aureus) is a common coloniser, or pathogen, among humans as well as among wild and domestic animals
We describe a clonal complex of S. aureus that we identified in several Middle Eastern countries
A couple of publicly available genomes, deposited in GenBank (GenBank FQHT01000000) and/or the Short Read Archive (SAMEA2661948, SAMEA2661956, SAMEA2662240, SAMEA2662319, SAMEA2710354, SAMEA2710468, SAMEA3214613, SAMEA3448866, SAMEA3448996, SAMEA4547522, SAMN03289718) belong to it, but to the best of our knowledge, this clonal complex has not yet been reviewed. Three of these sequences originated from Thailand (GenBank FQHT01000000.1 as well as BioSamples SAMEA3448866 and SAMEA3448996), and one from the United Kingdom (SAMN03289718) while for the others, no locations were reported

Summary

Introduction

Staphylococcus aureus (S. aureus) is a common coloniser, or pathogen, among humans as well as among wild and domestic animals. Most closely related sequences of fusC-associated genes were identified in the S. aureus CC5 strain 06BA18369, GenBank ARXY, and in the Staphylococcus hominis subsp. These strains carry Q8CU82, tarF-SCC, A9UFT0, Q9KX75, Q7A207, Q7A206, ccrB-1, ccrA-1, cch-1, DUF1413, Q83ZD5, helicase M06, Q6GD51, D3QFP0-scc, D3JCW9, fusC, tnpIS150, tnp_A8YYY6, Q4LAG7-SCCfus and yobV (for explanations and GenBank entries of the genes discussed, see Table 1 and Supplemental File 4).

Results

Conclusion