Your search keyword '"Langeland, Nina"' showing total 31 results

1. Highly contiguous genomes of human clinical isolates of Giardia duodenalis reveal assemblage- and sub-assemblage-specific presence-absence variation in protein-coding genes.

Author

Klotz, Christian, Klotz, Christian, Schmid, Marc William, Winter, Katja, Ignatius, Ralf, Weisz, Filip, Saghaug, Christina Skar, Langeland, Nina, Dawson, Scott, Lalle, Marco, Hanevik, Kurt, Cacciò, Simone M, Aebischer, Toni, Klotz, Christian, Klotz, Christian, Schmid, Marc William, Winter, Katja, Ignatius, Ralf, Weisz, Filip, Saghaug, Christina Skar, Langeland, Nina, Dawson, Scott, Lalle, Marco, Hanevik, Kurt, Cacciò, Simone M, and Aebischer, Toni

Abstract

Giardia duodenalis (syn. G. intestinalis, G. lamblia) is a widespread gastrointestinal protozoan parasite with debated taxonomic status. Currently, eight distinct genetic sub-groups, termed assemblages A-H, are defined based on a few genetic markers. Assemblages A and B may represent distinct species and are both of human public health relevance. Genomic studies are scarce and the few reference genomes available, in particular for assemblage B, are insufficient for adequate comparative genomics. Here, by combining long- and short-read sequences generated by PacBio and Illumina sequencing technologies, we provide nine annotated genome sequences for reference from new clinical isolates (four assemblage A and five assemblage B parasite isolates). Isolates chosen represent the currently accepted classification of sub-assemblages AI, AII, BIII and BIV. Synteny over the whole genome was generally high, but we report chromosome-level translocations as a feature that distinguishes assemblage A from B parasites. Orthologue gene group analysis was used to define gene content differences between assemblage A and B and to contribute a gene-set-based operational definition of respective taxonomic units. Giardia is tetraploid, and high allelic sequence heterogeneity (ASH) for assemblage B vs. assemblage A has been observed so far. Noteworthy, here we report an extremely low ASH (0.002%) for one of the assemblage B isolates (a value even lower than the reference assemblage A isolate WB-C6). This challenges the view of low ASH being a notable feature that distinguishes assemblage A from B parasites, and low ASH allowed assembly of the most contiguous assemblage B genome currently available for reference. In conclusion, the description of nine highly contiguous genome assemblies of new isolates of G. duodenalis assemblage A and B adds to our understanding of the genomics and species population structure of this widespread zoonotic parasite.

Published

2023

2. Oocyst Shedding Dynamics in Children with Cryptosporidiosis:a Prospective Clinical Case Series in Ethiopia

Author

Johansen, Øystein H., Abdissa, Alemseged, Bjørang, Ola, Zangenberg, Mike, Sharew, Bizuwarek, Alemu, Yonas, Moyo, Sabrina, Mekonnen, Zeleke, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein H., Abdissa, Alemseged, Bjørang, Ola, Zangenberg, Mike, Sharew, Bizuwarek, Alemu, Yonas, Moyo, Sabrina, Mekonnen, Zeleke, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Knowledge on the duration of Cryptosporidium oocyst shedding, and how shedding may be affected by subtypes and clinical parameters, is limited. Reduced transmission may be a secondary benefit of cryptosporidiosis treatment in high-prevalence areas. We conducted a prospective clinical case series in children of <5 years presenting with diarrhea to a health center and a hospital in Ethiopia over an 18-month period. Stool samples were collected repeatedly from children diagnosed with cryptosporidiosis for up to 60 days. Samples were examined, and Cryptosporidium shedding was quantified, using auramine phenol, immunofluorescent antibody staining, and quantitative PCR (qPCR). In addition, species determination and subtyping were used to attempt to distinguish between new infections and ongoing shedding. Duration and quantity of shedding over time were estimated by time-to-event and quantitative models (sex- and age-adjusted). We also explored how diarrheal severity, acute malnutrition, and Cryptosporidium subtypes correlated with temporal shedding patterns. From 53 confirmed cryptosporidiosis cases, a median of 4 (range 1 to 5) follow-up stool samples were collected and tested for Cryptosporidium. The median duration of oocyst shedding was 31 days (95% confidence interval [CI], 26 to 36 days) after onset of diarrhea, with similar estimates from the quantitative models (31 days, 95% CI 27 to 37 days). Genotype shift occurred in 5 cases (9%). A 10-fold drop in quantity occurred per week for the first 4 weeks. Prolonged oocyst shedding is common in a pediatric clinical population with cryptosporidiosis. We suggest that future intervention trials should evaluate both clinical efficacy and total parasite shedding duration as trial endpoints. IMPORTANCE Cryptosporidiosis is an important cause of diarrhea, malnutrition, and deaths in young children in low-income countries. The infection spreads from person to person. After infection, prolonged release of the Cryptosporidi

Published

2022

3. Oocyst Shedding Dynamics in Children with Cryptosporidiosis:a Prospective Clinical Case Series in Ethiopia

Author

Johansen, Øystein H., Abdissa, Alemseged, Bjørang, Ola, Zangenberg, Mike, Sharew, Bizuwarek, Alemu, Yonas, Moyo, Sabrina, Mekonnen, Zeleke, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein H., Abdissa, Alemseged, Bjørang, Ola, Zangenberg, Mike, Sharew, Bizuwarek, Alemu, Yonas, Moyo, Sabrina, Mekonnen, Zeleke, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Knowledge on the duration of Cryptosporidium oocyst shedding, and how shedding may be affected by subtypes and clinical parameters, is limited. Reduced transmission may be a secondary benefit of cryptosporidiosis treatment in high-prevalence areas. We conducted a prospective clinical case series in children of <5 years presenting with diarrhea to a health center and a hospital in Ethiopia over an 18-month period. Stool samples were collected repeatedly from children diagnosed with cryptosporidiosis for up to 60 days. Samples were examined, and Cryptosporidium shedding was quantified, using auramine phenol, immunofluorescent antibody staining, and quantitative PCR (qPCR). In addition, species determination and subtyping were used to attempt to distinguish between new infections and ongoing shedding. Duration and quantity of shedding over time were estimated by time-to-event and quantitative models (sex- and age-adjusted). We also explored how diarrheal severity, acute malnutrition, and Cryptosporidium subtypes correlated with temporal shedding patterns. From 53 confirmed cryptosporidiosis cases, a median of 4 (range 1 to 5) follow-up stool samples were collected and tested for Cryptosporidium. The median duration of oocyst shedding was 31 days (95% confidence interval [CI], 26 to 36 days) after onset of diarrhea, with similar estimates from the quantitative models (31 days, 95% CI 27 to 37 days). Genotype shift occurred in 5 cases (9%). A 10-fold drop in quantity occurred per week for the first 4 weeks. Prolonged oocyst shedding is common in a pediatric clinical population with cryptosporidiosis. We suggest that future intervention trials should evaluate both clinical efficacy and total parasite shedding duration as trial endpoints. IMPORTANCE Cryptosporidiosis is an important cause of diarrhea, malnutrition, and deaths in young children in low-income countries. The infection spreads from person to person. After infection, prolonged release of the Cryptosporidi

Published

2022

4. A comparison of risk factors for cryptosporidiosis and non-cryptosporidiosis diarrhoea:A case-case-control study in Ethiopian children

Author

Johansen, Øystein Haarklau, Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Sharew, Bizuwarek, Moyo, Sabrina, Sommerfelt, Halvor, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein Haarklau, Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Sharew, Bizuwarek, Moyo, Sabrina, Sommerfelt, Halvor, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Background Cryptosporidiosis is a major cause of diarrhoea in young children in low-and-middle-income countries. New interventions should be informed by evidence pertaining to risk factors and their relative importance. Inconsistencies in the literature may to some extent be explained by choice of methodology, furthermore, most previous risk factor studies compared crypto-sporidiosis cases to diarrhoea cases of other aetiologies rather than with controls without diarrhoea. Methodology/Principal findings We investigated a broad set of factors in under-2-year-olds presenting with diarrhoea to a hospital and a health center in southwestern Ethiopia. We applied quantitative cut-offs to distinguish between cryptosporidiosis and incidental Cryptosporidium infection or carriage, a hierarchical causal framework to minimize confounding and overadjustment, and a case-case-control design, to describe risk factors for both cryptosporidiosis and non-cryptosporid-iosis diarrhoea. Moderate and severe acute malnutrition were strongly associated with both cryptosporidiosis and non-cryptosporidiosis diarrhoea. Previous healthcare attendance and low maternal education were only associated with cryptosporidiosis, whereas unsafe child stool disposal, prematurity and early cessation of exclusive breastfeeding were significantly associated with non-cryptosporidiosis diarrhoea only. By estimation of population attributable fractions, socioeconomic factors—specifically low maternal education—and public tap water use, were apparently more important risk factors for cryptosporidiosis than for non-cryptosporidiosis diarrhoea. Conclusions/Significance Nutritional management of moderate acute malnutrition may be an effective intervention against cryptosporidiosis, particularly if combined with targeted therapy for cryptosporidiosis which, again, may mitigate nutritional insult. Focused caregiver education in healthcare settings and follow-up of children with acute malnutrition may prevent or

Published

2022

5. A comparison of risk factors for cryptosporidiosis and non-cryptosporidiosis diarrhoea:A case-case-control study in Ethiopian children

Author

Johansen, Øystein Haarklau, Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Sharew, Bizuwarek, Moyo, Sabrina, Sommerfelt, Halvor, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein Haarklau, Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Sharew, Bizuwarek, Moyo, Sabrina, Sommerfelt, Halvor, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Background Cryptosporidiosis is a major cause of diarrhoea in young children in low-and-middle-income countries. New interventions should be informed by evidence pertaining to risk factors and their relative importance. Inconsistencies in the literature may to some extent be explained by choice of methodology, furthermore, most previous risk factor studies compared crypto-sporidiosis cases to diarrhoea cases of other aetiologies rather than with controls without diarrhoea. Methodology/Principal findings We investigated a broad set of factors in under-2-year-olds presenting with diarrhoea to a hospital and a health center in southwestern Ethiopia. We applied quantitative cut-offs to distinguish between cryptosporidiosis and incidental Cryptosporidium infection or carriage, a hierarchical causal framework to minimize confounding and overadjustment, and a case-case-control design, to describe risk factors for both cryptosporidiosis and non-cryptosporid-iosis diarrhoea. Moderate and severe acute malnutrition were strongly associated with both cryptosporidiosis and non-cryptosporidiosis diarrhoea. Previous healthcare attendance and low maternal education were only associated with cryptosporidiosis, whereas unsafe child stool disposal, prematurity and early cessation of exclusive breastfeeding were significantly associated with non-cryptosporidiosis diarrhoea only. By estimation of population attributable fractions, socioeconomic factors—specifically low maternal education—and public tap water use, were apparently more important risk factors for cryptosporidiosis than for non-cryptosporidiosis diarrhoea. Conclusions/Significance Nutritional management of moderate acute malnutrition may be an effective intervention against cryptosporidiosis, particularly if combined with targeted therapy for cryptosporidiosis which, again, may mitigate nutritional insult. Focused caregiver education in healthcare settings and follow-up of children with acute malnutrition may prevent or

Published

2022

6. Genetic Variation in Metronidazole Metabolism and Oxidative Stress Pathways in Clinical Giardia lamblia Assemblage A and B Isolates [Corrigendum]

Author

Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Brattbakk,Hans-Richard, Stokowy,Tomasz, Aebischer,Toni, Kursula,Inari, Langeland,Nina, Hanevik,Kurt, Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Brattbakk,Hans-Richard, Stokowy,Tomasz, Aebischer,Toni, Kursula,Inari, Langeland,Nina, and Hanevik,Kurt

Abstract

Saghaug CS, Klotz C, Kallio JP, et al. Infect Drug Resist. 2019;12:1221–1235. The authors have advised NR-1 was used throughout the paper to denote the gene named in GiardiaDB as “Nitroreductase family protein fused to ferredoxin domain Fd-NR1” (DHA2_153380/GSB_153178), while in recent literature this is often denoted NR2/GlNR2. Likewise, NR-2 was used to denote the gene named in GiardiaDB as “Nitroreductase Fd-NR-2” (DHA2_22677/GSB_22677), while in recent literature this is often denoted NR1/GlNR1. The authors acknowledge that using the NR gene names as annotated in GiardiaDB may cause confusion and therefore, bring this to the attention of readers that more correctly what is named “NR-1” in the paper should be read as “NR-2”, and “NR-1” should be read as “NR-2”. The authors apologize for not having considered this issue in the original manuscript. Read the original article

Published

2021

7. Performance and operational feasibility of two diagnostic tests for cryptosporidiosis in children (CRYPTO-POC):a clinical, prospective, diagnostic accuracy study

Author

Johansen, Øystein H., Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Bjørang, Ola, Alemu, Yonas, Sharew, Bizuwarek, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein H., Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Bjørang, Ola, Alemu, Yonas, Sharew, Bizuwarek, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Background: Cryptosporidiosis is a common cause of diarrhoea in young children (aged younger than 24 months) in low-resource settings but is currently challenging to diagnose. Light-emitting diode fluorescence microscopy with auramine-phenol staining (LED-AP), recommended for tuberculosis testing, can also detect Cryptosporidium species. A lateral-flow test not requiring refrigerator storage (by contrast with most immunochromatographic lateral-flow assays) has also recently been developed for Cryptosporidium spp detection. We aimed to evaluate the diagnostic accuracy and operational feasibility of LED-AP and the lateral-flow test strip for cryptosporidiosis in children. Methods: We did a prospective diagnostic accuracy study in two health-care facilities in Ethiopia, in a consecutive series of children younger than 5 years of age with diarrhoea (three or more loose stools within the previous 24 h) or dysentery (at least one loose stool with stains of blood within the previous 24 h). Stool samples were tested for Cryptosporidium spp by LED-AP and the lateral-flow test strip; accuracy of each test was estimated by independent and blind comparison with a composite reference standard comprising quantitative immunofluorescent antibody test (qIFAT), ELISA, and quantitative PCR (qPCR). Quantitative cutoff values for diarrhoea-associated infection were established in an embedded case-control substudy, with cases of cryptosporidiosis coming from the 15 districts in and around Jimma and the eight districts surrounding Serbo, and community controls without diarrhoea in the previous 48 h recruited by weekly frequency matching by geographical district of the household, age group, and enrolment week. Findings: Stool samples from 912 children with diarrhoea or dysentery and 706 controls from the case-control substudy were tested between Dec 22, 2016, and July 6, 2018. Estimated reference-standard cutoff values for cryptosporidiosis positivity were 2·3 × 105 DNA copie

Published

2021

8. Performance and operational feasibility of two diagnostic tests for cryptosporidiosis in children (CRYPTO-POC):a clinical, prospective, diagnostic accuracy study

Author

Johansen, Øystein H., Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Bjørang, Ola, Alemu, Yonas, Sharew, Bizuwarek, Langeland, Nina, Robertson, Lucy J., Hanevik, Kurt, Johansen, Øystein H., Abdissa, Alemseged, Zangenberg, Mike, Mekonnen, Zeleke, Eshetu, Beza, Bjørang, Ola, Alemu, Yonas, Sharew, Bizuwarek, Langeland, Nina, Robertson, Lucy J., and Hanevik, Kurt

Abstract

Background: Cryptosporidiosis is a common cause of diarrhoea in young children (aged younger than 24 months) in low-resource settings but is currently challenging to diagnose. Light-emitting diode fluorescence microscopy with auramine-phenol staining (LED-AP), recommended for tuberculosis testing, can also detect Cryptosporidium species. A lateral-flow test not requiring refrigerator storage (by contrast with most immunochromatographic lateral-flow assays) has also recently been developed for Cryptosporidium spp detection. We aimed to evaluate the diagnostic accuracy and operational feasibility of LED-AP and the lateral-flow test strip for cryptosporidiosis in children. Methods: We did a prospective diagnostic accuracy study in two health-care facilities in Ethiopia, in a consecutive series of children younger than 5 years of age with diarrhoea (three or more loose stools within the previous 24 h) or dysentery (at least one loose stool with stains of blood within the previous 24 h). Stool samples were tested for Cryptosporidium spp by LED-AP and the lateral-flow test strip; accuracy of each test was estimated by independent and blind comparison with a composite reference standard comprising quantitative immunofluorescent antibody test (qIFAT), ELISA, and quantitative PCR (qPCR). Quantitative cutoff values for diarrhoea-associated infection were established in an embedded case-control substudy, with cases of cryptosporidiosis coming from the 15 districts in and around Jimma and the eight districts surrounding Serbo, and community controls without diarrhoea in the previous 48 h recruited by weekly frequency matching by geographical district of the household, age group, and enrolment week. Findings: Stool samples from 912 children with diarrhoea or dysentery and 706 controls from the case-control substudy were tested between Dec 22, 2016, and July 6, 2018. Estimated reference-standard cutoff values for cryptosporidiosis positivity were 2·3 × 105 DNA copie

Published

2021

9. Genetic Diversity of the Flavohemoprotein Gene of Giardia lamblia: Evidence for High Allelic Heterozygosity and Copy Number Variation

Author

Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Aebischer,Toni, Langeland,Nina, Hanevik,Kurt, Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Aebischer,Toni, Langeland,Nina, and Hanevik,Kurt

Abstract

Christina S Saghaug,1,2 Christian Klotz,3 Juha P Kallio,4 Toni Aebischer,3 Nina Langeland,1,2,5 Kurt Hanevik1 1Department of Clinical Science, University of Bergen, Bergen, Norway; 2Norwegian National Advisory Unit on Tropical Infectious Diseases, Department of Medicine, Haukeland University Hospital, Bergen, Norway; 3Department of Infectious Diseases, Unit 16 Mycotic and Parasitic Agents and Mycobacteria, Robert Koch-Institute, Berlin, Germany; 4Department of Biomedicine, University of Bergen, Bergen, Norway; 5Department of Medicine, Haraldsplass Deaconess Hospital, Bergen, NorwayCorrespondence: Christina S SaghaugDepartment of Clinical Science, University of Bergen, 8th Floor, Lab-Building, Bergen N-5021, NorwayTel +47 90 13 24 14Email christina.saghaug@uib.noPurpose: The flavohemoprotein (gFlHb) in Giardia plays an important role in managing nitrosative and oxidative stress, and potentially also in virulence and nitroimidazole drug tolerance. The aim of this study was to analyze the genetic diversity of gFlHb in Giardia assemblages A and B clinical isolates.Methods: gFlHb genes from 20 cultured clinical Giardia isolates were subjected to PCR amplification and cloning, followed by Sanger sequencing. Sequences of all cloned PCR fragments from each isolate were analyzed for single nucleotide variants (SNVs) and compared to genomic Illumina sequence data. Identical clone sequences were sorted into alleles, and diversity was further analyzed. The number of gFlHb gene copies was assessed by mining PacBio de novo assembled genomes in eight isolates. Homology models for assessment of SNV’s potential impact on protein function were created using Phyre2.Results: A variable copy number of the gFlHb gene, between two and six copies, depending on isolate, was found. A total of 37 distinct sequences, representing different alleles of the gFlHb gene, were identified in AII isolates, and 41 were identified in B isolates. In some isolates, up to 12 different alleles wer

Published

2020

10. Identification of Conserved Candidate Vaccine Antigens in the Surface Proteome of Giardia lamblia

Author

Davids, Barbara J., Liu, Ching M., Hanson, Elaine M., Le, Christine H. Y., Ang, Jonathan, Hanevik, Kurt, Fischer, Marvin, Radunovic, Matej, Langeland, Nina, Ferella, Marcela, Svärd, Staffan, Ghassemian, Majid, Miyamoto, Yukiko, Eckmann, Lars, Davids, Barbara J., Liu, Ching M., Hanson, Elaine M., Le, Christine H. Y., Ang, Jonathan, Hanevik, Kurt, Fischer, Marvin, Radunovic, Matej, Langeland, Nina, Ferella, Marcela, Svärd, Staffan, Ghassemian, Majid, Miyamoto, Yukiko, and Eckmann, Lars

Abstract

Giardia lamblia, one of the most common protozoal infections of the human intestine, is an important worldwide cause of diarrheal disease, malabsorption, malnutrition, delayed cognitive development in children, and protracted postinfectious syndromes. Despite its medical importance, no human vaccine is available against giardiasis. A crude veterinary vaccine has been developed, and experimental vaccines based on expression of multiple variant-specific surface proteins have been reported, but poorly defined vaccine components and excessive antigen variability are problematic for pharmaceutical vaccine production. To expand the repertoire of antigen candidates for vaccines, we reasoned that surface proteins may provide an enriched source of such antigens since key host effectors, such as secretory IgA, can directly bind to such antigens in the intestinal lumen and interfere with epithelial attachment. Here, we have applied a proteomics approach to identify 23 novel surface antigens of G. lamblia that show >90% amino acid sequence identity between the two human-pathogenic genetic assemblages (A and B) of the parasite. Surface localization of a representative subset of these proteins was confirmed by immunostaining. Four selected proteins, uridine phosphorylase-like protein-1, protein 21.1 (GL50803_ 27925), alpha 1-giardin, and alpha 11-giardin, were subsequently produced in recombinant form and shown to be immunogenic in mice and G. lamblia-infected humans and confer protection against G. lamblia infection upon intranasal immunization in rodent models of giardiasis. These results demonstrate that identification of conserved surface antigens provides a powerful approach for overcoming a key rate-limiting step in the design and construction of an effective vaccine against giardiasis.

Published

2019

11. Genetic variation in metronidazole metabolism and oxidative stress pathways in clinical Giardia lamblia assemblage A and B isolates

Author

Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Brattbakk,Hans-Richard, Stokowy,Tomasz, Aebischer,Toni, Kursula,Inari, Langeland,Nina, Hanevik,Kurt, Saghaug,Christina S, Klotz,Christian, Kallio,Juha P, Brattbakk,Hans-Richard, Stokowy,Tomasz, Aebischer,Toni, Kursula,Inari, Langeland,Nina, and Hanevik,Kurt

Abstract

Christina S Saghaug, 1, 2 Christian Klotz, 3 Juha P Kallio, 4 Hans-Richard Brattbakk, 1, 5 Tomasz Stokowy, 1, 5 Toni Aebischer, 3 Inari Kursula, 4, 6 Nina Langeland, 1– 2, 7 Kurt Hanevik 1, 2 1Department of Clinical Science, University of Bergen, Bergen, Hordaland, Norway; 2Norwegian National Advisory Unit on Tropical Infectious Diseases, Department of Medicine, Haukeland University Hospital, Bergen, Hordaland, Norway; 3Department of Infectious Diseases, Unit 16 Mycotic and Parasitic Agents and Mycobacteria, Robert Koch-Institute, Berlin, Germany; 4Department of Biomedicine, University of Bergen, Bergen, Hordaland, Norway; 5Center for Medical Genetics and Molecular Medicine, Haukeland University Hospital, Bergen, Hordaland, Norway; 6Biocenter Oulu and Faculty of Biochemistry and Molecular Medicine, University of Oulu, Oulu, Finland; 7Department of Medicine, Haraldsplass Deaconess Hospital, Bergen, Hordaland, NorwayPurpose: Treatment-refractory Giardia cases have increased rapidly within the last decade. No markers of resistance nor a standardized susceptibility test have been established yet, but several enzymes and their pathways have been associated with metronidazole (MTZ) resistant Giardia. Very limited data are available regarding genetic variation in these pathways. We aimed to investigate genetic variation in metabolic pathway genes proposed to be involved in MTZ resistance in recently acquired, cultured clinical isolates.Methods: Whole genome sequencing of 12 assemblage A2 and 8 assemblage B isolates was done, to decipher genomic variation in Giardia. Twenty-nine genes were identified in a literature search and investigated for their single nucleotide variants (SNVs) in the coding/non-coding regions of the genes, either as amino acid changing (non-synonymous SNVs) or non-changing SNVs (synonymous).Results: In Giardia assemblage B, several genes involved in MTZ activation or oxidative stress management were found to have higher numbers of non-synony

Published

2019

12. Prolonged and persistent diarrhoea is not restricted to children with acute malnutrition:An observational study in Ethiopia

Author

Zangenberg, Mike, Johansen, Øystein H, Abdissa, Alemseged, Eshetu, Beza, Kurtzhals, Jørgen, Friis, Henrik, Sommerfelt, Halvor, Langeland, Nina, Hanevik, Kurt, Zangenberg, Mike, Johansen, Øystein H, Abdissa, Alemseged, Eshetu, Beza, Kurtzhals, Jørgen, Friis, Henrik, Sommerfelt, Halvor, Langeland, Nina, and Hanevik, Kurt

Abstract

Objectives: To assess the prevalence of prolonged and persistent diarrhoea, to estimate their co-occurrence with acute malnutrition and association with demographic and clinical factors.Methods: Case-control study where cases were children under 5 years of age with diarrhoea and controls were children without diarrhoea, frequency-matched weekly by age and district of residency. Controls for cases 0-11 months were recruited from vaccination rooms and controls for cases 12-59 months were recruited by house visits using random locations in the catchment area of the study sites. Data were analysed by mixed model logistic regression.Results: We enrolled 1134 cases and 946 controls. Among the cases, 967 (85%) had acute diarrhoea (AD), 129 (11%) had ProD and 36 (3.2%) had PD. More cases had acute malnutrition at enrolment (17% vs 4%, p<0.0001) and more were born prematurely (5.7% vs 1.8%, p<0.0001) than controls. 75% of ProPD cases did not have acute malnutrition. Cases with AD and ProPD had different symptomatology, even beyond illness duration.Conclusions: ProPD is common among children presenting with diarrhoea and is not confined to children with acute malnutrition. There is an urgent need for studies assessing causes of ProPD with and without acute malnutrition to develop treatment guidelines for these conditions.

Published

2019

13. Prolonged and persistent diarrhoea is not restricted to children with acute malnutrition:An observational study in Ethiopia

Author

Zangenberg, Mike, Johansen, Øystein H, Abdissa, Alemseged, Eshetu, Beza, Kurtzhals, Jørgen, Friis, Henrik, Sommerfelt, Halvor, Langeland, Nina, Hanevik, Kurt, Zangenberg, Mike, Johansen, Øystein H, Abdissa, Alemseged, Eshetu, Beza, Kurtzhals, Jørgen, Friis, Henrik, Sommerfelt, Halvor, Langeland, Nina, and Hanevik, Kurt

Abstract

Objectives: To assess the prevalence of prolonged and persistent diarrhoea, to estimate their co-occurrence with acute malnutrition and association with demographic and clinical factors.Methods: Case-control study where cases were children under 5 years of age with diarrhoea and controls were children without diarrhoea, frequency-matched weekly by age and district of residency. Controls for cases 0-11 months were recruited from vaccination rooms and controls for cases 12-59 months were recruited by house visits using random locations in the catchment area of the study sites. Data were analysed by mixed model logistic regression.Results: We enrolled 1134 cases and 946 controls. Among the cases, 967 (85%) had acute diarrhoea (AD), 129 (11%) had ProD and 36 (3.2%) had PD. More cases had acute malnutrition at enrolment (17% vs 4%, p<0.0001) and more were born prematurely (5.7% vs 1.8%, p<0.0001) than controls. 75% of ProPD cases did not have acute malnutrition. Cases with AD and ProPD had different symptomatology, even beyond illness duration.Conclusions: ProPD is common among children presenting with diarrhoea and is not confined to children with acute malnutrition. There is an urgent need for studies assessing causes of ProPD with and without acute malnutrition to develop treatment guidelines for these conditions.

Published

2019

14. Giardia-specific cellular immune responses in post-giardiasis chronic fatigue syndrome

Author

Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, and Langeland, Nina

Abstract

Background: The role of pathogen specific cellular immune responses against the eliciting pathogen in development of post-infectious chronic fatigue syndrome (PI-CFS) is not known and such studies are difficult to perform. The aim of this study was to evaluate specific anti-Giardia cellular immunity in cases that developed CFS after Giardia infection compared to cases that recovered well. Patients reporting chronic fatigue in a questionnaire study three years after a Giardia outbreak were clinically evaluated five years after the outbreak and grouped according to Fukuda criteria for CFS and idiopathic chronic fatigue. Giardia specific immune responses were evaluated in 39 of these patients by proliferation assay, T cell activation and cytokine release analysis. 20 Giardia exposed non-fatigued individuals and 10 healthy unexposed individuals were recruited as controls. Results: Patients were clinically classified into CFS (n = 15), idiopathic chronic fatigue (n = 5), fatigue from other causes (n = 9) and recovered from fatigue (n = 10). There were statistically significant antigen specific differences between these Giardia exposed groups and unexposed controls. However, we did not find differences between the Giardia exposed fatigue classification groups with regard to CD4 T cell activation, proliferation or cytokine levels in 6 days cultured PBMCs. Interestingly, sCD40L was increased in patients with PI-CFS and other persons with fatigue after Giardia infection compared to the non-fatigued group, and correlated well with fatigue levels at the time of sampling. Conclusion: Our data show antigen specific cellular immune responses in the groups previously exposed to Giardia and increased sCD40L in fatigued patients.

Published

2017

15. Giardia-specific cellular immune responses in post-giardiasis chronic fatigue syndrome

Author

Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, and Langeland, Nina

Abstract

Background: The role of pathogen specific cellular immune responses against the eliciting pathogen in development of post-infectious chronic fatigue syndrome (PI-CFS) is not known and such studies are difficult to perform. The aim of this study was to evaluate specific anti-Giardia cellular immunity in cases that developed CFS after Giardia infection compared to cases that recovered well. Patients reporting chronic fatigue in a questionnaire study three years after a Giardia outbreak were clinically evaluated five years after the outbreak and grouped according to Fukuda criteria for CFS and idiopathic chronic fatigue. Giardia specific immune responses were evaluated in 39 of these patients by proliferation assay, T cell activation and cytokine release analysis. 20 Giardia exposed non-fatigued individuals and 10 healthy unexposed individuals were recruited as controls. Results: Patients were clinically classified into CFS (n = 15), idiopathic chronic fatigue (n = 5), fatigue from other causes (n = 9) and recovered from fatigue (n = 10). There were statistically significant antigen specific differences between these Giardia exposed groups and unexposed controls. However, we did not find differences between the Giardia exposed fatigue classification groups with regard to CD4 T cell activation, proliferation or cytokine levels in 6 days cultured PBMCs. Interestingly, sCD40L was increased in patients with PI-CFS and other persons with fatigue after Giardia infection compared to the non-fatigued group, and correlated well with fatigue levels at the time of sampling. Conclusion: Our data show antigen specific cellular immune responses in the groups previously exposed to Giardia and increased sCD40L in fatigued patients.

Published

2017

16. Giardia-specific cellular immune responses in post-giardiasis chronic fatigue syndrome

Author

Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, and Langeland, Nina

Abstract

Background: The role of pathogen specific cellular immune responses against the eliciting pathogen in development of post-infectious chronic fatigue syndrome (PI-CFS) is not known and such studies are difficult to perform. The aim of this study was to evaluate specific anti-Giardia cellular immunity in cases that developed CFS after Giardia infection compared to cases that recovered well. Patients reporting chronic fatigue in a questionnaire study three years after a Giardia outbreak were clinically evaluated five years after the outbreak and grouped according to Fukuda criteria for CFS and idiopathic chronic fatigue. Giardia specific immune responses were evaluated in 39 of these patients by proliferation assay, T cell activation and cytokine release analysis. 20 Giardia exposed non-fatigued individuals and 10 healthy unexposed individuals were recruited as controls. Results: Patients were clinically classified into CFS (n = 15), idiopathic chronic fatigue (n = 5), fatigue from other causes (n = 9) and recovered from fatigue (n = 10). There were statistically significant antigen specific differences between these Giardia exposed groups and unexposed controls. However, we did not find differences between the Giardia exposed fatigue classification groups with regard to CD4 T cell activation, proliferation or cytokine levels in 6 days cultured PBMCs. Interestingly, sCD40L was increased in patients with PI-CFS and other persons with fatigue after Giardia infection compared to the non-fatigued group, and correlated well with fatigue levels at the time of sampling. Conclusion: Our data show antigen specific cellular immune responses in the groups previously exposed to Giardia and increased sCD40L in fatigued patients.

Published

2017

17. Giardia-specific cellular immune responses in post-giardiasis chronic fatigue syndrome

Author

Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, and Langeland, Nina

Abstract

Background: The role of pathogen specific cellular immune responses against the eliciting pathogen in development of post-infectious chronic fatigue syndrome (PI-CFS) is not known and such studies are difficult to perform. The aim of this study was to evaluate specific anti-Giardia cellular immunity in cases that developed CFS after Giardia infection compared to cases that recovered well. Patients reporting chronic fatigue in a questionnaire study three years after a Giardia outbreak were clinically evaluated five years after the outbreak and grouped according to Fukuda criteria for CFS and idiopathic chronic fatigue. Giardia specific immune responses were evaluated in 39 of these patients by proliferation assay, T cell activation and cytokine release analysis. 20 Giardia exposed non-fatigued individuals and 10 healthy unexposed individuals were recruited as controls. Results: Patients were clinically classified into CFS (n = 15), idiopathic chronic fatigue (n = 5), fatigue from other causes (n = 9) and recovered from fatigue (n = 10). There were statistically significant antigen specific differences between these Giardia exposed groups and unexposed controls. However, we did not find differences between the Giardia exposed fatigue classification groups with regard to CD4 T cell activation, proliferation or cytokine levels in 6 days cultured PBMCs. Interestingly, sCD40L was increased in patients with PI-CFS and other persons with fatigue after Giardia infection compared to the non-fatigued group, and correlated well with fatigue levels at the time of sampling. Conclusion: Our data show antigen specific cellular immune responses in the groups previously exposed to Giardia and increased sCD40L in fatigued patients.

Published

2017

18. Giardia-specific cellular immune responses in post-giardiasis chronic fatigue syndrome

Author

Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Morch, Kristine, Rye, Kristin Paulsen, Sornes, Steinar, Svärd, Staffan, Bruserud, Oystein, and Langeland, Nina

Abstract

Background: The role of pathogen specific cellular immune responses against the eliciting pathogen in development of post-infectious chronic fatigue syndrome (PI-CFS) is not known and such studies are difficult to perform. The aim of this study was to evaluate specific anti-Giardia cellular immunity in cases that developed CFS after Giardia infection compared to cases that recovered well. Patients reporting chronic fatigue in a questionnaire study three years after a Giardia outbreak were clinically evaluated five years after the outbreak and grouped according to Fukuda criteria for CFS and idiopathic chronic fatigue. Giardia specific immune responses were evaluated in 39 of these patients by proliferation assay, T cell activation and cytokine release analysis. 20 Giardia exposed non-fatigued individuals and 10 healthy unexposed individuals were recruited as controls. Results: Patients were clinically classified into CFS (n = 15), idiopathic chronic fatigue (n = 5), fatigue from other causes (n = 9) and recovered from fatigue (n = 10). There were statistically significant antigen specific differences between these Giardia exposed groups and unexposed controls. However, we did not find differences between the Giardia exposed fatigue classification groups with regard to CD4 T cell activation, proliferation or cytokine levels in 6 days cultured PBMCs. Interestingly, sCD40L was increased in patients with PI-CFS and other persons with fatigue after Giardia infection compared to the non-fatigued group, and correlated well with fatigue levels at the time of sampling. Conclusion: Our data show antigen specific cellular immune responses in the groups previously exposed to Giardia and increased sCD40L in fatigued patients.

Published

2017

19. Human Memory CD4+ T Cell Immune Responses against Giardia lamblia

Author

Saghaug, Christina Skar, Sornes, Steinar, Peirasmaki, Dimitra, Svärd, Staffan, Langeland, Nina, Hanevik, Kurt, Saghaug, Christina Skar, Sornes, Steinar, Peirasmaki, Dimitra, Svärd, Staffan, Langeland, Nina, and Hanevik, Kurt

Abstract

The intestinal protozoan parasite Giardia lamblia may cause severe prolonged diarrheal disease or pass unnoticed as an asymptomatic infection. T cells seem to play an important role in the immune response to Giardia infection, and memory responses may last years. Recently, T(H)17 responses have been found in three animal studies of Giardia infection. The aim of this study was to characterize the human CD4+ T cell responses to Giardia. Peripheral blood mononuclear cells (PBMCs) were obtained from 21 returning travelers with recent or ongoing giardiasis and 12 low-risk healthy controls and stimulated in vitro with Giardia lamblia proteins. Production of tumor necrosis factor alpha (TNF-alpha), gamma interferon, interleukin-17A (IL-17A), IL-10, and IL-4 was measured in CD4+ effector memory (EM) T cells after 24 h by flow cytometry. After 6 days of culture, activation and proliferation were measured by flow cytometry, while an array of inflammatory cytokine levels in supernatants were measured with multiplex assays. We found the number of IL-17A-producing CD4+ EM T cells, as well as that of cells simultaneously producing both IL-17A and TNF-alpha, to be significantly elevated in the Giardia-exposed individuals after 24 h of antigen stimulation. In supernatants of PBMCs stimulated with Giardia antigens for 6 days, we found inflammation-associated cytokines, including 1L-17A, as well as CD4+ T cell activation and proliferation, to be significantly elevated in the Giardia-exposed individuals. We conclude that symptomatic Giardia infection in humans induces a CD4+ EM T cell response of which IL-17A production seems to be an important component.

Published

2016

20. Short interferon and ribavirin treatment for HCV genotype 2 or 3 infection: NORDynamIC trial and real-life experience

Author

University of Helsinki, Clinicum, University of Helsinki, Gastroenterologian yksikkö, Waldenstrom, Jesper, Farkkila, Martti, Rembeck, Karolina, Norkrans, Gunnar, Langeland, Nina, Morch, Kristine, Pedersen, Court, Rauning Buhl, Mads, Nieminen, Urpo, Nuutinen, Hannu, Alsio, Asa, Holmstrom, Lars, Jungnelius, Rolf, Lund, Katarina, Rubensson, Anders, Torell, Erik, Westin, Johan, Lagging, Martin, University of Helsinki, Clinicum, University of Helsinki, Gastroenterologian yksikkö, Waldenstrom, Jesper, Farkkila, Martti, Rembeck, Karolina, Norkrans, Gunnar, Langeland, Nina, Morch, Kristine, Pedersen, Court, Rauning Buhl, Mads, Nieminen, Urpo, Nuutinen, Hannu, Alsio, Asa, Holmstrom, Lars, Jungnelius, Rolf, Lund, Katarina, Rubensson, Anders, Torell, Erik, Westin, Johan, and Lagging, Martin

Published

2016

21. Complement Activation Correlates With Disease Severity and Contributes to Cytokine Responses in Plasmodium falciparum Malaria

Author

Berg, Aase, Otterdal, Karl, Patel, Sam, Gonca, Miguel, David, Catarina, Dalen, Ingvild, Nymo, Stig, Nilsson, Margareta, Nordling, Sofia, Magnusson, Peetra, Ueland, Thor, Prato, Mauro, Giribaldi, Giuliana, Mollnes, Tom Eirik, Aukrust, Pål, Langeland, Nina, Nilsson, Per, Berg, Aase, Otterdal, Karl, Patel, Sam, Gonca, Miguel, David, Catarina, Dalen, Ingvild, Nymo, Stig, Nilsson, Margareta, Nordling, Sofia, Magnusson, Peetra, Ueland, Thor, Prato, Mauro, Giribaldi, Giuliana, Mollnes, Tom Eirik, Aukrust, Pål, Langeland, Nina, and Nilsson, Per

Abstract

The impact of complement activation and its possible relation to cytokine responses during malaria pathology was investigated in plasma samples from patients with confirmed Plasmodium falciparum malaria and in human whole-blood specimens stimulated with malaria-relevant agents ex vivo. Complement was significantly activated in the malaria cohort, compared with healthy controls, and was positively correlated with disease severity and with certain cytokines, in particular interleukin 8 (IL-8)/CXCL8. This was confirmed in ex vivo-stimulated blood specimens, in which complement inhibition significantly reduced IL-8/CXCL8 release. P. falciparum malaria is associated with systemic complement activation and complement-dependent release of inflammatory cytokines, of which IL-8/CXCL8 is particularly prominent.

Published

2015

22. Genetic relatedness and risk factor analysis of ampicillin-resistant and high-level gentamicin-resistant enterococci causing bloodstream infections in Tanzanian children

Author

Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, Blomberg, Bjørn, Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, and Blomberg, Bjørn

Published

2015

23. Genetic relatedness and risk factor analysis of ampicillin-resistant and high-level gentamicin-resistant enterococci causing bloodstream infections in Tanzanian children

Author

Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, Blomberg, Bjørn, Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, and Blomberg, Bjørn

Published

2015

24. Genetic relatedness and risk factor analysis of ampicillin-resistant and high-level gentamicin-resistant enterococci causing bloodstream infections in Tanzanian children

Author

Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, Blomberg, Bjørn, Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, and Blomberg, Bjørn

Published

2015

25. Genetic relatedness and risk factor analysis of ampicillin-resistant and high-level gentamicin-resistant enterococci causing bloodstream infections in Tanzanian children

Author

MMB Infectiepreventie, Infection & Immunity, Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, Blomberg, Bjørn, MMB Infectiepreventie, Infection & Immunity, Aamodt, Håvard, Mohn, Stein Christian, Maselle, Samuel, Manji, Karim P., Willems, Rob, Jureen, Roland, Langeland, Nina, and Blomberg, Bjørn

Published

2015

26. Complement Activation Correlates With Disease Severity and Contributes to Cytokine Responses in Plasmodium falciparum Malaria.

Author

Berg, Aase, Otterdal, Kari, Patel, Sam, Gonca, Miguel, David, Catarina, Dalen, Ingvild, Nymo, Stig, Nilsson, Margareta, Nordling, Sofia, Magnusson, Peetra U, Ueland, Thor, Prato, Mauro, Giribaldi, Giuliana, Mollnes, Tom Eirik, Aukrust, Pål, Langeland, Nina, Nilsson, Per H., Berg, Aase, Otterdal, Kari, Patel, Sam, Gonca, Miguel, David, Catarina, Dalen, Ingvild, Nymo, Stig, Nilsson, Margareta, Nordling, Sofia, Magnusson, Peetra U, Ueland, Thor, Prato, Mauro, Giribaldi, Giuliana, Mollnes, Tom Eirik, Aukrust, Pål, Langeland, Nina, and Nilsson, Per H.

Abstract

The impact of complement activation and its possible relation to cytokine responses during malaria pathology was investigated in plasma samples from patients with confirmed Plasmodium falciparum malaria and in human whole-blood specimens stimulated with malaria-relevant agents ex vivo. Complement was significantly activated in the malaria cohort, compared with healthy controls, and was positively correlated with disease severity and with certain cytokines, in particular interleukin 8 (IL-8)/CXCL8. This was confirmed in ex vivo-stimulated blood specimens, in which complement inhibition significantly reduced IL-8/CXCL8 release. P. falciparum malaria is associated with systemic complement activation and complement-dependent release of inflammatory cytokines, of which IL-8/CXCL8 is particularly prominent.

Published

2015

27. A Novel Fibrosis Index Comprising a Non-Cholesterol Sterol Accurately Predicts HCV-Related Liver Cirrhosis

Author

University of Helsinki, Clinicum, Ydreborg, Magdalena, Lisovskaja, Vera, Lagging, Martin, Christensen, Peer Brehm, Langeland, Nina, Buhl, Mads Rauning, Pedersen, Court, Morch, Kristine, Wejstal, Rune, Norkrans, Gunnar, Lindh, Magnus, Farkkila, Martti, Westin, Johan, University of Helsinki, Clinicum, Ydreborg, Magdalena, Lisovskaja, Vera, Lagging, Martin, Christensen, Peer Brehm, Langeland, Nina, Buhl, Mads Rauning, Pedersen, Court, Morch, Kristine, Wejstal, Rune, Norkrans, Gunnar, Lindh, Magnus, Farkkila, Martti, and Westin, Johan

Published

2014

28. Impact of Obesity on the Bioavailability of Peginterferon-alpha 2a and Ribavirin and Treatment Outcome for Chronic Hepatitis C Genotype 2 or 3

Author

University of Helsinki, Clinicum, Alsio, Asa, Rembeck, Karolina, Askarieh, Galia, Christensen, Peer Brehm, Färkkilä, Martti Antero, Langeland, Nina, Buhl, Mads Rauning, Pedersen, Court, Morch, Kristine, Haagmans, Bart L., Nasic, Salmir, Westin, Johan, Hellstrand, Kristoffer, Norkrans, Gunnar, Lagging, Martin, University of Helsinki, Clinicum, Alsio, Asa, Rembeck, Karolina, Askarieh, Galia, Christensen, Peer Brehm, Färkkilä, Martti Antero, Langeland, Nina, Buhl, Mads Rauning, Pedersen, Court, Morch, Kristine, Haagmans, Bart L., Nasic, Salmir, Westin, Johan, Hellstrand, Kristoffer, Norkrans, Gunnar, and Lagging, Martin

Published

2012

29. Human Cellular Immune Response Against Giardia lamblia 5 Years After Acute Giardiasis

Author

Hanevik, Kurt, Kristoffersen, Einar, Svärd, Staffan, Bruserud, Oystein, Ringqvist, Emma, Sornes, Steinar, Langeland, Nina, Hanevik, Kurt, Kristoffersen, Einar, Svärd, Staffan, Bruserud, Oystein, Ringqvist, Emma, Sornes, Steinar, and Langeland, Nina

Abstract

Background. Clinical and epidemiological studies have suggested the development of acquired immunity in individuals previously infected with Giardia lamblia. However, there are no data on the long-term cellular immunity and genotype cross-reactivity. An outbreak of assemblage B giardiasis in a nonendemic area made it possible to evaluate the long-term cellular mediated immunity and its specificity toward the 2 Giardia assemblages known to infect humans. Methods. Peripheral blood mononuclear cells from 19 individuals infected with Giardia assemblage B 5 years previously and from 10 uninfected controls were cultured with antigens from assemblage A and B Giardia trophozoites for 6 days. Cell-mediated immunity was measured by a (3)H-thymidine proliferation assay and flow cytometric analysis of activation markers HLA-DR, CD45RO, CD25, and CD26 in T-cell subsets. Results. Proliferation responses were significantly elevated in the group previously exposed to Giardia for nearly all Giardia antigens tested. Individual responses toward Giardia trophozoite whole cell, cytosolic, and excretory-secretory antigens from both assemblages correlated well. Activation marker responses were mainly seen in CD4 T cells. Conclusions. G. lamblia infection induces long-term, albeit variable, cellular immune responses that are not assemblage specific and that are largely driven by CD4 T-cell activation.

Published

2011

30. Evaluation of depression as a risk factor for treatment failure in chronic hepatitis C

Author

Leutscher, Peter Derek Christian, Lagging, Martin, Buhl, Mads Rauning, Pedersen, Court, Norkrans, Gunnar, Langeland, Nina, Mørch, Kristine, Färkkilä, Martti, Hjerrild, Simon, Hellstrand, Kristoffer, Bech, Per, Leutscher, Peter Derek Christian, Lagging, Martin, Buhl, Mads Rauning, Pedersen, Court, Norkrans, Gunnar, Langeland, Nina, Mørch, Kristine, Färkkilä, Martti, Hjerrild, Simon, Hellstrand, Kristoffer, and Bech, Per

Abstract

The Major Depression Inventory (MDI) was used to estimate the value of routine medical interviews in diagnosing major depression among patients receiving peginterferon alfa-2a and ribavirin therapy for chronic hepatitis C virus (HCV) infection (n = 325). According to criteria from the MDI and Diagnostic and Statistical Manual of Mental Disorders (DSM-IV), 19 patients (6%) had major depression at baseline. An additional 114 (37%) developed depression while on HCV combination therapy, with baseline MDI score and female sex independently predicting the emergence of major depression during treatment in a multivariate analysis. Only 36 (32%) of the 114 patients developing major depression according to MDI/DSM-IV criteria were correctly diagnosed during routine medical interviews. The emergence of major depression frequently led to premature discontinuation of peginterferon/ribavirin therapy, and an on-treatment MDI score increment exceeding 30 points (i.e., a validated marker of idiopathic DSM-IV major depression) was correlated with impaired outcome of HCV therapy (P = 0.02). This difference was even more pronounced among patients with an on-treatment increase in MDI score greater than 35 points (P = 0.003). Conclusion: We conclude that (1) depressive symptoms among patients undergoing HCV therapy are commonly overlooked by routine clinical interviews, (2) the emergence of depression compromises the outcome of HCV therapy, and (3) the MDI scale may be useful in identifying patients at risk for treatment-induced depression.

Published

2010

31. Evaluation of depression as a risk factor for treatment failure in chronic hepatitis C

Author

Leutscher, Peter Derek Christian, Lagging, Martin, Buhl, Mads Rauning, Pedersen, Court, Norkrans, Gunnar, Langeland, Nina, Mørch, Kristine, Färkkilä, Martti, Hjerrild, Simon, Hellstrand, Kristoffer, Bech, Per, Leutscher, Peter Derek Christian, Lagging, Martin, Buhl, Mads Rauning, Pedersen, Court, Norkrans, Gunnar, Langeland, Nina, Mørch, Kristine, Färkkilä, Martti, Hjerrild, Simon, Hellstrand, Kristoffer, and Bech, Per

Abstract

The Major Depression Inventory (MDI) was used to estimate the value of routine medical interviews in diagnosing major depression among patients receiving peginterferon alfa-2a and ribavirin therapy for chronic hepatitis C virus (HCV) infection (n = 325). According to criteria from the MDI and Diagnostic and Statistical Manual of Mental Disorders (DSM-IV), 19 patients (6%) had major depression at baseline. An additional 114 (37%) developed depression while on HCV combination therapy, with baseline MDI score and female sex independently predicting the emergence of major depression during treatment in a multivariate analysis. Only 36 (32%) of the 114 patients developing major depression according to MDI/DSM-IV criteria were correctly diagnosed during routine medical interviews. The emergence of major depression frequently led to premature discontinuation of peginterferon/ribavirin therapy, and an on-treatment MDI score increment exceeding 30 points (i.e., a validated marker of idiopathic DSM-IV major depression) was correlated with impaired outcome of HCV therapy (P = 0.02). This difference was even more pronounced among patients with an on-treatment increase in MDI score greater than 35 points (P = 0.003). Conclusion: We conclude that (1) depressive symptoms among patients undergoing HCV therapy are commonly overlooked by routine clinical interviews, (2) the emergence of depression compromises the outcome of HCV therapy, and (3) the MDI scale may be useful in identifying patients at risk for treatment-induced depression.

Published

2010