Prevalence of Pandemic Thermostable Direct Hemolysin-Producing
            <i>Vibrio parahaemolyticus</i>
            O3:K6 in Seafood and the Coastal Environment in Japan

Hara-Kudo, Yukiko; Sugiyama, Ken; Nishibuchi, Mitsuaki; Chowdhury, A. K. M. Alauddin; Yatsuyanagi, Jun; Ohtomo, Yoshimitsu; Saito, Akinobu; Nagano, Hidetoshi; Nishina, Takuya; Nakagawa, Hiroshi; Konuma, Hirotaka; Miyahara, Makoto; Kumagai, Shinya

doi:10.1128/aem.69.7.3883-3891.2003

Cited by 141 publications

(89 citation statements)

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“…While most strains and serotypes of V. parahaemolyticus are nonpathogenic, those that are pathogenic have rapidly become major etiologic agents of human gastroenteritis, wound infections, and septicemia. Since 1996, one serotype in particular, V. parahaemolyticus O3:K6 (and its clonal derivatives O4:K68, O1:K25, and O1:KUT) (7), has received increasing notoriety, as it is the first documented V. parahaemolyticus serotype to cause pandemic disease (19,24) and has recently been linked to gastroenteritis outbreaks on the Asian (6,11,24,40), North American (8,21), South American (10), European (18,31), and African (1) continents. To compound matters, serotype-based detection and surveillance efforts have been complicated by serotype transition and variation within the pandemic lineage, as additional serotypes (O1: K26 [26], O6:K18 [39], O1:K41, O4:K12 [16], O1:K56, O3:K75, O4:K8, O4:KUT, and O5:KUT [5]) from specific locales have now been identified as having been derived from the original pathogenic O3:K6 clone.…”

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confidence: 99%

Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

et al. 2007

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Vibrio parahaemolyticus is a halophilic bacterium capable of causing food-and waterborne gastroenteritis, wound infections, and septicemia in humans. The organism has recently received increasing attention, as the emergence of a new clone, V. parahaemolyticus O3:K6, has resulted in the first documented pandemic spread of V. parahaemolyticus. We used microarray analyses to explore the presence of known virulence factors and genetic markers thought to be specific for V. parahaemolyticus O3:K6 and its clonal derivatives. Analyses of 48 human clinical isolates collected between 1997 and 2005 revealed that the V. parahaemolyticus chromosome 2 type III secretion system is not specifically associated with pandemic strains and can be found in tdh-negative (i.e., Kanagawa-negative) clinical isolates. These results highlight the genetic dynamism of V. parahaemolyticus and aid in refining the genetic definition of the pandemic group members.

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Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

et al. 2007

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“…Moreover, the positive reaction of galactosidases (ONPG) indicated the identifiable characteristics feature of V. parahaemolyticus rather than sugar fermentation process i.e. sucrose [30]. Identification of V. parahaemolyticus with the help of PCR-based 16S rDNA technique is more efficient, reliable and faster in comparison with the conventional biochemical reaction pattern analysis [23].…”

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confidence: 99%

Biochemical Differentiation and Molecular Characterization of Biofield Treated <i>Vibrio parahaemolyticus</i>

Trivedi¹,

Branton²,

Trivedi³

et al. 2015

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Abstract:The recent emergence of the Vibrio parahaemolyticus (V. parahaemolyticus) is a pandemic. For the safety concern of seafood, consumer monitoring of this organism in seafood is very much essential. The current study was undertaken to evaluate the impact of Mr. Trivedi's biofield energy treatment on [ATCC-17802] strain of V. parahaemolyticus for its biochemical characteristics, biotype and 16S rDNA analysis. The lyophilized strain of V. parahaemolyticus was divided into two parts, Group (Gr.) I: control and Gr. II: treated. Gr. II was further subdivided into two parts, Gr. IIA and Gr. IIB. Gr. IIA was analyzed on day 10, whereas, Gr. IIB was stored and analyzed on day 142 (Study I). After retreatment of Gr. IIB on day 142 (Study II), the sample was divided into three separate tubes. The tubes first, second and third were analyzed on day 5, 10, and 15, respectively. The biochemical reaction and biotyping were performed using automated MicroScan Walk-Away ® system. The 16S rDNA sequencing was carried out to correlate the phylogenetic relationship of V. parahaemolyticus with other bacterial species after the treatment. The results of biochemical reactions were altered 24.24%, out of thirty-three in the treated groups with respect to the control. Moreover, negative (-) reaction of urea was changed to positive (+) in the revived treated Gr. IIB, Study II on day 15 as compared to the control. Besides, biotype number was substantially changed in all the treated groups as compared to the control. However, change in organisms were reported in Gr. IIA on day 10 and in Gr. IIB; Study II on day 5 as Shewanella putrefaciens and Moraxella/Psychrobacter spp., respectively with respect to the control i.e. Vibrio sp. SF. 16S rDNA analysis showed that the identified sample in this experiment was V. parahaemolyticus after biofield treatment, and the nearest homolog genus-species was observed as Vibrio natriegens with 98% gene identity. The results envisaged that the biofield energy treatment showed an alteration in biochemical reaction pattern and biotype number on the strain of V. parahaemolyticus.

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“…En febrero de 1996 en Calcuta, India, se detectó por primera vez un nuevo clon de V. parahaemolyticus perteneciente al serotipo O3:K6, TDH positivo, TRH negativo, siendo responsable de un gran aumento de los casos de enfermedad diarreica en esa zona 29 . Posteriormente este clon pandémi-co 25,28,[29][30][31][32][33][34] ha sido el responsable del aumento de casos en otras regiones de Asia, llegando incluso a Norteamérica y finalmente a Chile, donde se ha detectado su presencia desde el año 1998; desde entonces ha sido el responsable de todos los grandes brotes ocurridos 35 (comunicación verbal ISP). El fundamento de la expansión de este clon permanece sin dilucidar, puesto que su nivel de producción de TDH y su susceptibilidad antimicrobiana no es distinta a la de otras cepas patógenas de V. parahaemolyticus.…”

Section: Aspectos Microbiológicosunclassified

Revisión y recomendaciones para el manejo de diarrea por Vibrio parahaemolyticus

et al. 2005

Rev. chil. infectol.

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In Chile Vibrio parahaemolyticus has been detected in 3 gastroenteritis outbreaks since 1998. The most recent outbreak occurred during the summer of 2005, affecting over 10.000 people of whom one died. Affected individuals presented with one or more of the following symptoms: diarrhea, nausea, vomiting, abdominal pain and/or fever. Fecal white blood cells were detected in only 6% of patients. The predominant serotype in the 3 outbreaks was the pandemic O3:K6 strain. Diagnosis was confirmed by isolation and identification of V. parahaemolyticus in stool cultures and/or by establishing an epidemiological link. V. parahaemolyticus isolates were 100% susceptible to tetracycline, ciprofloxacin and chloramphenicol, and universally resistant to ampicillin. Due to the public health impact of the 2005 outbreak, the Ministry of Health called for a National Task Force mandated to review epidemiological, clinical and microbiological features of the outbreak and to propose management guidelines.Key words: Vibrio; Vibrio parahaemolyticus; Foodborne disease; Seafood; Diarrhea; Diarrhea outbreak.Palabras claves: Vibrio; Vibrio parahaemolyticus; Enfermedad transmitida por alimentos; Mariscos; Diarrea; Brote epidémico de diarrea.El género Vibrio, de la familia Vibrionaceae, posee más de 48 especies, y su taxonomía está en constante revisión gracias a la incorporación de técnicas de biología molecular. Al menos 12 de ellas son patógenas para el hombre y varias son también patógenas para animales tanto vertebrados como invertebrados 6 (Tabla 1).El hábitat natural de V. parahaemolyticus está en las aguas marinas costeras, especialmente los estuarios, las que representan su reservorio. La población microbiana es afectada por los cambios en la temperatura, salinidad, disponibilidad de nutrientes y su asociación con animales marinos. La temperatura óptima para su desarrollo es entre 20 y 30º C, la que permite una mayor concentración de bacterias; bajo 20º C disminuye IntroduccciónDurante mucho tiempo el interés de los médi-cos clínicos se ha centrado en Vibrio cholerae, responsable de brotes de gran magnitud con una alta letalidad, especialmente en países en desarrollo 1 . En la última década han emergido otros Vibrio productores de enfermedades que, aunque generalmente de menor severidad, tienen la capacidad de producir importantes brotes epidé-micos, como Vibrio parahaemolyticus 2 .La infección por Vibrio es adquirida por la vía oral o por inoculación a través de piel no intacta 3 , afectando así al tracto digestivo, y produciendo ocasionalmente infecciones cutáneas y síndromes sépticos 4,5 .

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Prevalence of Pandemic Thermostable Direct Hemolysin-Producing Vibrio parahaemolyticus O3:K6 in Seafood and the Coastal Environment in Japan

Cited by 141 publications

References 20 publications

Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

Biochemical Differentiation and Molecular Characterization of Biofield Treated <i>Vibrio parahaemolyticus</i>

Revisión y recomendaciones para el manejo de diarrea por Vibrio parahaemolyticus

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Prevalence of Pandemic Thermostable Direct Hemolysin-Producing Vibrio parahaemolyticus O3:K6 in Seafood and the Coastal Environment in Japan

Cited by 141 publications

References 20 publications

Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

Virulence Gene- and Pandemic Group-Specific Marker Profiling of Clinical Vibrio parahaemolyticus Isolates

Biochemical Differentiation and Molecular Characterization of Biofield Treated &lt;i&gt;Vibrio parahaemolyticus&lt;/i&gt;

Revisión y recomendaciones para el manejo de diarrea por Vibrio parahaemolyticus

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Biochemical Differentiation and Molecular Characterization of Biofield Treated <i>Vibrio parahaemolyticus</i>