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1. Cerebral near infrared spectroscopy oximetry in extremely preterm infants : phase II randomised clinical trial

Author

Hyttel-Sorensen, Simon, Pellicer, Adelina, Alderliesten, Thomas, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Franz, Axel R, Fumagalli, Monica, Gluud, Christian, Grevstad, Berit, Hagmann, Cornelia, Lemmers, Petra, van Oeveren, Wim, Pichler, Gerhard, Plomgaard, Anne Mette, Riera, Joan, Sanchez, Laura, Winkel, Per, Wolf, Martin, and Greisen, Gorm

Published
2015

4. Cerebral near infrared spectroscopy oximetry in extremely preterm infants: Phase II randomised clinical trial

Author

MS Neonatologie, Brain, Hyttel-Sorensen, Simon, Pellicer, Adelina, Alderliesten, Thomas, Austin, Topun, Van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Franz, Axel R., Fumagalli, Monica, Gluud, Christian, Grevstad, Berit, Hagmann, Cornelia, Lemmers, Petra, Van Oeveren, Wim, Pichler, Gerhard, Plomgaard, Anne Mette, Riera, Joan, Sanchez, Laura, Winkel, Per, Wolf, Martin, Greisen, Gorm, MS Neonatologie, Brain, Hyttel-Sorensen, Simon, Pellicer, Adelina, Alderliesten, Thomas, Austin, Topun, Van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Franz, Axel R., Fumagalli, Monica, Gluud, Christian, Grevstad, Berit, Hagmann, Cornelia, Lemmers, Petra, Van Oeveren, Wim, Pichler, Gerhard, Plomgaard, Anne Mette, Riera, Joan, Sanchez, Laura, Winkel, Per, Wolf, Martin, and Greisen, Gorm

Published
2015

5. Cerebral near infrared spectroscopy oximetry in extremely preterm infants:phase II randomised clinical trial

Author

Hyttel-Sorensen, Simon, Pellicer, Adelina, Alderliesten, Thomas, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Franz, Axel R, Fumagalli, Monica, Gluud, Christian, Grevstad, Berit, Hagmann, Cornelia, Lemmers, Petra, van Oeveren, Wim, Pichler, Gerhard, Plomgaard, Anne Mette, Riera, Joan, Sanchez, Laura, Winkel, Per, Wolf, Martin, Greisen, Gorm, Hyttel-Sorensen, Simon, Pellicer, Adelina, Alderliesten, Thomas, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Franz, Axel R, Fumagalli, Monica, Gluud, Christian, Grevstad, Berit, Hagmann, Cornelia, Lemmers, Petra, van Oeveren, Wim, Pichler, Gerhard, Plomgaard, Anne Mette, Riera, Joan, Sanchez, Laura, Winkel, Per, Wolf, Martin, and Greisen, Gorm

Abstract

OBJECTIVE: To determine if it is possible to stabilise the cerebral oxygenation of extremely preterm infants monitored by cerebral near infrared spectroscopy (NIRS) oximetry.DESIGN: Phase II randomised, single blinded, parallel clinical trial.SETTING: Eight tertiary neonatal intensive care units in eight European countries.PARTICIPANTS: 166 extremely preterm infants born before 28 weeks of gestation: 86 were randomised to cerebral NIRS monitoring and 80 to blinded NIRS monitoring. The only exclusion criterion was a decision not to provide life support.INTERVENTIONS: Monitoring of cerebral oxygenation using NIRS in combination with a dedicated treatment guideline during the first 72 hours of life (experimental) compared with blinded NIRS oxygenation monitoring with standard care (control).MAIN OUTCOME MEASURES: The primary outcome measure was the time spent outside the target range of 55-85% for cerebral oxygenation multiplied by the mean absolute deviation, expressed in %hours (burden of hypoxia and hyperoxia). One hour with an oxygenation of 50% gives 5%hours of hypoxia. Secondary outcomes were all cause mortality at term equivalent age and a brain injury score assessed by cerebral ultrasonography.RANDOMISATION: Allocation sequence 1:1 with block sizes 4 and 6 in random order concealed for the investigators. The allocation was stratified for gestational age (<26 weeks or ≥ 26 weeks).BLINDING: Cerebral oxygenation measurements were blinded in the control group. All outcome assessors were blinded to group allocation.RESULTS: The 86 infants randomised to the NIRS group had a median burden of hypoxia and hyperoxia of 36.1%hours (interquartile range 9.2-79.5%hours) compared with 81.3 (38.5-181.3) %hours in the control group, a reduction of 58% (95% confidence interval 35% to 73%, P<0.001). In the experimental group the median burden of hypoxia was 16.6 (interquartile range 5.4-68.1) %hours, compared with 5

Published
2015

6. Targeting intensive versus conventional glycaemic control for type 1 diabetes mellitus:a systematic review with meta-analyses and trial sequential analyses of randomised clinical trials

Author

Kähler, Pernille, Grevstad, Berit, Almdal, Thomas, Gluud, Christian, Wetterslev, Jørn, Vaag, Allan, Hemmingsen, Bianca, Kähler, Pernille, Grevstad, Berit, Almdal, Thomas, Gluud, Christian, Wetterslev, Jørn, Vaag, Allan, and Hemmingsen, Bianca

Abstract

OBJECTIVE: To assess the benefits and harms of targeting intensive versus conventional glycaemic control in patients with type 1 diabetes mellitus.DESIGN: A systematic review with meta-analyses and trial sequential analyses of randomised clinical trials.DATA SOURCES: The Cochrane Library, MEDLINE, EMBASE, Science Citation Index Expanded and LILACS to January 2013.STUDY SELECTION: Randomised clinical trials that prespecified different targets of glycaemic control in participants at any age with type 1 diabetes mellitus were included.DATA EXTRACTION: Two authors independently assessed studies for inclusion and extracted data.RESULTS: 18 randomised clinical trials included 2254 participants with type 1 diabetes mellitus. All trials had high risk of bias. There was no statistically significant effect of targeting intensive glycaemic control on all-cause mortality (risk ratio 1.16, 95% CI 0.65 to 2.08) or cardiovascular mortality (0.49, 0.19 to 1.24). Targeting intensive glycaemic control reduced the relative risks for the composite macrovascular outcome (0.63, 0.41 to 0.96; p=0.03), and nephropathy (0.37, 0.27 to 0.50; p<0.00001. The effect estimates of retinopathy, ketoacidosis and retinal photocoagulation were not consistently statistically significant between random and fixed effects models. The risk of severe hypoglycaemia was significantly increased with intensive glycaemic targets (1.40, 1.01 to 1.94). Trial sequential analyses showed that the amount of data needed to demonstrate a relative risk reduction of 10% were, in general, inadequate.CONCLUSIONS: There was no significant effect towards improved all-cause mortality when targeting intensive glycaemic control compared with conventional glycaemic control. However, there may be beneficial effects of targeting intensive glycaemic control on the composite macrovascular outcome and on nephropathy, and detrimental effects on severe hypoglycaemia. Notably, the data for

Published
2014

8. A phase II randomized clinical trial on cerebral near-infrared spectroscopy plus a treatment guideline versus treatment as usual for extremely preterm infants during the first three days of life (SafeBoosC) : study protocol for a randomized controlled trial

Author

Hyttel-Sorensen, Simon, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Fumagalli, Monica, Greisen, Gorm, Grevstad, Berit, Hagmann, Cornelia, Hellström-Westas, Lena, Lemmers, Petra, Lindschou, Jane, Naulaers, Gunnar, van Oeveren, Wim, Pellicer, Adelina, Pichler, Gerhard, Roll, Claudia, Skoog, Maria, Winkel, Per, Wolf, Martin, Gluud, Christian, Hyttel-Sorensen, Simon, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Fumagalli, Monica, Greisen, Gorm, Grevstad, Berit, Hagmann, Cornelia, Hellström-Westas, Lena, Lemmers, Petra, Lindschou, Jane, Naulaers, Gunnar, van Oeveren, Wim, Pellicer, Adelina, Pichler, Gerhard, Roll, Claudia, Skoog, Maria, Winkel, Per, Wolf, Martin, and Gluud, Christian

Abstract

Background: Every year in Europe about 25,000 infants are born extremely preterm. These infants have a 20% mortality rate, and 25% of survivors have severe long-term cerebral impairment. Preventative measures are key to reduce mortality and morbidity in an extremely preterm population. The primary objective of the SafeBoosC phase II trial is to examine if it is possible to stabilize the cerebral oxygenation of extremely preterm infants during the first 72 hours of life through the application of cerebral near-infrared spectroscopy (NIRS) oximetry and implementation of an clinical treatment guideline based on intervention thresholds of cerebral regional tissue saturation rStO(2). Methods/Design: SafeBoosC is a randomized, blinded, multinational, phase II clinical trial. The inclusion criteria are: neonates born more than 12 weeks preterm; decision to conduct full life support; parental informed consent; and possibility to place the cerebral NIRS oximeter within 3 hours after birth. The infants will be randomized into one of two groups. Both groups will have a cerebral oximeter monitoring device placed within three hours of birth. In the experimental group, the cerebral oxygenation reading will supplement the standard treatment using a predefined treatment guideline. In the control group, the cerebral oxygenation reading will not be visible and the infant will be treated according to the local standards. The primary outcome is the multiplication of the duration and magnitude of rStO(2) values outside the target ranges of 55% to 85%, that is, the 'burden of hypoxia and hyperoxia' expressed in '%hours'. To detect a 50% difference between the experimental and control group in %hours, 166 infants in total must be randomized. Secondary outcomes are mortality at term date, cerebral ultrasound score, and interburst intervals on an amplitude-integrated electroencephalogram at 64 hours of life and explorative outcomes include neurodevelopmental outcome at 2 years corrected age

Published
2013
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9. A phase II randomized clinical trial on cerebral near-infrared spectroscopy plus a treatment guideline versus treatment as usual for extremely preterm infants during the first three days of life (SafeBoosC):study protocol for a randomized controlled trial

Author

Hyttel-Sorensen, Simon, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Fumagalli, Monica, Greisen, Gorm, Grevstad, Berit, Hagmann, Cornelia, Hellström-Westas, Lena, Lemmers, Petra, Lindschou, Jane, Naulaers, Gunnar, van Oeveren, Wim, Pellicer, Adelina, Pichler, Gerhard, Roll, Claudia, Skoog, Maria, Winkel, Per, Wolf, Martin, Gluud, Christian, Hyttel-Sorensen, Simon, Austin, Topun, van Bel, Frank, Benders, Manon, Claris, Olivier, Dempsey, Eugene, Fumagalli, Monica, Greisen, Gorm, Grevstad, Berit, Hagmann, Cornelia, Hellström-Westas, Lena, Lemmers, Petra, Lindschou, Jane, Naulaers, Gunnar, van Oeveren, Wim, Pellicer, Adelina, Pichler, Gerhard, Roll, Claudia, Skoog, Maria, Winkel, Per, Wolf, Martin, and Gluud, Christian

Published
2013

10. Selected HIV-1 Env Trimeric Formulations Act as Potent Immunogens in a Rabbit Vaccination Model

Author

Heyndrickx, Leo, Stewart-Jones, Guillaume, Jansson, Marianne, Schuitemaker, Hanneke, Bowles, Emma, Buonaguro, Luigi, Grevstad, Berit, Vinner, Lasse, Vereecken, Katleen, Parker, Joe, Ramaswamy, Meghna, Biswas, Priscilla, Vanham, Guido, Scarlatti, Gabriella, Fomsgaard, Anders, Heyndrickx, Leo, Stewart-Jones, Guillaume, Jansson, Marianne, Schuitemaker, Hanneke, Bowles, Emma, Buonaguro, Luigi, Grevstad, Berit, Vinner, Lasse, Vereecken, Katleen, Parker, Joe, Ramaswamy, Meghna, Biswas, Priscilla, Vanham, Guido, Scarlatti, Gabriella, and Fomsgaard, Anders

Abstract

Background: Ten to 30% of HIV-1 infected subjects develop broadly neutralizing antibodies (bNAbs) during chronic infection. We hypothesized that immunizing rabbits with viral envelope glycoproteins (Envs) from these patients may induce bNAbs, when formulated as a trimeric protein and in the presence of an adjuvant. Methods: Based on in vitro neutralizing activity in serum, patients with bNAbs were selected for cloning of their HIV-1 Env. Seven stable soluble trimeric gp140 proteins were generated from sequences derived from four adults and two children infected with either clade A or B HIV-1. From one of the clade A Envs both the monomeric and trimeric Env were produced for comparison. Rabbits were immunized with soluble gp120 or trimeric gp140 proteins in combination with the adjuvant dimethyl dioctadecyl ammonium/trehalose dibehenate (CAF01). Env binding in rabbit immune serum was determined using ELISAs based on gp120-IIIB protein. Neutralizing activity of IgG purified from rabbit immune sera was measured with the pseudovirus-TZMbl assay and a PBMC-based neutralization assay for selected experiments. Results: It was initially established that gp140 trimers induce better antibody responses over gp120 monomers and that the adjuvant CAF01 was necessary for such strong responses. Gp140 trimers, based on HIV-1 variants from patients with bNAbs, were able to elicit both gp120(IIIB) specific IgG and NAbs to Tier 1 viruses of different subtypes. Potency of NAbs closely correlated with titers, and an gp120-binding IgG titer above a threshold of 100,000 was predictive of neutralization capability. Finally, peptide inhibition experiments showed that a large fraction of the neutralizing IgG was directed against the gp120 V3 region. Conclusions: Our results indicate that the strategy of reverse immunology based on selected Env sequences is promising when immunogens are delivered as stabilized trimers in CAF01 adjuvant and that the rabbit is a valuable model for HIV vaccine st

Published
2013

11. Characterization of humoral responses to soluble trimeric HIV gp140 from a clade A Ugandan field isolate

Author

Visciano, Maria Luisa, Tagliamonte, Maria, Stewart-Jones, Guillaume, Heyndrickx, Leo, Vanham, Guido, Jansson, Marianne, Fomsgaard, Anders, Grevstad, Berit, Ramaswamy, Meghna, Buonaguro, Franco M., Tornesello, Maria Lina, Biswas, Priscilla, Scarlatti, Gabriella, Buonaguro, Luigi, Visciano, Maria Luisa, Tagliamonte, Maria, Stewart-Jones, Guillaume, Heyndrickx, Leo, Vanham, Guido, Jansson, Marianne, Fomsgaard, Anders, Grevstad, Berit, Ramaswamy, Meghna, Buonaguro, Franco M., Tornesello, Maria Lina, Biswas, Priscilla, Scarlatti, Gabriella, and Buonaguro, Luigi

Abstract

Trimeric soluble forms of HIV gp140 envelope glycoproteins represent one of the closest molecular structures compared to native spikes present on intact virus particles. Trimeric soluble gp140 have been generated by several groups and such molecules have been shown to induce antibodies with neutralizing activity against homologous and heterologous viruses. In the present study, we generated a recombinant trimeric soluble gp140, derived from a previously identified Ugandan A-clade HIV field isolate (gp140(94UG018)). Antibodies elicited in immunized rabbits show a broad binding pattern to HIV envelopes of different clades. An epitope mapping analysis reveals that, on average, the binding is mostly focused on the C1, C2, V3, V5 and C5 regions. Immune sera show neutralization activity to Tier 1 isolates of different clades, demonstrating cross clade neutralizing activity which needs to be further broadened by possible structural modifications of the clade A gp140(94UG018). Our results provide a rationale for the design and evaluation of immunogens and the clade A gp140(94UG018) shows promising characteristics for potential involvement in an effective HIV vaccine with broad activity.

Published
2013

12. Optimization of HIV-1 Envelope DNA Vaccine Candidates within Three Different Animal Models, Guinea Pigs, Rabbits and Cynomolgus Macaques

Author

Borggren, Marie, primary, Vinner, Lasse, additional, Andresen, Betina, additional, Grevstad, Berit, additional, Repits, Johanna, additional, Melchers, Mark, additional, Elvang, Tara, additional, Sanders, Rogier, additional, Martinon, Frédéric, additional, Dereuddre-Bosquet, Nathalie, additional, Bowles, Emma, additional, Stewart-Jones, Guillaume, additional, Biswas, Priscilla, additional, Scarlatti, Gabriella, additional, Jansson, Marianne, additional, Heyndrickx, Leo, additional, Grand, Roger, additional, and Fomsgaard, Anders, additional

Published
2013
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14. A phase II randomized clinical trial on cerebral near-infrared spectroscopy plus a treatment guideline versus treatment as usual for extremely preterm infants during the first three days of life (SafeBoosC): study protocol for a randomized controlled trial

Author

Hyttel-Sorensen, Simon, primary, Austin, Topun, additional, van Bel, Frank, additional, Benders, Manon, additional, Claris, Olivier, additional, Dempsey, Eugene, additional, Fumagalli, Monica, additional, Greisen, Gorm, additional, Grevstad, Berit, additional, Hagmann, Cornelia, additional, Hellstr�m-Westas, Lena, additional, Lemmers, Petra, additional, Lindschou, Jane, additional, Naulaers, Gunnar, additional, van Oeveren, Wim, additional, Pellicer, Adelina, additional, Pichler, Gerhard, additional, Roll, Claudia, additional, Skoog, Maria, additional, Winkel, Per, additional, Wolf, Martin, additional, and Gluud, Christian, additional

Published
2013
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15. Differential induction of immunoglobulin G to Plasmodium falciparum variant surface antigens during the transmission season in Daraweesh, Sudan

Author

Nielsen, Morten A, Grevstad, Berit, A-Elgadir, Thoraya M E, Kurtzhals, Jørgen, Giha, Haider, Staalsoe, Trine, Hviid, Lars, Theander, Thor G, Nielsen, Morten A, Grevstad, Berit, A-Elgadir, Thoraya M E, Kurtzhals, Jørgen, Giha, Haider, Staalsoe, Trine, Hviid, Lars, and Theander, Thor G

Abstract

Udgivelsesdato: 2005-Aug-1, BACKGROUND: The acquisition of immunoglobulin (Ig) G to variant surface antigens (VSAs) seems important for the development of protective immunity against malaria. Unlike VSAs expressed by parasite isolates associated with uncomplicated malaria, VSAs expressed by parasite isolates associated with severe malaria (VSA(SM)) are frequently recognized by IgG. METHODS: We analyzed levels of anti-VSA IgG in 57 individuals in Daraweesh, Sudan, before and after the transmission season. IgG responses to 79 Plasmodium falciparum isolates from children with defined malaria syndromes and exposed to high transmission in a different part of Africa were also analyzed. RESULTS: After the transmission season, individuals with malaria had an increase in IgG recognition to 25.8% (95% confidence interval [CI], 19.9%-31.7%) and a decrease in IgG recognition to 7.6% (95% CI, 4.4%-10.8%) of 79 parasite isolates, and individuals without malaria had an increase in IgG recognition to 8.1% (95% CI, 6.0%-10.2%) and a decrease in IgG recognition to 11.9% (95% CI, 7.0%-16.8%) of 79 parasite isolates. Most newly acquired IgG responses were against parasite isolates expressing VSAs(SM) that are frequently recognized by IgG. CONCLUSIONS: Anti-VSA IgG levels decrease in the absence of infection, and an episode of clinical malaria induces IgG against a range of VSAs, particularly VSAs(SM).

Published
2005

16. Geographical and temporal conservation of antibody recognition of Plasmodium falciparum variant surface antigens

Author

Nielsen, Morten A, Vestergaard, Lasse S, Lusingu, John, Kurtzhals, Jørgen, Giha, Haider A, Grevstad, Berit, Goka, Bamenla Q, Lemnge, Martha M, Jensen, James B, Akanmori, Bartholomew D, Theander, Thor G, Staalsoe, Trine, Hviid, Lars, Nielsen, Morten A, Vestergaard, Lasse S, Lusingu, John, Kurtzhals, Jørgen, Giha, Haider A, Grevstad, Berit, Goka, Bamenla Q, Lemnge, Martha M, Jensen, James B, Akanmori, Bartholomew D, Theander, Thor G, Staalsoe, Trine, and Hviid, Lars

Abstract

Udgivelsesdato: 2004-Jun, The slow acquisition of protection against Plasmodium falciparum malaria probably reflects the extensive diversity of important antigens. The variant surface antigens (VSA) that mediate parasite adhesion to a range of host molecules are regarded as important targets of acquired protective immunity, but their diversity makes them questionable vaccine candidates. We determined levels of VSA-specific immunoglobulin G (IgG) in human plasma collected at four geographically distant and epidemiologically distinct localities with specificity for VSA expressed by P. falciparum isolates from three African countries. Plasma levels of VSA-specific IgG recognizing individual parasite isolates depended on the transmission intensity at the site of plasma collection but were largely independent of the geographical origin of the parasites. The total repertoire of immunologically distinct VSA thus appears to be finite and geographically conserved, most likely due to functional constraints. Furthermore, plasma samples frequently had high IgG reactivity to VSA expressed by parasites isolated more than 10 years later, showing that the repertoire is also temporally stable. Parasites from patients with severe malaria expressed VSA (VSASM) that were better recognized by plasma IgG than VSA expressed by other parasites, but importantly, VSASM-type antigens also appeared to show substantial antigenic homogeneity. Our finding that the repertoire of immunologically distinct VSA in general, and in particular that of VSASM, is geographically and temporally conserved raises hopes for the feasibility of developing VSA-based vaccines specifically designed to accelerate naturally acquired immunity, thereby enhancing protection against severe and life-threatening P. falciparum malaria.

Published
2004

18. Geographical and Temporal Conservation of Antibody Recognition of Plasmodium falciparum Variant Surface Antigens

Author

Nielsen, Morten A., primary, Vestergaard, Lasse S., additional, Lusingu, John, additional, Kurtzhals, Jørgen A. L., additional, Giha, Haider A., additional, Grevstad, Berit, additional, Goka, Bamenla Q., additional, Lemnge, Martha M., additional, Jensen, James B., additional, Akanmori, Bartholomew D., additional, Theander, Thor G., additional, Staalsoe, Trine, additional, and Hviid, Lars, additional

Published
2004
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19. Targeting intensive versus conventional glycaemic control for type 1 diabetes mellitus: a systematic review with meta-analyses and trial sequential analyses of randomised clinical trials.

Author

Kähler, Pernille, Grevstad, Berit, Almdal, Thomas, Gluud, Christian, Wetterslev, Jørn, Vaag, Allan, and Hemmingsen, Bianca

Abstract

Objective: To assess the benefits and harms of targeting intensive versus conventional glycaemic control in patients with type 1 diabetes mellitus. Design: A systematic review with meta-analyses and trial sequential analyses of randomised clinical trials. Data sources: The Cochrane Library, MEDLINE, EMBASE, Science Citation Index Expanded and LILACS to January 2013. Study selection: Randomised clinical trials that prespecified different targets of glycaemic control in participants at any age with type 1 diabetes mellitus were included. Data extraction: Two authors independently assessed studies for inclusion and extracted data. Results: 18 randomised clinical trials included 2254 participants with type 1 diabetes mellitus. All trials had high risk of bias. There was no statistically significant effect of targeting intensive glycaemic control on all-cause mortality (risk ratio 1.16, 95% CI 0.65 to 2.08) or cardiovascular mortality (0.49, 0.19 to 1.24). Targeting intensive glycaemic control reduced the relative risks for the composite macrovascular outcome (0.63, 0.41 to 0.96; p=0.03), and nephropathy (0.37, 0.27 to 0.50; p<0.00001. The effect estimates of retinopathy, ketoacidosis and retinal photocoagulation were not consistently statistically significant between random and fixed effects models. The risk of severe hypoglycaemia was significantly increased with intensive glycaemic targets (1.40, 1.01 to 1.94). Trial sequential analyses showed that the amount of data needed to demonstrate a relative risk reduction of 10% were, in general, inadequate. Conclusions: There was no significant effect towards improved all-cause mortality when targeting intensive glycaemic control compared with conventional glycaemic control. However, there may be beneficial effects of targeting intensive glycaemic control on the composite macrovascular outcome and on nephropathy, and detrimental effects on severe hypoglycaemia. Notably, the data for retinopathy and ketoacidosis were inconsistent. There was a severe lack of reporting on patient relevant outcomes, and all trials had poor bias control. [ABSTRACT FROM AUTHOR]

Published
2014
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20. Geographical and Temporal Conservation of Antibody Recognition of Plasmodium falciparumVariant Surface Antigens

Author

Nielsen, Morten A., Vestergaard, Lasse S., Lusingu, John, Kurtzhals, Jørgen A. L., Giha, Haider A., Grevstad, Berit, Goka, Bamenla Q., Lemnge, Martha M., Jensen, James B., Akanmori, Bartholomew D., Theander, Thor G., Staalsoe, Trine, and Hviid, Lars

Abstract

ABSTRACTThe slow acquisition of protection against Plasmodium falciparummalaria probably reflects the extensive diversity of important antigens. The variant surface antigens (VSA) that mediate parasite adhesion to a range of host molecules are regarded as important targets of acquired protective immunity, but their diversity makes them questionable vaccine candidates. We determined levels of VSA-specific immunoglobulin G (IgG) in human plasma collected at four geographically distant and epidemiologically distinct localities with specificity for VSA expressed by P. falciparumisolates from three African countries. Plasma levels of VSA-specific IgG recognizing individual parasite isolates depended on the transmission intensity at the site of plasma collection but were largely independent of the geographical origin of the parasites. The total repertoire of immunologically distinct VSA thus appears to be finite and geographically conserved, most likely due to functional constraints. Furthermore, plasma samples frequently had high IgG reactivity to VSA expressed by parasites isolated more than 10 years later, showing that the repertoire is also temporally stable. Parasites from patients with severe malaria expressed VSA (VSASM) that were better recognized by plasma IgG than VSA expressed by other parasites, but importantly, VSASM-type antigens also appeared to show substantial antigenic homogeneity. Our finding that the repertoire of immunologically distinct VSA in general, and in particular that of VSASM, is geographically and temporally conserved raises hopes for the feasibility of developing VSA-based vaccines specifically designed to accelerate naturally acquired immunity, thereby enhancing protection against severe and life-threatening P. falciparummalaria.

Published
2004
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21. Cerebral near infrared spectroscopy oximetry in extremely preterm infants: phase II randomised clinical trial.

Author

Hyttel-Sorensen S, Pellicer A, Alderliesten T, Austin T, van Bel F, Benders M, Claris O, Dempsey E, Franz AR, Fumagalli M, Gluud C, Grevstad B, Hagmann C, Lemmers P, van Oeveren W, Pichler G, Plomgaard AM, Riera J, Sanchez L, Winkel P, Wolf M, and Greisen G

Subjects
Cerebrovascular Circulation, Clinical Protocols, Europe, Humans, Hypoxia pathology, Infant, Extremely Premature, Infant, Newborn, Intensive Care Units, Neonatal, Practice Guidelines as Topic, Time Factors, Treatment Outcome, Brain blood supply, Guideline Adherence, Hypoxia diagnosis, Intensive Care, Neonatal, Monitoring, Physiologic methods, Oximetry methods, Spectroscopy, Near-Infrared methods
Abstract

Objective: To determine if it is possible to stabilise the cerebral oxygenation of extremely preterm infants monitored by cerebral near infrared spectroscopy (NIRS) oximetry., Design: Phase II randomised, single blinded, parallel clinical trial., Setting: Eight tertiary neonatal intensive care units in eight European countries., Participants: 166 extremely preterm infants born before 28 weeks of gestation: 86 were randomised to cerebral NIRS monitoring and 80 to blinded NIRS monitoring. The only exclusion criterion was a decision not to provide life support., Interventions: Monitoring of cerebral oxygenation using NIRS in combination with a dedicated treatment guideline during the first 72 hours of life (experimental) compared with blinded NIRS oxygenation monitoring with standard care (control)., Main Outcome Measures: The primary outcome measure was the time spent outside the target range of 55-85% for cerebral oxygenation multiplied by the mean absolute deviation, expressed in %hours (burden of hypoxia and hyperoxia). One hour with an oxygenation of 50% gives 5%hours of hypoxia. Secondary outcomes were all cause mortality at term equivalent age and a brain injury score assessed by cerebral ultrasonography., Randomisation: Allocation sequence 1:1 with block sizes 4 and 6 in random order concealed for the investigators. The allocation was stratified for gestational age (<26 weeks or ≥ 26 weeks)., Blinding: Cerebral oxygenation measurements were blinded in the control group. All outcome assessors were blinded to group allocation., Results: The 86 infants randomised to the NIRS group had a median burden of hypoxia and hyperoxia of 36.1%hours (interquartile range 9.2-79.5%hours) compared with 81.3 (38.5-181.3) %hours in the control group, a reduction of 58% (95% confidence interval 35% to 73%, P<0.001). In the experimental group the median burden of hypoxia was 16.6 (interquartile range 5.4-68.1) %hours, compared with 53.6 (17.4-171.3) %hours in the control group (P=0.0012). The median burden of hyperoxia was similar between the groups: 1.2 (interquartile range 0.3-9.6) %hours in the experimental group compared with 1.1 (0.1-23.4) %hours in the control group (P=0.98). We found no statistically significant differences between the two groups at term corrected age. No severe adverse reactions were associated with the device., Conclusions: Cerebral oxygenation was stabilised in extremely preterm infants using a dedicated treatment guideline in combination with cerebral NIRS monitoring.Trial registration ClinicalTrial.gov NCT01590316., (© Hyttel-Sorensen et al 2015.)

Published
2015
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22. Selected HIV-1 Env trimeric formulations act as potent immunogens in a rabbit vaccination model.

Author

Heyndrickx L, Stewart-Jones G, Jansson M, Schuitemaker H, Bowles E, Buonaguro L, Grevstad B, Vinner L, Vereecken K, Parker J, Ramaswamy M, Biswas P, Vanham G, Scarlatti G, and Fomsgaard A

Subjects
Animals, Antibodies, Neutralizing immunology, Chemistry, Pharmaceutical, Female, Humans, Kinetics, Male, Models, Animal, Peptide Fragments immunology, Protein Structure, Quaternary, Rabbits, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 immunology, HIV-1 immunology, Protein Multimerization, Vaccination, env Gene Products, Human Immunodeficiency Virus chemistry, env Gene Products, Human Immunodeficiency Virus immunology
Abstract

Background: Ten to 30% of HIV-1 infected subjects develop broadly neutralizing antibodies (bNAbs) during chronic infection. We hypothesized that immunizing rabbits with viral envelope glycoproteins (Envs) from these patients may induce bNAbs, when formulated as a trimeric protein and in the presence of an adjuvant., Methods: Based on in vitro neutralizing activity in serum, patients with bNAbs were selected for cloning of their HIV-1 Env. Seven stable soluble trimeric gp140 proteins were generated from sequences derived from four adults and two children infected with either clade A or B HIV-1. From one of the clade A Envs both the monomeric and trimeric Env were produced for comparison. Rabbits were immunized with soluble gp120 or trimeric gp140 proteins in combination with the adjuvant dimethyl dioctadecyl ammonium/trehalose dibehenate (CAF01). Env binding in rabbit immune serum was determined using ELISAs based on gp120-IIIB protein. Neutralizing activity of IgG purified from rabbit immune sera was measured with the pseudovirus-TZMbl assay and a PBMC-based neutralization assay for selected experiments., Results: It was initially established that gp140 trimers induce better antibody responses over gp120 monomers and that the adjuvant CAF01 was necessary for such strong responses. Gp140 trimers, based on HIV-1 variants from patients with bNAbs, were able to elicit both gp120IIIB specific IgG and NAbs to Tier 1 viruses of different subtypes. Potency of NAbs closely correlated with titers, and an gp120-binding IgG titer above a threshold of 100,000 was predictive of neutralization capability. Finally, peptide inhibition experiments showed that a large fraction of the neutralizing IgG was directed against the gp120 V3 region., Conclusions: Our results indicate that the strategy of reverse immunology based on selected Env sequences is promising when immunogens are delivered as stabilized trimers in CAF01 adjuvant and that the rabbit is a valuable model for HIV vaccine studies.

Published
2013
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23. Characterization of humoral responses to soluble trimeric HIV gp140 from a clade A Ugandan field isolate.

Author

Visciano ML, Tagliamonte M, Stewart-Jones G, Heyndrickx L, Vanham G, Jansson M, Fomsgaard A, Grevstad B, Ramaswamy M, Buonaguro FM, Tornesello ML, Biswas P, Scarlatti G, and Buonaguro L

Subjects
Animals, Antibodies, Neutralizing immunology, Antibodies, Viral immunology, Enzyme-Linked Immunosorbent Assay, Epitopes, B-Lymphocyte immunology, Female, HEK293 Cells, HIV Infections virology, HIV-1 classification, Humans, Immunization, Neutralization Tests, Rabbits, Recombinant Proteins immunology, Uganda, HIV Infections immunology, Immunity, Humoral, env Gene Products, Human Immunodeficiency Virus immunology
Abstract

Trimeric soluble forms of HIV gp140 envelope glycoproteins represent one of the closest molecular structures compared to native spikes present on intact virus particles. Trimeric soluble gp140 have been generated by several groups and such molecules have been shown to induce antibodies with neutralizing activity against homologous and heterologous viruses. In the present study, we generated a recombinant trimeric soluble gp140, derived from a previously identified Ugandan A-clade HIV field isolate (gp14094UG018). Antibodies elicited in immunized rabbits show a broad binding pattern to HIV envelopes of different clades. An epitope mapping analysis reveals that, on average, the binding is mostly focused on the C1, C2, V3, V5 and C5 regions. Immune sera show neutralization activity to Tier 1 isolates of different clades, demonstrating cross clade neutralizing activity which needs to be further broadened by possible structural modifications of the clade A gp14094UG018. Our results provide a rationale for the design and evaluation of immunogens and the clade A gp14094UG018 shows promising characteristics for potential involvement in an effective HIV vaccine with broad activity.

Published
2013
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