| Literature DB >> 29617454 |
Fabio Tramuto1,2, Carmelo Massimo Maida1,2, Fanny Pojero1, Giuseppina Maria Elena Colomba1, Alessandra Casuccio1, Vincenzo Restivo1, Francesco Vitale1,2.
Abstract
Following the indication of the World Health Organization, a national plan for the elimination of measles was approved in Italy and this included the improvement of the molecular surveillance of measles viruses and the interruption of indigenous transmission of the disease. Nevertheless, large outbreaks continue to occur in almost all regions of the country, including Sicily. Here we describe the epidemiology and molecular dynamics of measles viruses as a result of the measles surveillance activity carried out by the "Reference Laboratory for Measles and Rubella" in Sicily over a 5-year period. Biological samples of 259 suspected measles cases were tested for viral RNA detection and a total of 223 (86.1%) were classified as laboratory confirmed. The median age of confirmed measles cases was 21.0 years and about half of them were adults aged 19 years and older. Overall, one-third of the patients showed clinical complications and these latter were more common among adults than children (44.9% vs. 25.7%). The vast majority of measles cases were unvaccinated (94.2%, n = 210). The phylogenetic analysis of 221 measles virus nucleotide sequences revealed sporadic detections of genotypes D4 and H1, while endemic circulation of genotypes D8 and B3 was documented. Genotype D8 was associated with epidemics occurred between 2013 and 2016, whereas genotype B3 was more recently introduced into Sicily characterizing the current measles outbreak. The results of this study confirm the autochthonous co-circulation of viral variants belonging to different genotypes during the study period, and emphasizes the need of measles surveillance programmes in order to investigate the viral dynamics, the pathways of disease transmission, and to eventually adapt the development of successfull vaccine formulations.Entities:
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Year: 2018 PMID: 29617454 PMCID: PMC5884552 DOI: 10.1371/journal.pone.0195256
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Reported measles cases by health settings, Sicily, March 2012—August 2017.
| Total | Confirmed | |||
|---|---|---|---|---|
| 161 (72.2) | 62 (27.8) | |||
| | 129 (49.8) | 111 (49.8) | 79 (49.1) | 32 (51.6) |
| | 130 (50.2) | 112 (50.2) | 82 (50.9) | 30 (48.4) |
| 14.0 (25.0) | 21.0 (26.0) | 13.0 (26.0) | 24.5 (26.0) | |
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| <1 | 13 (5.0) | 11 (4.9) | 6 (3.7) | 5 (8.1) |
| 1–4 | 71 (27.4) | 55 (24.7) | 50 (31.1) | 5 (8.1) |
| 5–9 | 28 (10.8) | 21 (9.4) | 14 (8.7) | 7 (11.3) |
| 10–18 | 25 (9.74) | 18 (8.1) | 14 (8.7) | 4 (6.4) |
| 19–29 | 64 (24.7) | 62 (27.8) | 40 (24.8) | 22 (35.5) |
| ≥30 | 58 (22.4) | 56 (25.1) | 37 (23.0) | 19 (30.6) |
p = 0.044
Laboratory confirmed measles cases by clinical complications and age-group, Sicily, March 2012—August 2017.
| Total | Age-group (years) | ||
|---|---|---|---|
| Children | Adults | ||
| | 143 (64.1) | 78 (74.3) | 65 (55.1) |
| | 80 (35.9) | 27 (25.7) | 53 (44.9) |
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Children, ≤18 years old; adults: >18 years old.
Complications are listed according to the PNEMoRc 2010–2015 [6]. Individual cases could have multiple complications and the percentages of each complication are calculated using as the denominator the total number of measles cases with at least one complication, n = 80.
Odds ratio = 2.35 (95%CI: 1.33–4.16), p = 0.003; multiple complications (children vs. adults), odds ratio = 2.29 (95%CI: 0.85–6.13), p = 0.100; children as reference.
Other: bronchitis (n = 2), hemorrhagic rash (n = 1), febrile seizures (n = 1), skin desquamation on the face (n = 1), leukopenia (n = 1).
Laboratory confirmed measles cases by vaccination status and age-group, Sicily, March 2012—August 2017.
| Number of confirmed measles cases, n (%) | Age-group (years) | ||||||
|---|---|---|---|---|---|---|---|
| Total | <1 | 1–4 | 5–9 | 10–18 | 19–29 | ≥30 | |
| | 210 (94.2) | 11 (100.0) | 50 (90.9) | 20 (95.2) | 16 (88.9) | 57 (91.9) | 56 (100.0) |
| | 13 (5.8) | 0 | 5 (9.1) | 1 (4.8) | 2 (11.1) | 5 (8.1) | 0 |
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Fig 1Neighbour-joining tree for measles nucleotide sequences beloging to genotypes A, D4 and H1.
MV strains detected in Sicily are shown in bold and blue color. The reference and named strains recommended by WHO are included for comparison and indicated in red color (plain and italic, respectively), together with GenBank accession numbers. The tree was based on nucleotide sequences encoding the C-terminus of the MV N gene and rooted on the WHO reference strain MVs/Madrid.SPA/94 SSPE [F].
Fig 3Neighbour-joining tree for measles nucleotide sequences beloging to genotypes A and B3.
MV strains detected in Sicily are shown in bold and blue color. The reference and named strains recommended by WHO are included for comparison and indicated in red color (plain and italic, respectively), together with GenBank accession numbers. The tree was based on nucleotide sequences encoding the C-terminus of the MV N gene and rooted on the WHO reference strain MVs/Madrid.SPA/94 SSPE [F]. All relevant information on genotype D8 Sicilian MV sequences included into groups A-E are reported in S1 Table.
Fig 2Neighbour-joining tree for measles nucleotide sequences beloging to genotypes D8.
MV strains detected in Sicily are shown in bold and blue color. The reference and named strains recommended by WHO are included for comparison and indicated in red color (plain and italic, respectively), together with GenBank accession numbers. The tree was based on nucleotide sequences encoding the C-terminus of the MV N gene and rooted on the WHO reference strain MVs/Madrid.SPA/94 SSPE [F]. All relevant information on genotype D8 Sicilian MV sequences included into groups A-D are reported in S1 Table.
Fig 4Timeline of measles genotypes and variants identified in Sicily during the surveillance period March 2012—August 2017.