| Literature DB >> 20031047 |
Johan Nordgren1, Elin Kindberg, Per Eric Lindgren, Andreas Matussek, Lennart Svensson.
Abstract
Norovirus (NoV) is recognized as the commonest cause of acute gastroenteritis among adults. Susceptibility to disease has been associated with histo-blood group antigens and secretor status; nonsecretors are almost completely resistant to disease. We report a foodborne outbreak of GI.3 NoV gastroenteritis that affected 33/83 (40%) persons. Symptomatic disease was as likely to develop in nonsecretors as in secretors (odds ratio [OR] 1.41, 95% confidence interval [CI] 0.46-4.36 vs. OR 0.71, 95% CI 0.23-2.18, p = 0.57). Moreover, no statistical difference in susceptibility was found between persons of different Lewis or ABO phenotypes. The capsid gene of the outbreak strain shares high amino acid homology with the Kashiwa645 GI.3 strain, previously shown to recognize nonsecretor saliva, as well as synthetic Lewis a. This norovirus outbreak affected persons regardless of secretor status or Lewis or ABO phenotypes.Entities:
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Year: 2010 PMID: 20031047 PMCID: PMC2874438 DOI: 10.3201/eid1601.090633
Source DB: PubMed Journal: Emerg Infect Dis ISSN: 1080-6040 Impact factor: 6.883
Figure 1Time to onset of symptoms after patient exposure to norovirus-contaminated food (n = 30), Sweden. Zero indicates the time point for serving and ingesting the contaminated food.
Distribution of histo-blood group antigens phenotypes and secretor status among 83 participants in a case–control study of a norovirus gastroenteritis outbreak in Sweden, 2007*
| Antigen and secretor status | No. (%) symptomatic persons, n = 33 | No. (%) asymptomatic/ nonexposed persons, n = 50† | Total no. (%) persons, n = 83 | Normal distribution, % (95% CI)†‡ |
|---|---|---|---|---|
| Blood type (n = 68) | ||||
| A | 14 (44) | 18 (56) | 32 (47) | 47 (37–56) |
| B | 2 (17) | 10 (83) | 12 (18) | 15 (8–22) |
| O | 10 (43) | 13 (57) | 23 (34) | 33 (23–40) |
| AB | 0 | 1 (100) | 1 (1) | 7 (2–12) |
| Lewis (n = 83) | ||||
| Lea+b– | 7 (58) | 5 (42) | 12 (14) | 18 (11–26) |
| Lea–b+ | 23 (38) | 38 (62) | 61 (73) | 76 (68–84) |
| Lea–b– | 3 (30) | 7 (70) | 10 (12) | 6 (1–10) |
| Secretor status (n = 83) | ||||
| Secretor§ | 26 (38) | 42 (62) | 68 (82) | 80 (72–88) |
| Nonsecretor | 7 (47) | 8 (53) | 15 (18) | 20 (12–28) |
*ABO blood group could only be determined for the 68 secretor-positive persons (26 symptomatic and 42 asymptomatic). CI, confidence interval. †p>0.15 ‡See Larsson et al. (27). §Homozygous and heterozygous.
Influence of secretor status, FUT2 polymorphism, and histo-blood group antigens on risk for norovirus GI.3 symptomatic infection, Sweden*
| Secretor status | OR (95% CI) | p value |
|---|---|---|
| Secretor, n = 68 | 0.71 (0.23–2.18) | 0.57 |
| Nonsecretor, n = 15 | 1.41 (0.46-4.36) | 0.57 |
| G/G (secretor), n = 35 | 0.67 (0.27–1.65) | 0.50 |
| G/A (secretor), n = 33 | 1.20 (0.49–2.95) | 0.82 |
| A/A (nonsecretor), n = 15 | 1.41 (0.46–4.36) | 0.57 |
| Histo-blood group antigens | ||
| Blood type,† n = 68 | ||
| A, n = 32 | 1.56 (0.58–4.16) | 0.46 |
| B, n = 12 | 0.27 (0.05–1.33) | 0.11 |
| O, n = 23 | 1.39 (0.50–3.89) | 0.60 |
| AB, n = 1 | Not applicable‡ | 1.0 |
| Lewis, n = 83 | ||
| Lea+b–, n = 12 | 2.42 (0.70–8.42) | 0.21 |
| Lea-b+, n = 61 | 0.73 (0.27–1.95) | 0.61 |
| Lea–b–, n = 10 | 0.61 (0.15–2.57) | 0.73 |
*FUT, fucosyltransferase; OR, odds ratio; CI, confidence interval. †Compared between secretors. ABO blood group could only be determined for the 68 secretor-positive persons. ‡No carrier of blood type AB was symptomatically infected with norovirus.
Relationship between clinical symptoms of norovirus infection and secretor status and blood type distribution among 83 participants in a case–control study of a norovirus gastroenteritis outbreak in Sweden, 2007*
| Data | No. (%) persons reporting symptom | |||
|---|---|---|---|---|
| Diarrhea | Vomiting | Joint pain | Headache | |
| Blood type | ||||
| A, n = 14 | 9 (64) | 12 (86) | 9 (64) | 7 (50) |
| B, n = 2† | 1 (50) | 0 (0) | 0 (0) | 0(0) |
| O, n = 9‡ | 6 (67) | 6 (67) | 4 (44) | 5 (56) |
| Secretor, n = 25‡ | 16 (64) | 18 (72) | 13 (52) | 12 (48) |
| Nonsecretor, n = 7 | 4 (57) | 5 (71) | 5 (71) | 2 (29) |
| Total | 20 (63) | 23 (72) | 18 (56) | 14 (44) |
*HBGA, histo-blood group antigen. †One person with HBGA type B experienced only nausea and stomachache. ‡One secretor-positive person with HBGA type O did not provide a description of symptoms.
Figure 2Phylogenetic analysis of amino acids of the norovirus capsid gene from the gastroenteritis outbreak in Jönköping, Sweden (JKPG, •) and reference strains. The tree was constructed using the neighbor-joining and Poisson correction methods, with MEGA 4.0 software (www.megasoftware.net). Bootstrap values are shown at the branch nodes (values <70% are not shown). Reference sequences were collected from Genbank and represent the 8 genotypes of GI as described by Zheng et al. (). Scale bar indicates nucleotide substitutions per site. NV-USA [M87661], Aich124-JPN [AB031013], SOV-GBR [L07418], C59-USA [AF435807], HLL219-USA [AF414403], Stav-Nor [AF145709], LR316-USA [AF414405], VA115-USA [AY038598], Kashiwa645-JAP [BD011871], PD196-DEU [AF439267], JKPG-SWE [FJ711163] DSV-USA [U04469], Chiba-JPN [AB042808], Valetta-MLT [AJ277616], Musgrove-GBR [AJ277614], SzUG1-JPN [AB039774], Hesse-DEU [AF093797], Wiscon-USA [AY502008], Wnchest-GBR [AJ277609], Boxer-USA [AF538679].