Your search keyword '"Allander, Tobias"' showing total 8 results

1. Polyomaviruses BK, JC, KI, WU, MC, and TS in children with allogeneic hematopoietic stem cell transplantation.

Author

Rahiala, Jaana, Koskenvuo, Minna, Sadeghi, Mohammadreza, Waris, Matti, Vuorinen, Tytti, Lappalainen, Maija, Saarinen‐Pihkala, Ulla, Allander, Tobias, Söderlund‐Venermo, Maria, Hedman, Klaus, Ruuskanen, Olli, and Vettenranta, Kim

Subjects

POLYOMAVIRUSES, HEMATOPOIETIC stem cell transplantation, CHILD patients, VIREMIA, GRAFT versus host disease

Abstract

Timely and reliable detection of viruses is of key importance in early diagnosis of infection(s) following allogeneic HSCT. Among the immunocompetent, infections with BKPy V and JCPyV are mostly subclinical, while post- HSCT, the former may cause HC and the latter PML. The epidemiology and clinical impact of the newly identified KIPyV, WUPyV, MCPyV, and TSPyV in this context remain to be defined. To assess the incidence and clinical impact of BKPyV, JCPyV, KIPyV, WUPyV, MCPyV, and TSPyV infections, we performed longitudinal molecular surveillance for DNAemias of these HPyVs among 53 pediatric HSCT recipients. Surveillance pre- HSCT and for three months post- HSCT revealed BKPyV DNAemia in 20 (38%) patients. Our data demonstrate frequent BKPyV DNAemia among pediatric patients with HSCT and the confinement of clinical symptoms to high copy numbers alone. MCPyV and JCPyV viremias occurred at low and TSPyV viremia at very low prevalences. KIPyV or WUPyV viremias were not demonstrable in this group of immunocompromised patients. [ABSTRACT FROM AUTHOR]

Published

2016

2. Taxonomical developments in the family Polyomaviridae.

Author

Johne, Reimar, Buck, Christopher, Allander, Tobias, Atwood, Walter, Garcea, Robert, Imperiale, Michael, Major, Eugene, Ramqvist, Torbjorn, and Norkin, Leonard

Subjects

POLYOMAVIRUSES, CLASSIFICATION of viruses, SPECIES distribution, BIOLOGICAL classification, VIROLOGY, ONCOGENIC DNA viruses

Abstract

The Polyomaviridae Study Group of the International Committee on Taxonomy of Viruses (ICTV) has recommended several taxonomical revisions, as follows: The family Polyomaviridae, which is currently constituted as a single genus ( Polyomavirus), will be comprised of three genera: two containing mammalian viruses and one containing avian viruses. The two mammalian genera will be designated Orthopolyomavirus and Wukipolyomavirus, and the avian genus will be named Avipolyomavirus. These genera will be created by the redistribution of species from the current single genus ( Polyomavirus) and by the inclusion of several new species. In addition, the names of several species will be changed to reflect current usage. [ABSTRACT FROM AUTHOR]

Published

2011

3. DNA from KI, WU and Merkel Cell Polyomaviruses Is Not Detected in Childhood Central Nervous System Tumours or Neuroblastomas.

Author

Giraud, Géraldine, Ramqvist, Torbjörn, Pastrana, Diana V., Pavot, Vincent, Lindau, Cecilia, Kogner, Per, Orrego, Abiel, Buck, Christopher B., Allander, Tobias, Holm, Stefan, Gustavsson, Bengt, and Dalianis, Tina

Subjects

MERKEL cell carcinoma, POLYOMAVIRUSES, NEUROBLASTOMA, CENTRAL nervous system, NERVOUS system cancer, TROPISMS, NUCLEOTIDE sequence, NUCLEIC acid analysis, DNA

Abstract

Background: BK and JC polyomaviruses (BKV and JCV) are potentially oncogenic and have in the past inconclusively been associated with tumours of the central nervous system (CNS), while BKV has been hinted, but not confirmed to be associated with neuroblastomas. Recently three new polyomaviruses (KIPyV, WUPyV and MCPyV) were identified in humans. So far KIPyV and WUPyV have not been associated to human diseases, while MCPyV was discovered in Merkel Cell carcinomas and may have neuroepithelial cell tropism. However, all three viruses can be potentially oncogenic and this compelled us to investigate for their presence in childhood CNS and neuroblastomas. Methodology: The presence of KI, WU and MCPyV DNA was analysed, by a joint WU and KI specific PCR (covering part of VP1) and by a MCPyV specific regular and real time quantitative PCR (covering part of Large T) in 25 CNS tumour biopsies and 31 neuroblastoma biopsies from the Karolinska University Hospital, Sweden. None of the three new human polyomaviruses were found to be associated with any of the tumours, despite the presence of PCR amplifiable DNA assayed by a S14 housekeeping gene PCR. Conclusion: In this pilot study, the presence of MCPyV, KI and WU was not observed in childhood CNS tumours and neuroblastomas. Nonetheless, we suggest that additional data are warranted in tumours of the central and peripheral nervous systems and we do not exclude that other still not yet detected polyomaviruses could be present in these tumours. [ABSTRACT FROM AUTHOR]

Published

2009

4. Merkel Cell Polyomavirus in Respiratory Tract Secretions.

Author

Shan Goh, Lindau, Cecilia, Tiveljung-Lindell, Annika, and Allander, Tobias

Subjects

MERKEL cells, POLYOMAVIRUSES, DISEASES in older people, RESPIRATORY infections, DNA viruses, DNA

Abstract

Merkel cell polyomavirus (MCPyV), associated with Merkel cell carcinoma, was detected in 27 of 635 nasopharyngeal aspirate samples by real-time PCR. MCPyV was more commonly found in adults than in children. Presence in the upper respiratory tract may be a general property of human PyVs. [ABSTRACT FROM AUTHOR]

Published

2009

5. Identification of a Third Human Polyomavirus.

Author

Allander, Tobias, Andreasson, Kalle, Gupta, Shawon, Bjerkner, Annelie, Bogdanovic, Gordana, Persson, Mats A. A., Dalianis, Tina, Ramqvist, Torbjörn, and Andersson, Björn

Subjects

*VIRUSES, *RESPIRATORY infections, *POLYOMAVIRUSES, *GENOMES, *HOMOLOGY (Biology)

Abstract

We have previously reported on a system for large-scale molecular virus screening of clinical samples. As part of an effort to systematically search for unrecognized human pathogens, the technology was applied for virus screening of human respiratory tract samples. This resulted in the identification of a previously unknown polyomavirus provisionally named KI polyomavirus. The virus is phylogenetically related to other primate polyomaviruses in the early region of the genome but has very little homology (<30% amino acid identity) to known polyomaviruses in the late region. The virus was found by PCR in 6 (1%) of 637 nasopharyngeal aspirates and in 1 (0.5%) of 192 fecal samples but was not detected in sets of urine and blood samples. Since polyomaviruses have oncogenic potential and may produce severe disease in immunosuppressed individuals, continued searching for the virus in different medical contexts is important. This finding further illustrates how unbiased screening of respiratory tract samples can be used for the discovery of diverse virus types. [ABSTRACT FROM AUTHOR]

Published

2007

6. Metagenomic characterization of viruses in the serum of children with newly diagnosed cancer.

Author

Leijonhufvud, Gustaf, Soratto, Tatiany Aparecida Teixeira, Matos, Gabriel Machado, Bajalan, Amanj, Eichler-Jonsson, Claudia, Gustafsson, Britt, Bogdanovic, Gordana, Allander, Tobias, Ljungman, Gustaf, and Andersson, Björn

Subjects

*TORQUE teno virus, *VIRUS diseases, *ONCOGENIC viruses, *HUMAN papillomavirus, *HEPATITIS C virus, *POLYOMAVIRUSES, *RHINOVIRUSES

Abstract

• What's Known on This Subject • Virus infections, both chronic and transient are common in children. There are several known cancer-causing viruses, and viruses that may complicate cancer treatment in children. There are many studies on individual viruses, but few larger studies. • What This Study Adds • This study provides an overview of the human virome in children diagnosed with different cancer types. It provides data on the prevalence of many viruses. Novel information on HPgV and TTV infections and a new virus were revealed. A large cohort of pediatric patients with various forms of childhood cancer was investigated for the presence of viruses using metagenomics. A total of 476 patient samples, collected between 1989 and 2018, were analyzed, representing various pediatric oncological diagnoses and a control group of non-malignant diagnoses. The study was carried out using metagenomic sequencing of serum samples. Viruses were identified and analyzed using bioinformatics methods, followed by Polymerase chain reaction (PCR) confirmation The results indicate that a wide range of viruses can be detected in the bloodstream of children with newly diagnosed cancer. Nine viral genomes were identified: Human Pegivirus (HPgV), Hepatitis C virus, Parechovirus 1, Rhinovirus C, Human papillomavirus 116, Human polyomavirus 10, Parvovirus B19, and different variants of Torque Teno Virus (TTV). In this study, a previously unknown virus was found belonging to the Iflavirdae family in the order Picornavirales. HPGV was significantly more common in patients with leukemia compared to other conditions. These results highlight the abundance of systemic virus infections in children, and the value of metagenomic sequencing for hypothesis forming regarding the associations between virus infections and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

7. A single-tube, real-time PCR assay for detection of the two newly characterized human KI and WU polyomaviruses

Author

Lindau, Cecilia, Tiveljung-Lindell, Annika, Goh, Shan, Ramqvist, Torbjörn, and Allander, Tobias

Subjects

*POLYOMAVIRUSES, *PAPILLOMAVIRUS pathogenicity, *POLYMERASE chain reaction, *VIRUS diseases, *NASOPHARYNGITIS, *MEDICAL screening

Abstract

Abstract: Background: Three new human polyomaviruses have been recently described, and investigating their in vivo biology and pathogenicity will require sensitive and rational detection assays. Objectives: To develop and evaluate a sensitive and rational assay for detection of the newly identified KI and WU polyomaviruses. Study design: A single-tube, dual-probe, real-time PCR assay for simultaneous detection and discrimination of KI and WU polyomaviruses was developed. Results: The assay had near single-molecule sensitivity for both viruses and no cross-reactivity was observed. A panel of 637 nasopharyngeal aspirates was screened, resulting in a frequency of 1.4% for KIPyV and 1.3% for WUPyV. Conclusions: The dual-probe assay provides a rational approach for further studies of KIPyV and WUPyV. [Copyright &y& Elsevier]

Published

2009

8. Whole-Genome Characterization and Genotyping of Global WU Polyomavirus Strains.

Author

Bialasiewicz, Seweryn, Rockett, Rebecca, Whiley, David W., Abed, Yacine, Allander, Tobias, Binks, Michael, Boivin, Guy, Cheng, Allen C., Ju-Young Chung, Ferguson, Patricia E., Gilroy, Nicole M., Leach, Amanda J., Lindau, Cecilia, Rossen, John W., Sorrell, Tania C., Nissen, Michael D., and Sloots, Theo P.

Subjects

*POLYOMAVIRUSES, *GENOMES, *SEQUENCE alignment, *NUCLEOTIDES, *GENETICS

Abstract

Exploration of the genetic diversity of WU polyomavirus (WUV) has been limited in terms of the specimen numbers and particularly the sizes of the genomic fragments analyzed. Using whole-genome sequencing of 48 WUV strains collected in four continents over a 5-year period and 16 publicly available whole-genome sequences, we identified three main WUV clades and five subtypes, provisionally termed Ia, Ib, Ic, II, IIIa, and IIIb. Overall nucleotide variation was low (0 to 1.2%). The discriminatory power of the previous VP2 fragment typing method was found to be limited, and a new, larger genotyping region within the VP2/1 interface was proposed. [ABSTRACT FROM AUTHOR]

Published

2010