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151. Ytring

Author

Torleiv Ole Rognum

Subjects
Complementary and alternative medicine, Pharmaceutical Science, Pharmacology (medical)
Published
2007

152. A mitochondrial DNA polymorphism associated with cardiac arrhythmia investigated in sudden infant death syndrome

Author

Siri H. Opdal, Torleiv O. Rognum, Åshild Vege, and Marianne Arnestad

Subjects
Male, ERG1 Potassium Channel, medicine.medical_specialty, Mitochondrial disease, Long QT syndrome, Physiology, DNA, Mitochondrial, Polymerase Chain Reaction, Sudden death, Mitochondrial myopathy, Internal medicine, Genotype, Humans, Medicine, Cause of death, Polymorphism, Genetic, business.industry, Infant, Newborn, Infant, NADH Dehydrogenase, General Medicine, Sudden infant death syndrome, medicine.disease, Ether-A-Go-Go Potassium Channels, Long QT Syndrome, Endocrinology, Case-Control Studies, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, Female, Restriction fragment length polymorphism, business, Sudden Infant Death
Abstract

Aim: Long QT syndrome (LQTS) has been shown to be the cause of death in some cases originally diagnosed as sudden infant death syndrome (SIDS). Such cardiac arrhythmias have also been noted in families with mitochondrial disease, and studies indicate that mitochondrial disease could be involved in SIDS. This makes the mtDNA polymorphism T3394C interesting, as a previous study has shown it to be associated with electrocardiographic (ECG) changes after exercise in a family with LQTS, where some members harboured a KCNH2 mutation. Subjects: A total of 245 SIDS cases and 176 control cases. Methods: DNA was prepared from blood/tissue samples. Polymerase chain reaction (PCR) and restriction fragment length polymorphism (RFLP) were performed to search for the mtDNA polymorphism and KCNH2 mutation. Differences were confirmed by sequencing. Results: The T3394C polymorphism was found in 3 pure SIDS cases (1.5%), 2 borderline SIDS cases (4.4%), 1 case of explained death (1.6%) and 2 living control cases (1.8%) (p = 0.62). The KCNH2 mutation was not found in cases or controls. Conclusion: The mtDNA polymorphism studied was found in a small number of SIDS cases and the frequency did not differ statistically from control subjects, making an association with increased SIDS risk unlikely.

Published
2007

153. Are substitutions in the first hypervariable region of the mitochondrial DNA displacement-loop in sudden infant death syndrome due to maternal inheritance?

Author

Musse Ahmed Musse, Åshild Vege, Torleiv O. Rognum, Siri H. Opdal, and Marianne Arnestad

Subjects
Genetics, Mitochondrial DNA, Non-Mendelian inheritance, D-loop, Pediatrics, Perinatology and Child Health, Haplotype, General Medicine, Biology, Sudden infant death syndrome, Sudden death, Hypervariable region, Sequence (medicine)
Abstract

Arnestad M, Opdal SH, Musse MA, Vege AE , Rognum TO. Are substitutions in the e rst hypervariable region of the mitochondrial DNA displacement-loop in sudden infant death syndrome due to maternal inheritance? Acta Paediatr 2002; 91: 1060‐1064. Stockholm. ISSN 0803-5253 Aim: To investigate whether all substitutions in the e rst hypervariable region (HVR1) in sudden infant death syndrome (SIDS) can be recovered along the maternal line of the family (inherited), or whether SIDS victims have new substitutions compared to maternal relatives (somatic mutations) that may be related to environmental factors. Methods: Seventy-one SIDS/mother pairs, including 11 families with SIDS, mother and mother’s relatives and/or SIDS siblings, were studied. The HVR1 sequence was recorded in the base-pair range 16056‐16400. The recorded HVR1 sequence was compared with the Cambridge sequence, and differences were recorded as substitutions. The substitution pattern in the SIDS victims was compared with the pattern found in family members along the maternal line. Results: All the substitutions found in SIDS victims could be traced in the maternal line of the family; in 5 cases this was observed through three generations, and in 3 cases through four generations. Discussion: In patients with known mitochondrial (mt) DNA disease, a large number of sequence variants have been found in the Dloop region. Substitutions in the D-loop may be part of a haplotype with mutations elsewhere in the mtDNA.

Published
2007

154. Increased number of substitutions in the D-loop of mitochondrial DNA in the sudden infant death syndrome

Author

A. K. Stave, Åshild Vege, T Egeland, BM Dupuy, Torleiv O. Rognum, and Siri H. Opdal

Subjects
Genetics, Mitochondrial DNA, Nucleic acid sequence, General Medicine, Sudden infant death syndrome, Mitochondrion, Biology, Sudden death, symbols.namesake, D-loop, Pediatrics, Perinatology and Child Health, DNA Mutational Analysis, Mendelian inheritance, symbols
Abstract

The purpose of the present study was to investigate substitutions in the D-loop of mitochondrial DNA (mtDNA) in sudden infant death syndrome (SIDS) and controls, since several observations indicate the involvement of mtDNA mutations in SIDS. These include elevated levels of vitreous humour hypoxanthine in SIDS victims, familial clustering without mendelian traits, and observations of increased sleepiness and a lower activity score in infants who later succumbed to SIDS. Eighty-two cases of SIDS and 133 controls were investigated and the D-loop sequences were recorded in the base-pair range 16055-16500 in the mtDNA sequence. The sequencing was carried out using the Applied Biosystems Sequenase dye terminator method and a ABD373A sequencer. The recorded D-loop sequences were compared with the Cambridge sequence and differences were recorded as substitutions. The SIDS cases had a tendency towards a higher substitution rate in the D-loop than the controls (p = 0.088). This observation makes it interesting to search for deleterious mutations in other locations in the mtDNA.

Published
2007

155. Sudden infant death syndrome (SIDS)—Standardised investigations and classification: Recommendations

Author

Charlotte de Lange, Reinhard Dettmeyer, Martin Schlaud, Åshild Vege, Henry F. Krous, Siri H. Opdal, C. V. Isaksen, Liliana Bachs, Marianne Arnestad, Peter Gaustad, Jens V. Jorgensen, Thomas Bajanowski, Jørg Mørland, Arne Stray-Pedersen, Peter J. Fleming, Ellen Holter, Peter S Blair, Markil Gregersen, Lisbeth Sveum, Peter Sidebotham, Torleiv O. Rognum, Roger W. Byard, Kari Skullerud, Arne Borthne, Jytte Banner, Petra Råsten-Almqvist, Gisela Stoltenburg-Didinger, Isabella Moore, Jens Grøgaard, and Burkhard Madea

Subjects
Central Nervous System, Research design, medicine.medical_specialty, Pediatrics, Endogenous Factors, Respiratory System, MEDLINE, Sudden death, Pathology and Forensic Medicine, Virology, medicine, Humans, Intensive care medicine, Bacteriological Techniques, business.industry, Myocardium, Forensic Sciences, Medical jurisprudence, International comparisons, Infant, Sudden infant death syndrome, Immunohistochemistry, Infant mortality, Research Design, business, Law, Sudden Infant Death
Abstract

Sudden infant death syndrome (SIDS) still accounts for considerable numbers of unexpected infant deaths in many countries. While numerous theories have been advanced to explain these events, it is increasingly clear that this group of infant deaths results from the complex interaction of a variety of heritable and idiosyncratic endogenous factors interacting with exogenous factors. This has been elegantly summarised in the "three hit" or "triple risk" model. Contradictions and lack of consistencies in the literature have arisen from diverse autopsy approaches, variable applications of diagnostic criteria and inconsistent use of definitions. An approach to sudden infant death is outlined with discussion of appropriate tissue sampling, ancillary investigations and the use of controls in research projects. Standardisation of infant death investigations with the application of uniform definitions and protocols will ensure optimal investigation of individual cases and enable international comparisons of trends.

Published
2007

156. Regulator of Chromosome Condensation 2 Identifies High-Risk Patients within Both Major Phenotypes of Colorectal Cancer

Author

Matthias Kolberg, Knut Liestøl, Terje Johansen, Edward Leithe, Ellen C. Røyrvik, Xiao-Feng Sun, Jarle Bruun, Torleiv O. Rognum, Marianne A. Merok, Geir Bjørkøy, Ragnhild A. Lothe, Torfinn Nome, Terje Cruickshank Ahlquist, Guro Elisabeth Lind, Arild Nesbakken, Annika Lindblom, Aud Svindland, and Rolf Inge Skotheim

Subjects
Oncology, Male, Cancer Research, medicine.medical_specialty, Colorectal cancer, Chromosomal Proteins, Non-Histone, Population, DNA Mutational Analysis, Biology, medicine.disease_cause, Bioinformatics, Chromosomes, Disease-Free Survival, Internal medicine, Cell Line, Tumor, medicine, Biomarkers, Tumor, Guanine Nucleotide Exchange Factors, Humans, education, Aged, Neoplasm Staging, Aged, 80 and over, education.field_of_study, Mutation, Massive parallel sequencing, Age Factors, Klinisk medicin, Cancer, Microsatellite instability, Middle Aged, medicine.disease, Prognosis, digestive system diseases, Biomarker (medicine), Immunohistochemistry, Female, Microsatellite Instability, Clinical Medicine, Colorectal Neoplasms
Abstract

Purpose: Colorectal cancer has high incidence and mortality worldwide. Patients with microsatellite instable (MSI) tumors have significantly better prognosis than patients with microsatellite stable (MSS) tumors. Considerable variation in disease outcome remains a challenge within each subgroup, and our purpose was to identify biomarkers that improve prediction of colorectal cancer prognosis. Experimental Design: Mutation analyses of 42 MSI target genes were performed in two independent MSI tumor series (n = 209). Markers that were significantly associated with prognosis in the test series were assessed in the validation series, followed by functional and genetic explorations. The clinical potential was further investigated by immunohistochemistry in a population-based colorectal cancer series (n = 903). Results: We identified the cell-cycle gene regulator of chromosome condensation 2 (RCC2) as a cancer biomarker. We found a mutation in the 5′ UTR region of RCC2 that in univariate and multivariate analyses was significantly associated with improved outcome in the MSI group. This mutation caused reduction of protein expression in dual luciferase gene reporter assays. siRNA knockdown in MSI colon cancer cells (HCT15) caused reduced cell proliferation, cell-cycle arrest, and increased apoptosis. Massive parallel sequencing revealed few RCC2 mutations in MSS tumors. However, weak RCC2 protein expression was significantly associated with poor prognosis, independent of clinical high-risk parameters, and stratifies clinically important patient subgroups with MSS tumors, including elderly patients (>75 years), stage II patients, and those with rectal cancer. Conclusions: Impaired RCC2 affects functional and clinical endpoints of colorectal cancer. High-risk patients with either MSI or MSS tumors can be identified with cost-effective routine RCC2 assays. Clin Cancer Res; 21(16); 3759–70. ©2015 AACR.

Published
2015

158. Polymorphisms in the myeloid differentiation primary response 88 pathway do not explain low expression levels in sudden infant death syndrome.

Author

Bjørnvall, Christina Dybdrodt, Opdal, Siri H., Rognum, Torleiv O., and Ferrante, Linda

Subjects
SUDDEN infant death syndrome, INFANT death, FORENSIC sciences, TOLL-like receptors
Abstract

Aim: The aim of this study was to investigate if a range of known rare and common genetic variants in the Toll-like receptor 4 (TLR4)/myeloid differentiation primary response 88 (MyD88) pathway were present or overrepresented in sudden infant death syndrome (SIDS) compared to controls.Methods: Genetic variations in the genes encoding TLR4, MyD88 and Interleukin-1 receptor-associated kinase 4 were analysed. The subjects investigated included 158 SIDS cases with a median age of 15.25 weeks (2-47 weeks), 80 cases of infectious death with a median age of 24.9 weeks (0-285 weeks) and 199 adult controls with a median age of 50 years (11-86 years). The cases were collected in the years 1988-2017, and the autopsies were performed at the Department of Forensic Sciences at Oslo University Hospital, Oslo, Norway.Results: The results showed that none of the genetic variants selected from the MyD88 pathway were associated with neither SIDS nor infectious death. Most of the rare genetic variants were homozygote for the common allele in all groups, while the rest revealed allelic variation.Conclusion: The genetic variations investigated in this study did not appear to be involved in the pathogenesis of SIDS. [ABSTRACT FROM AUTHOR]

Published
2019
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159. The Sudden Infant Death Syndrome Gene: Does It Exist?

Author

Siri H. Opdal and Torleiv Ole Rognum

Subjects
Pathology, medicine.medical_specialty, Bioinformatics, medicine.disease_cause, Acyl-CoA Dehydrogenase, Lipid Metabolism, Inborn Errors, Genotype, Humans, Medicine, Genetic Predisposition to Disease, Allele, Serotonin transporter, Cause of death, Complement component 4, Mutation, Polymorphism, Genetic, biology, business.industry, Genetic disorder, Infant, Sudden infant death syndrome, medicine.disease, Long QT Syndrome, Pediatrics, Perinatology and Child Health, biology.protein, business, Sudden Infant Death
Abstract

Background. Sudden infant death syndrome (SIDS) is in a difficult position between the legal and medical systems. In the United Kingdom, prosecutors have for years applied the simple rule that 1 unexpected death in a family is a tragedy, 2 are suspicious, and 3 are murder. However, it seems that the pendulum has now swung to the opposite extreme; mutations or polymorphisms with unclear biological significance are accepted in court as possible causes of death. This development makes research on genetic predisposing factors for SIDS increasingly important, from the standpoint of the legal protection of infants. The genetic component of sudden infant death can be divided into 2 categories, ie (1) mutations that give rise to genetic disorders that constitute the cause of death by themselves and (2) polymorphisms that might predispose infants to death in critical situations. Distinguishing between these 2 categories is essential, and cases in which a mutation causing a lethal genetic disorder is identified should be diagnosed not as SIDS but as explained death.Genetic Alterations That May Cause Sudden Infant Death. Deficiencies in fatty acid metabolism have been extensively studied in cases of SIDS, and by far the most well-investigated mutation is the A985G mutation in the medium-chain acyl-CoA dehydrogenase (MCAD) gene, which is the most prevalent mutation causing MCAD deficiency. However, Gene Polymorphisms That May Predispose Infants to Sudden Infant Death Under Certain Circumstances. Many SIDS victims have an activated immune system, which may indicate that they are vulnerable to simple infections. One reason for such vulnerability may be partial deletions of the complement component 4 gene. In cases of SIDS, an association between slight infections before death and partial deletions of the complement component 4 gene has been identified, which may indicate that this combination represents increased risk of sudden infant death. There have been a few studies investigating HLA-DR genotypes and SIDS, but no association has been demonstrated. The most common polymorphisms in the interleukin-10 (IL-10) gene promoter have been investigated in SIDS cases, and the ATA/ATA genotype has been reported to be associated with both SIDS and infectious death. The findings may indicate that, in a given situation, an infant with an unfavorable IL-10 genotype may exhibit aberrant IL-10 production, and they confirm the assumption that genes involved in the immune system are of importance with respect to sudden unexpected infant death. Another gene that has been investigated is the serotonin transporter gene, and an association between the long alleles of this gene and SIDS has been demonstrated. Serotonin influences a broad range of physiologic systems, as well as the interactions between the immune and nervous systems, and findings of decreased serotonergic binding in parts of the brainstem, together with the findings in the serotonin transporter gene, may indicate that serotonin plays a regulatory role in SIDS. It has also been speculated that inadequate thermal regulation is involved in SIDS, but investigations of genes encoding heat-shock proteins and genes encoding proteins involved in lipolysis from brown adipose tissue have not found evidence of linkages between common polymorphisms in these genes and SIDS. A number of human diseases are attributable to mutations in mitochondrial DNA (mtDNA), and there are several reasons to think that mtDNA mutations also are involved in SIDS. Both a higher substitution frequency and a different substitution pattern in the HVR-I region of mtDNA have been reported in SIDS cases, compared with control cases. A number of coding region mtDNA mutations have also been reported, but many are found only in 1 or a few SIDS cases, and, to date, no predominant mtDNA mutation has been found to be associated with SIDS.Conclusions. All mutations giving rise to metabolic disorders known to be associated with life-threatening events are possible candidates for genes involved in cases of sudden infant death, either as a cause of death or as a predisposing factor. It is necessary to distinguish between lethal mutations leading to diseases such as MCAD and LQTS, and polymorphisms (for instance, in the IL-10 gene and mtDNA) that are normal gene variants but might be suboptimal in critical situations and thus predispose infants to sudden infant death. It is unlikely that one mutation or polymorphism is the predisposing factor in all SIDS cases. However, it is likely that there are “SIDS genes” operating as a polygenic inheritance predisposing infants to sudden infant death, in combination with environmental risk factors. For genetically predisposed infants, a combination of, for instance, a slight infection, a prone sleeping position, and a warm environment may trigger a vicious circle with a death mechanism, including hyperthermia, irregular breathing, hypoxemia, and defective autoresuscitation, eventually leading to severe hypoxia, coma, and death.

Published
2004

160. Cardiac potassium channel dysfunction in sudden infant death syndrome

Author

Rhodes, T, Abraham, R, Welch, R, Vanoye, C, Crotti, L, Arnestad, M, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Rognum, T, Roden, D, Schwartz, P, George AL, J, Rhodes TE, Abraham RL, Welch RC, Vanoye CG, Crotti L, Arnestad M, Insolia R, Pedrazzini M, Ferrandi C, Vege A, Rognum T, Roden DM, Schwartz PJ, George AL Jr, Rhodes, T, Abraham, R, Welch, R, Vanoye, C, Crotti, L, Arnestad, M, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Rognum, T, Roden, D, Schwartz, P, George AL, J, Rhodes TE, Abraham RL, Welch RC, Vanoye CG, Crotti L, Arnestad M, Insolia R, Pedrazzini M, Ferrandi C, Vege A, Rognum T, Roden DM, Schwartz PJ, and George AL Jr

Abstract

Life-threatening arrhythmias have been suspected as one cause of the sudden infant death syndrome (SIDS), and this hypothesis is supported by the observation that mutations in arrhythmia susceptibility genes occur in 5-10% of cases. However, the functional consequences of cardiac potassium channel gene mutations associated with SIDS and how these alleles might mechanistically predispose to sudden death are unknown. To address these questions, we studied four missense KCNH2 (encoding HERG) variants, one compound KCNH2 genotype, and a missense KCNQ1 mutation all previously identified in Norwegian SIDS cases. Three of the six variants exhibited functional impairments while three were biophysically similar to wild-type channels (KCNH2 variants V279M, R885C, and S1040G). When co-expressed with WT-HERG, R273Q and K897T/R954C generated currents resembling the rapid component of the cardiac delayed rectifier current (I(Kr)) but with significantly diminished amplitude. Action potential modeling demonstrated that this level of functional impairment was sufficient to evoke increased action potential duration and pause-dependent early afterdepolarizations. By contrast, KCNQ1-I274V causes a gain-of-function in I(Ks) characterized by increased current density, faster activation, and slower deactivation leading to accumulation of instantaneous current upon repeated stimulation. Action potential simulations using a Markov model of heterozygous I274V-I(Ks) incorporated into the Luo-Rudy (LRd) ventricular cell model demonstrated marked rate-dependent shortening of action potential duration predicting a short QT phenotype. Our results indicate that certain potassium channel mutations associated with SIDS confer overt functional defects consistent with either LQTS or SQTS, and further emphasize the role of congenital arrhythmia susceptibility in this syndrome

Published
2008

161. Sudden infant death syndrome, infection and inflammatory responses

Author

Åshild Vege and Torleiv Ole Rognum

Subjects
Inflammation, Microbiology (medical), Immune Stimulation, Interleukin-6, business.industry, Mechanism (biology), Inflammatory response, Immunology, Infant, Newborn, Infant, Autopsy, General Medicine, Sudden infant death syndrome, Infections, Microbiology, Unexpected death, Sudden death, Virtuous circle and vicious circle, Infectious Diseases, Humans, Immunology and Allergy, Medicine, business, Sudden Infant Death
Abstract

Sudden infant death syndrome (SIDS) is sudden unexpected death in infancy for which there is no explanation after review of the history, a death scene investigation and a thorough autopsy. The use of common diagnostic criteria is a prerequisite for discussing the importance of infection, inflammatory responses and trigger mechanism in SIDS. Several observations of immune stimulation in the periphery and of interleukin-6 elevation in the cerebrospinal fluid of SIDS victims explain how infections can play a role in precipitating these deaths. Finally, these findings and important risk factors for SIDS are integrated in the concept of a vicious circle for understanding the death mechanism. The vicious circle is a concept to elucidate the interactions between unfavourable factors, including deficient auto-resuscitation, and how this could result in death.

Published
2004

162. Sudden Infant Death Syndrome and Unclassified Sudden Infant Deaths: A Definitional and Diagnostic Approach

Author

Roger W. Byard, Edwin A. Mitchell, Randy Hanzlick, J. Bruce Beckwith, Thomas G. Keens, Tracey S. Corey, Torleiv O. Rognum, Ernest Cutz, Thomas Bajanowski, and Henry F. Krous

Subjects
Nosology, Pediatrics, medicine.medical_specialty, business.industry, Pediatrics, Perinatology and Child Health, medicine, Sudden infant death syndrome, Medical diagnosis, business, Sudden death, Infant mortality, Sudden infant death, Ancillary test
Abstract

The definition of sudden infant death syndrome (SIDS) originally appeared in 1969 and was modified 2 decades later. During the following 15 years, an enormous amount of additional information has emerged, justifying additional refinement of the definition of SIDS to incorporate epidemiologic features, risk factors, pathologic features, and ancillary test findings. An expert panel of pediatric and forensic pathologists and pediatricians considered these issues and developed a new general definition of SIDS for administrative and vital statistics purposes. The new definition was then stratified to facilitate research into sudden infant death. Another category, defined as unclassified sudden infant deaths, was introduced for cases that do not meet the criteria for a diagnosis of SIDS and for which alternative diagnoses of natural or unnatural conditions were equivocal. It is anticipated that these new definitions will be modified in the future to accommodate new understanding of SIDS and sudden infant death.

Published
2004

163. Cardiac sodium channel dysfunction in sudden infant death syndrome

Author

Wang, D, Desai, R, Crotti, L, Arnestad, M, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Rognum, T, Schwartz, P, George AL, J, Wang DW, Desai RR, Crotti L, Arnestad M, Insolia R, Pedrazzini M, Ferrandi C, Vege A, Rognum T, Schwartz PJ, George AL Jr, Wang, D, Desai, R, Crotti, L, Arnestad, M, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Rognum, T, Schwartz, P, George AL, J, Wang DW, Desai RR, Crotti L, Arnestad M, Insolia R, Pedrazzini M, Ferrandi C, Vege A, Rognum T, Schwartz PJ, and George AL Jr

Abstract

BACKGROUND: Mutations in genes responsible for the congenital long-QT syndrome, especially SCN5A, have been identified in some cases of sudden infant death syndrome. In a large-scale collaborative genetic screen, several SCN5A variants were identified in a Norwegian sudden infant death syndrome cohort (n=201). We present functional characterization of 7 missense variants (S216L, R680H, T1304M, F1486L, V1951L, F2004L, and P2006A) and 1 in-frame deletion allele (delAL586-587) identified by these efforts. METHODS AND RESULTS: Whole-cell sodium currents were measured in tsA201 cells transiently transfected with recombinant wild-type or mutant SCN5A cDNA (hH1) coexpressed with the human beta1 subunit. All variants exhibited defects in the kinetics and voltage dependence of inactivation. Five variants (S216L, T1304M, F1486L, F2004L, and P2006A) exhibited significantly increased persistent sodium currents (range, 0.5% to 1.7% of peak current) typical of SCN5A mutations associated with long-QT syndrome. These same 5 variants also displayed significant depolarizing shifts in voltage dependence of inactivation (range, 5 to 14 mV) and faster recovery from inactivation, but F1486L uniquely exhibits a depolarizing shift in the conductance-voltage relationship. Three alleles (delAL586-587, R680H, and V1951L) exhibited increased persistent current only under conditions of internal acidosis (R680H) or when expressed in the context of a common splice variant (delQ1077), indicating that they have a latent dysfunctional phenotype. CONCLUSIONS: Our present results greatly expand the spectrum of functionally characterized SCN5A variants associated with sudden infant death syndrome and provide further biophysical correlates of arrhythmia susceptibility in this syndrome.

Published
2007

164. Prevalence of long-QT syndrome gene variants in sudden infant death syndrome

Author

Arnestad, M, Crotti, L, Rognum, T, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Wang, D, Rhodes, T, George, A, Schwartz, P, Rognum, TO, Wang, DW, Rhodes, TE, George, A Jr, Schwartz, PJ, Arnestad, M, Crotti, L, Rognum, T, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Wang, D, Rhodes, T, George, A, Schwartz, P, Rognum, TO, Wang, DW, Rhodes, TE, George, A Jr, and Schwartz, PJ

Abstract

BACKGROUND: The hypothesis that some cases of sudden infant death syndrome (SIDS) could be caused by long-QT syndrome (LQTS) has been supported by molecular studies. However, there are inadequate data regarding the true prevalence of mutations in arrhythmia-susceptibility genes among SIDS cases. Given the importance and potential implications of these observations, we performed a study to more accurately quantify the contribution to SIDS of LQTS gene mutations and rare variants. METHODS AND RESULTS: Molecular screening of 7 genes (KCNQ1, KCNH2, SCN5A, KCNE1, KCNE2, KCNJ2, CAV3) associated with LQTS was performed with denaturing high-performance liquid chromatography and nucleotide sequencing of genomic DNA from 201 cases diagnosed as SIDS according to the Nordic Criteria, and from 182 infant and adult controls. All SIDS and control cases originated from the same regions in Norway. Genetic analysis was blinded to diagnosis. Mutations and rare variants were found in 26 of 201 cases (12.9%). On the basis of their functional effect, however, we considered 8 mutations and 7 rare variants found in 19 of 201 cases as likely contributors to sudden death (9.5%; 95% CI, 5.8 to 14.4%). CONCLUSIONS: We demonstrated that 9.5% of cases diagnosed as SIDS carry functionally significant genetic variants in LQTS genes. The present study demonstrates that sudden arrhythmic death is an important contributor to SIDS. As these variants likely modify ventricular repolarization and QT interval duration, our results support the debated concept that an ECG would probably identify most infants at risk for sudden death due to LQTS either in infancy or later on in life

Published
2007

165. Il-10 gene polymorphisms are associated with infectious cause of sudden infant death

Author

Torleiv O. Rognum, Åshild Vege, Anette Opstad, and Siri H. Opdal

Subjects
Male, Genotype, medicine.medical_treatment, Immunology, Single-nucleotide polymorphism, Biology, Infections, Polymorphism, Single Nucleotide, Immune system, medicine, Humans, Immunology and Allergy, Promoter Regions, Genetic, Haplotype, Infant, General Medicine, Sudden infant death syndrome, Interleukin-10, Interleukin 10, Cytokine, Haplotypes, Infectious disease (medical specialty), Cytokines, Female, Sudden Infant Death, Microsatellite Repeats
Abstract

Cytokines are involved in regulating the intensity and duration of the immune response, and cytokine production is carefully regulated. With regard to sudden infant death, interleukin-10 (IL-10) is of special interest. This is an immunoregulatory cytokine that plays an important role in the development of infectious disease. The purpose of this study was to elucidate the relationship between polymorphisms in the promoter region of the IL-10 gene and sudden infant death due to either sudden infant death syndrome (SIDS) or infection. The polymorphisms investigated include the SNPs in base pairs (bp) -1082, -819, -592, and the two microsatellites IL-10G and IL-10R. The main finding is an association between the ATA haplotype and the ATA/ATA genotype and infectious death. The group of infectious deaths also had a higher percentage of the genotypes G21/G22 and G21/G23, compared with the SIDS patients. In addition, G21/G22 was found in a higher percentage of the SIDS patients than in the controls. These findings lead us to speculate that, in some situations, an infant with an unfavorable IL-10 genotype may exhibit aberrant IL-10 production, which in turn leads to an imbalance in the immune response and renders the infant unable to cope with the infection.

Published
2003

166. Genetic Tumor Markers With Prognostic Impact in Dukes’ Stages B and C Colorectal Cancer Patients

Author

Torleiv O. Rognum, L. Thorstensen, Gunn Iren Meling, Ragnhild A. Lothe, Chieu B. Diep, and Eva Skovlund

Subjects
Adult, Genetic Markers, Male, Oncology, Cancer Research, medicine.medical_specialty, Pathology, Tumor suppressor gene, Colorectal cancer, Chromosomes, Human, Pair 20, Loss of Heterozygosity, Loss of heterozygosity, Risk Factors, Internal medicine, Biomarkers, Tumor, medicine, Humans, Clinical significance, Prospective Studies, Allele, Survival rate, Alleles, Aged, Neoplasm Staging, Aged, 80 and over, Chromosomes, Human, Pair 14, business.industry, Cytogenetics, Microsatellite instability, DNA, Neoplasm, Middle Aged, Prognosis, medicine.disease, Survival Rate, Chromosomes, Human, Pair 1, Mutation, Female, Tumor Suppressor Protein p53, Chromosomes, Human, Pair 18, Colorectal Neoplasms, business, Chromosomes, Human, Pair 17, Microsatellite Repeats
Abstract

Purpose: To examine several genetic changes in primary colorectal carcinomas (CRCs) from patients with 10 years of follow-up and associate the findings with clinicopathologic variables. Material and Methods: DNA from 220 CRCs were analyzed for allelic imbalances at 12 loci on chromosome arms 1p, 14q, 17p, 18q, and 20q, and the microsatellite instability (MSI) status was determined. The clinical significance of the tumor protein 53 (TP53) mutations was re-evaluated. Results: Patients with tumors containing 17p or 18q deletions had shorter survival than those without these alterations (P = .021, P = .008, respectively). This was also significant for the Dukes’ B group (P = .025, P = .010, respectively). Furthermore, patients with tumors showing losses of both chromosome arms revealed an even poorer disease outcome than those with either 17p or 18q loss. Patients with low increase in 20q copy number in their tumors had longer survival compared with those without changes (P = .009) or those with a high increase of copy number (P = .037). This was also evident for the Dukes’ C group (P = .018, P = .030, respectively). MSI was seemingly a beneficial marker for survival (P = .071). A significant association between mutations affecting the L3 zinc-binding domain of TP53 and survival was confirmed in this cohort after 10 years of follow-up, and also was found to apply for patients in the Dukes’ B group. Several associations were found among genetic and pathologic data. Conclusion: The present study indicates that 17p, 18q, and 20q genotypes, and TP53 mutation status add information in the subclassification of Dukes’ B and C patients and may have impact on the choice of treatment.

Published
2003

167. Strong HLA-DR expression in microsatellite stable carcinomas of the large bowel is associated with good prognosis

Author

Solveig Norheim Andersen, L. Thorstensen, Gunn Iren Meling, Ragnhild A. Lothe, Tone Løvig, Chieu B. Diep, and Torleiv O. Rognum

Subjects
Male, Cancer Research, Pathology, medicine.medical_specialty, Colorectal cancer, Biology, survival, Antigen, Chromosome instability, HLA-DR, medicine, Humans, Survival analysis, Aged, Neoplasm Staging, Proportional Hazards Models, Sex Characteristics, Proportional hazards model, Age Factors, Molecular and Cellular Pathology, Microsatellite instability, HLA-DR Antigens, Middle Aged, colorectal neoplasms, Prognosis, medicine.disease, Immunohistochemistry, Survival Analysis, Gene Expression Regulation, Neoplastic, Oncology, Colonic Neoplasms, Cancer research, Female, microsatellite instability, Disease Susceptibility, Microsatellite Repeats
Abstract

Progression of colorectal cancer may follow either of two main genetic routes: the chromosome- or microsatellite-instability pathways. Association between the patients' prognosis and microsatellite instability has been questioned. Improved survival has previously been found in patients with expression of HLA-DR antigens on their tumour cells. In this study, the expression of HLA-DR antigen was investigated by immunohistochemistry in 357 large bowel carcinomas stratified by microsatellite instability status. Sixteen per cent of the tumours showed strong HLA-DR expression and 35% had weak DR expression. We confirmed that patients with strong positive HLA-DR staining had improved survival (P

Published
2002

168. Evaluation of diagnostic tools applied in the examination of sudden unexpected deaths in infancy and early childhood

Author

Marianne Arnestad, Åshild Vege, and Torleiv O. Rognum

Subjects
medicine.medical_specialty, Pediatrics, Norway, business.industry, Medical jurisprudence, Infant, Newborn, Infant, Autopsy, Neuropathology, Forensic Medicine, Sudden death, Infant mortality, Pathology and Forensic Medicine, Age Distribution, Homicide, Cause of Death, Child, Preschool, medicine, Humans, Medical history, business, Law, Sudden Infant Death, Cause of death
Abstract

During the period between 1984 and 1999, 309 cases of sudden unexpected death in infancy and early childhood (0–3 years) were investigated at the Institute of Forensic Medicine in Oslo. In 73 cases, an explainable cause of death was found. In this non-sudden infant death syndrome (SIDS) group, 42 cases were due to disease, 14 to accidents, 7 to neglect/abuse and 10 cases were due to homicide. In 43 cases, there were pathological findings at the autopsy or suspect features in the history and/or circumstances, which were, however, insufficient to explain death (“borderline” SIDS). In the remaining 193 cases, nothing of significance was detected (“pure” SIDS). The purpose of the present study was to evaluate the importance of the different diagnostic tools used in diagnosing non-SIDS and borderline SIDS cases. The definition of SIDS requires a negative history as well as a negative autopsy result. Thus, the following variables were analysed: circumstances, medical history and autopsy, which included a gross pathological investigation, histology, neuropathology, microbiology, radiology and toxicology. In diagnosing deaths due to disease, histology, neuropathology and microbiology were the most important diagnostic tools. In contrast, information about the circumstances of death and the gross pathological findings at autopsy most often revealed the cause of death in accidents and cases of neglect/abuse and homicide. Following the drop in SIDS rate in Norway after 1989, the share of pure SIDS in proportion to the total population of sudden unexpected deaths in infancy and early childhood has decreased. The increasing proportion of non-SIDS and borderline SIDS cases presents a challenge to improve the quality of the investigation in cases of sudden death in infancy and early childhood.

Published
2002

169. APC and CTNNB1 Mutations in a Large Series of Sporadic Colorectal Carcinomas Stratified by the Microsatellite Instability Status

Author

Ragnhild A. Lothe, Chieu B. Diep, S. Norheim Andersen, Gunn Iren Meling, L. Thorstensen, Torleiv O. Rognum, and Tone Løvig

Subjects
Adult, Male, Beta-catenin, Adenomatous polyposis coli, Adenomatous Polyposis Coli Protein, DNA Mutational Analysis, Biology, Frameshift mutation, Exon, Proto-Oncogene Proteins, Carcinoma, medicine, Humans, Gene, beta Catenin, Aged, Neoplasm Staging, Aged, 80 and over, Genetics, Gastroenterology, Microsatellite instability, Middle Aged, Zebrafish Proteins, medicine.disease, digestive system diseases, Wnt Proteins, Cytoskeletal Proteins, Catenin, Mutation, Trans-Activators, Cancer research, biology.protein, Female, Mitogens, Colorectal Neoplasms, Microsatellite Repeats, Signal Transduction
Abstract

Background: Adenomatous polyposis coli (APC) and b-catenin (encoded by CTNNB1) are important components in the WNT signalling pathway, a pathway altered in nearly all colorectal tumours. Cone icting results are reported on whether APC mutations are less common in tumours with a high degree ofmicrosatellite instability (MSI-H)than in microsatellite stable (MSS) ones,and whether mutations in the regulatory domain of CTNNB1 substitute for APC mutations in the MSI-H tumours. Methods: A consecutive series of 218 primary colorectal carcinomas, stratie ed by MSI status, were analysed for mutations in the APC gene (by the protein truncation test) and in the CTNNB1 gene (by single-strand conformation polymorphism). Results: APC mutations detected in 66% of the patients were signie cantly more frequent in the MSS and MSI-L (low) tumours than in the MSI-H tumour group (P < 0.001). The MSI-H tumours tended to have more frameshift mutations than the MSS/MSI-L tumours. The majority of the APC mutations were located in the mutation cluster region (MCR). Patients that had lost all b-catenin binding sites of the APC gene showed a shorter survival time than patients who retained some or all of these binding sites (P = 0.045). Two mutations were found in the CTNNB1 gene, but neither of them was located in the regulatory domain in exon 3. Conclusion: This study conerms that APC mutations are less frequent in MSI-H tumours than in MSS and MSI-L tumours. However, CTNNB1 mutations do not substitute for APC mutations in MSI-H tumours in these Norwegian patients.

Published
2002

170. [No real loss of referral obligations]

Author

Eilif, Haaland, Eivind, Meland, Morten, Magelssen, Harald, Salbu, Gunhild, Felde, Ola Didrik, Saugstad, and Torleiv, Rognum

Subjects
Norway, Pregnancy, Humans, Abortion, Induced, Female, Practice Patterns, Physicians', Referral and Consultation
Published
2014

171. A novel transcript, VNN1-AB, as a biomarker for colorectal cancer

Author

Marthe, Løvf, Torfinn, Nome, Jarle, Bruun, Mette, Eknaes, Anne C, Bakken, John P, Mpindi, Sami, Kilpinen, Torleiv O, Rognum, Arild, Nesbakken, Olli, Kallioniemi, Ragnhild A, Lothe, and Rolf I, Skotheim

Subjects
Adenoma, Colon, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Exons, GPI-Linked Proteins, Prognosis, Real-Time Polymerase Chain Reaction, Amidohydrolases, Alternative Splicing, Biomarkers, Tumor, Tumor Cells, Cultured, Humans, RNA, Messenger, Colorectal Neoplasms, Neoplasm Staging, Oligonucleotide Array Sequence Analysis
Abstract

Colorectal cancer is a global health challenge with high incidence rate and mortality. The patients' prognosis is strongly associated with disease stage and currently there is a need for improved prognostic and predictive biomarkers. In this study, novel colorectal cancer-specific transcript structures were nominated from whole transcriptome sequencing of seven colorectal cancer cell lines, two primary colorectal carcinomas with corresponding normal colonic mucosa and 16 normal tissues. The nominated transcripts were combined with gene level outlier expression analyses in a cohort of 505 colorectal cancers to identify biomarkers with capacity to stratify colorectal cancer subgroups. The transcriptome sequencing data and outlier expression analysis revealed 11 novel colorectal cancer-specific exon-exon junctions, of which 3 were located in the gene VNN1. The junctions within VNN1 were further characterized using rapid amplification of cDNA ends (RACE) and the prevalence of the subsequently characterized novel transcript, VNN1-AB, was investigated by real-time RT-PCR in 291 samples of miscellaneous origins. VNN1-AB was not present in any of the 43 normal colorectal tissue samples investigated, but in 5 of the 6 polyps, and 102 of the 136 (75%) colorectal cancers. We have identified a novel transcript of the VNN1 gene, with an organ-confined complete specificity for colorectal neoplasia.

Published
2014

172. Changes in the epidemiological pattern of sudden infant death syndrome in southeast Norway, 1984–1998: implications for future prevention and research

Author

Åshild Vege, Marianne Arnestad, M Andersen, and Torleiv O. Rognum

Subjects
Adult, Male, medicine.medical_specialty, Pediatrics, Adolescent, Statistics as Topic, Reproductive medicine, Sudden death, Pregnancy, Risk Factors, Epidemiology, Prone Position, medicine, Humans, Risk factor, Norway, business.industry, Public health, Smoking, Age Factors, Infant, Newborn, Case-control study, Infant, Sudden infant death syndrome, medicine.disease, Pregnancy Complications, Crowding, Community Child Health, Public Health, and Epidemiology, Case-Control Studies, Child, Preschool, Prenatal Exposure Delayed Effects, Pediatrics, Perinatology and Child Health, Female, Seasons, business, Sudden Infant Death, Maternal Age
Abstract

AIMTo look for changes in risk factors for sudden infant death syndrome (SIDS) after decrease and stabilisation of the SIDS rate.METHODSQuestionnaires were distributed to parents of 174 SIDS infants, dying between 1984 and 1998, and 375 age and sex matched controls in southeast Norway.RESULTSThe proportion of infants sleeping prone has decreased, along with the decrease in SIDS rate for the region during the periods studied, but over half of the SIDS victims are still found in the prone position. As the number of SIDS cases has decreased, additional risk factors have become more significant. Thus, after 1993, a significantly increased risk of SIDS is seen when the mother smokes during pregnancy. After 1993, young maternal age carries an increased risk. Maternal smoking and young maternal age are associated with each other. For SIDS victims, an increase in the number of infants found dead while co-sleeping is seen, and the age peak between 2 and 4 months and the winter peak have become less pronounced.CONCLUSIONChanges in risk factor profile following the decrease in SIDS rate in the early 1990s, as well as consistency of other factors, provides further clues to SIDS prevention and to the direction of further studies of death mechanisms.

Published
2001

173. A strategy combining flow sorting and comparative genomic hybridization for studying genetic aberrations at different stages of colorectal tumorigenesis in ulcerative colitis

Author

Solveig Norheim Andersen, Ole Petter F. Clausen, Torleiv O. Rognum, Helle Strømkjær, Steen Kølvraa, Viggo Nielsen, and Lars Bolund

Subjects
Biophysics, Cell Biology, Hematology, In situ hybridization, Biology, medicine.disease, medicine.disease_cause, Molecular biology, Pathology and Forensic Medicine, law.invention, Endocrinology, Genetic imbalance, Dysplasia, law, medicine, Primer (molecular biology), Carcinogenesis, Gene, Polymerase chain reaction, Comparative genomic hybridization
Abstract

Background DNA aneuploidy has been shown to increase the risk of developing dysplasia in ulcerative colitis (UC) and is related to tumorigenesis in the colorectum. Therefore, it is of particular interest to study genetic aberrations behind DNA aneuploidization during colorectal carcinogenesis. We wanted to elucidate further the relationship between mucosal morphology and DNA aberrations in UC. Methods DNA flow cytometry was applied to multiple lesions including regenerative, dysplastic, and carcinomatous mucosa from the colectomy specimen of a male patient with long-standing UC. The lesions harbored multiple DNA aneuploid stemlines that were subjected to flow sorting. We analyzed gene alterations by degenerate oligonucleotide primer (DOP; universal primers) polymerase chain reaction (PCR)-based comparative genomic hybridization (CGH) and fluorescent in situ hybridization (FISH) in diploid and aneuploid sorted cells. Results DOP-PCR–based CGH shows gains and losses that can be verified by FISH. We show that with this approach one can study genetic evolution of distinct DNA diploid and aberrant subpopulations through defined stages of colorectal tumorigenesis. This includes getting information related to tumor heterogeneity that cannot be obtained by CGH with DNA extracted from nonsorted cell populations. Genetic imbalance was also detected in diploid nondysplastic flow-sorted mucosal cells from the same bowel. Conclusions Similar gains and losses were found in aneuploid dysplasias and carcinomas at widely separated locations in the same bowel, indicating a common selection pressure in different areas of the same bowel. The common aberrations may be of importance for progression from dysplasia to carcinoma. Cytometry 43:46–54, 2001. © 2001 Wiley-Liss, Inc.

Published
2000

174. Cardiac potassium channel dysfunction in sudden infant death syndrome

Author

Troy E. Rhodes, Robert L. Abraham, Richard C. Welch, Carlos G. Vanoye, Lia Crotti, Marianne Arnestad, Roberto Insolia, Matteo Pedrazzini, Chiara Ferrandi, Ashild Vege, Torleiv Rognum, Dan M. Roden, Peter J. Schwartz, Alfred L. George, Rhodes, T, Abraham, R, Welch, R, Vanoye, C, Crotti, L, Arnestad, M, Insolia, R, Pedrazzini, M, Ferrandi, C, Vege, A, Rognum, T, Roden, D, Schwartz, P, and George AL, J

Subjects
medicine.medical_specialty, ERG1 Potassium Channel, Long QT syndrome, hERG, Mutation, Missense, CHO Cells, Gene mutation, Transfection, Sudden death, Article, Afterdepolarization, Membrane Potentials, Cricetulus, BIO/09 - FISIOLOGIA, Internal medicine, Cricetinae, Medicine, Animals, Humans, Genetic Predisposition to Disease, Molecular Biology, biology, business.industry, Infant, Newborn, Short QT syndrome, MED/11 - MALATTIE DELL'APPARATO CARDIOVASCOLARE, Sudden infant death syndrome, medicine.disease, Potassium channel, Ether-A-Go-Go Potassium Channels, Markov Chains, Electrophysiology, Long QT Syndrome, Anesthesia, Cardiology, biology.protein, long qt syndrome, sudden infant death syndrome, cardiac potassium channel, KCNH2, geneics, Cardiology and Cardiovascular Medicine, business, Sudden Infant Death
Abstract

Life-threatening arrhythmias have been suspected as one cause of the sudden infant death syndrome (SIDS), and this hypothesis is supported by the observation that mutations in arrhythmia susceptibility genes occur in 5-10% of cases. However, the functional consequences of cardiac potassium channel gene mutations associated with SIDS and how these alleles might mechanistically predispose to sudden death are unknown. To address these questions, we studied four missense KCNH2 (encoding HERG) variants, one compound KCNH2 genotype, and a missense KCNQ1 mutation all previously identified in Norwegian SIDS cases. Three of the six variants exhibited functional impairments while three were biophysically similar to wild-type channels (KCNH2 variants V279M, R885C, and S1040G). When co-expressed with WT-HERG, R273Q and K897T/R954C generated currents resembling the rapid component of the cardiac delayed rectifier current (I(Kr)) but with significantly diminished amplitude. Action potential modeling demonstrated that this level of functional impairment was sufficient to evoke increased action potential duration and pause-dependent early afterdepolarizations. By contrast, KCNQ1-I274V causes a gain-of-function in I(Ks) characterized by increased current density, faster activation, and slower deactivation leading to accumulation of instantaneous current upon repeated stimulation. Action potential simulations using a Markov model of heterozygous I274V-I(Ks) incorporated into the Luo-Rudy (LRd) ventricular cell model demonstrated marked rate-dependent shortening of action potential duration predicting a short QT phenotype. Our results indicate that certain potassium channel mutations associated with SIDS confer overt functional defects consistent with either LQTS or SQTS, and further emphasize the role of congenital arrhythmia susceptibility in this syndrome.

Published
2007

175. Villous, hypermucinous mucosa in long standing ulcerative colitis shows high frequency of K-ras mutations

Author

Torleiv O. Rognum, Arne Bakka, O. Fausa, Tone Løvig, Ole Petter F. Clausen, and Solveig Norheim Andersen

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Adenocarcinoma, Biology, medicine.disease_cause, Article, Lesion, Risk Factors, Carcinoma, medicine, Humans, Intestinal Mucosa, Mutation frequency, Aged, Mutation, Gastroenterology, Cancer, Middle Aged, medicine.disease, Ulcerative colitis, Genes, ras, Dysplasia, Colonic Neoplasms, Colitis, Ulcerative, Female, medicine.symptom, Carcinogenesis
Abstract

BACKGROUND—K-ras mutation is one of the first genetic alterations in classical colorectal carcinogenesis. AIMS—To investigate the role of K-ras mutations in carcinogenesis, in long standing ulcerative colitis. METHODS—A total of 161 microdissected and 100 DNA samples from 13 patients were analysed for K-ras codons 12 and 13 mutations by means of a combination of enriched polymerase chain reaction amplification and temporal temperature gradient electrophoresis. RESULTS—K-ras mutations were found in 21/161 (13%) microdissected samples in 7/13 large bowels (16 and five in codons 12 and 13, respectively), and in 10/100 (10%) mucosal DNA samples (six and four, respectively). One of four patients with six adenocarcinomas had a K-ras mutation in a carcinoma, as well as one of two patients with large dysplasia associated lesion or mass (DALM). Eight of 13 (61%) areas with villous architecture and large, distended goblet cells, had a K-ras mutation, which was significantly more frequent than in low grade dysplasia (one of 23, 4%) but did not reach significance versus high grade dysplasia (four of 14, 28.5%). K-ras mutations were found in one of 20 (5%) flat lesions indefinite for dysplasia, two of 14 (14%) in non-villous, hypermucinous mucosa, and in one of 57 flat areas negative for dysplasia. CONCLUSION—The highest K-ras mutation frequency was found in villous, hypermucinous mucosa. We suggest that this entity should be investigated further as a potential risk lesion for cancer development. It may represent a pathway directly from non-classical dysplasia to cancer, not previously described. Keywords: K-ras mutations; ulcerative colitis; dysplasia; dysplasia associated lesion or mass

Published
1999

177. Regulator of Chromosome Condensation 2 Identifies High-Risk Patients within Both Major Phenotypes of Colorectal Cancer

Author

Bruun, Jarle, Kolberg, Matthias, Ahlquist, Terje C., Royrvik, Ellen C., Nome, Torfinn, Leithe, Edward, Lind, Guro E., Merok, Marianne A., Rognum, Torleiv O., Bjorkoy, Geir, Johansen, Terje, Lindblom, Annika, Sun, Xiao-Feng, Svindland, Aud, Liestol, Knut, Nesbakken, Arild, Skotheim, Rolf I., Lothe, Ragnhild A., Bruun, Jarle, Kolberg, Matthias, Ahlquist, Terje C., Royrvik, Ellen C., Nome, Torfinn, Leithe, Edward, Lind, Guro E., Merok, Marianne A., Rognum, Torleiv O., Bjorkoy, Geir, Johansen, Terje, Lindblom, Annika, Sun, Xiao-Feng, Svindland, Aud, Liestol, Knut, Nesbakken, Arild, Skotheim, Rolf I., and Lothe, Ragnhild A.

Abstract

Purpose: Colorectal cancer has high incidence and mortality worldwide. Patients with microsatellite instable (MSI) tumors have significantly better prognosis than patients with microsatellite stable (MSS) tumors. Considerable variation in disease outcome remains a challenge within each subgroup, and our purpose was to identify biomarkers that improve prediction of colorectal cancer prognosis. Experimental Design: Mutation analyses of 42 MSI target genes were performed in two independent MSI tumor series (n = 209). Markers that were significantly associated with prognosis in the test series were assessed in the validation series, followed by functional and genetic explorations. The clinical potential was further investigated by immunohistochemistry in a population-based colorectal cancer series (n = 903). Results: We identified the cell-cycle gene regulator of chromosome condensation 2 (RCC2) as a cancer biomarker. We found a mutation in the 50 UTR region of RCC2 that in univariate and multivariate analyses was significantly associated with improved outcome in the MSI group. This mutation caused reduction of protein expression in dual luciferase gene reporter assays. siRNA knockdown in MSI colon cancer cells (HCT15) caused reduced cell proliferation, cell-cycle arrest, and increased apoptosis. Massive parallel sequencing revealed few RCC2 mutations in MSS tumors. However, weak RCC2 protein expression was significantly associated with poor prognosis, independent of clinical highrisk parameters, and stratifies clinically important patient subgroups with MSS tumors, including elderly patients (greater than 75 years), stage II patients, and those with rectal cancer. Conclusions: Impaired RCC2 affects functional and clinical endpoints of colorectal cancer. High-risk patients with either MSI or MSS tumors can be identified with cost-effective routine RCC2 assays. (C) 2015 AACR., Funding Agencies|Norwegian Cancer Society [PR-2006-0442, PR-2007-0166]; South-Eastern Norway Regional Health Authority

Published
2015
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178. Objective measurements of nicotine exposure in victims of sudden infant death syndrome and in other unexpected child deaths

Author

Åshild Vege, Torleiv O. Rognum, Siri H. Opdal, and J Milerad

Subjects
Parents, Pediatrics, medicine.medical_specialty, Passive smoking, Autopsy, medicine.disease_cause, Sudden death, Tobacco smoke, Nicotine, chemistry.chemical_compound, Risk Factors, Infant Mortality, Humans, Medicine, Risk factor, Norway, business.industry, Infant, Newborn, Infant, Sudden infant death syndrome, chemistry, Pediatrics, Perinatology and Child Health, Tobacco Smoke Pollution, Cotinine, business, Sudden Infant Death, medicine.drug
Abstract

Objective: Self-reported maternal smoking is associated with a dose-related increase in the risk of sudden infant death syndrome (SIDS). The aim of this study was to measure objectively whether victims of SIDS are more exposed to tobacco smoke before death than infants who die unexpectedly of other causes. Design: Cotinine levels in pericardial fluid were used as an indicator of exposure. Levels >5 ng/mL indicated significant exposure, and levels >20 ng/mL indicated heavy exposure. Samples were obtained from all sudden deaths in children

Published
1998

179. Different genetic pathways to proximal and distal colorectal cancer influenced by sex-related factors

Author

Anne Lise Børresen-Dale, Gunn Iren Meling, Torleiv O. Rognum, Ragnhild A. Lothe, Gustav Gaudernack, and Jarle Breivik

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Multivariate analysis, Tumor suppressor gene, business.industry, Colorectal cancer, Incidence (epidemiology), Rectum, Microsatellite instability, medicine.disease, medicine.disease_cause, Gastroenterology, medicine.anatomical_structure, Internal medicine, medicine, Carcinoma, business, Carcinogenesis
Abstract

Mutations in the k-ras and TP53 genes, as well as microsatellite instability (MIN), are frequent genetic alterations in colorectal carcinomas and represent 3 different mechanisms in the carcinogenic process. Both the incidence of colorectal cancer and the frequency of genetic alterations in such tumours have been related to different clinico-pathological variables, including age and gender of the patient and location of the tumour. A number of studies have also reported associations between different types of genetic alterations. We therefore wanted to explore the relationship between these genetic and clinico-pathological variables using multivariate analysis on material from 282 colorectal carcinomas. Three logistic regression models were constructed: 1) the presence of K-ras mutations was dependent on MIN and age and gender of patient, with an especially low frequency among younger males and in tumours with MIN (overall p = 0.0003); 2) the presence of TP53 mutations was only dependent on tumour location, with a positive association to cancers occurring distally (p = 0.002); and 3) the presence of MIN was dependent on age, gender and K-ras and TP53 mutations, as well as on tumour location. MIN was most frequent among younger male and older female patients, was rare in tumours with K-ras or TP53 mutations and was found almost exclusively in the proximal colon (overall p < 0.0001). Our data confirm that different genetic pathways to colorectal cancer dominate in the proximal and distal segments of the bowel and suggest that the K-ras- and MIN-dependent pathways are influenced by different sex-related factors.

Published
1997

180. Use of new Nordic criteria for classification of SIDS to re-evaluate diagnoses of sudden unexpected infant death in the Nordic countries

Author

Å Vege and TO Rognum

Subjects
Pediatrics, medicine.medical_specialty, Chi-Square Distribution, business.industry, International Cooperation, Infant, Reproducibility of Results, General Medicine, Norwegian, Scandinavian and Nordic Countries, Sudden death, language.human_language, Infant mortality, Disease Outbreaks, Pediatrics, Perinatology and Child Health, language, medicine, Humans, Diagnostic Errors, Medical diagnosis, business, Finland, Sudden Infant Death, Retrospective Studies
Abstract

To investigate whether changes in diagnostic practice might be the cause of the SIDS epidemic in the Nordic countries in the 1970s and 1980s a cooperative study was initiated in 1990. Common morphologic diagnostic criteria for SIDS were established in 1992 and 127 randomly selected sudden unexpected infant deaths from all Nordic countries from 1970 to 1995 and 205 cases from the Institute of Forensic Medicine, Oslo, Norway (RMI) from 1984 to 1995 were re-evaluated blindly using the new criteria. Neither the increase nor the decline in the SIDS rate since 1989 seemed to be due to changed diagnostic practices. SIDS seemed to have been under-diagnosed before the new criteria came into operation in 1992. There were fewer discrepancies between the original and revised diagnoses in the RMI cases than in the rest of the Norwegian cases, both before and after 1992.

Published
1997

181. K-rasMutations and Prognosis in Large-Bowel Carcinomas

Author

Gunn Iren Meling, S. Norheim Andersen, Torleiv O. Rognum, Gustav Gaudernack, Tone Løvig, Eiliv Lund, and Jarle Breivik

Subjects
Adult, Male, Biology, medicine.disease_cause, law.invention, Risk Factors, law, medicine, Carcinoma, Humans, Point Mutation, Gene, Polymerase chain reaction, Survival analysis, Aged, Neoplasm Staging, Aged, 80 and over, Genetics, Mutation, Point mutation, Gastroenterology, Middle Aged, Prognosis, medicine.disease, Survival Analysis, Genes, ras, Cancer research, Adenocarcinoma, Female, Neoplasm Recurrence, Local, Restriction fragment length polymorphism, Colorectal Neoplasms, Follow-Up Studies
Abstract

Colorectal carcinogenesis is regarded as a multistep process involving several genetic alterations, with mutation in the K-ras gene in about half of the tumours. We aimed at clarifying the role of this genetic alteration related to survival and clinicopathologic variables.One hundred large-bowel carcinomas operated on between 1978 and 1982 were studied for the presence of point mutations in codons 12 and 13 of the K-ras gene, using enriched polymerase chain reaction amplification, restriction fragment length polymorphism analysis, and direct sequencing.Forty mutations were found (40%): 31 in codon 12 and 9 in codon 13, 7 different types. There was no relationship between tumours with and without K-ras mutations with regard to Dukes' stages, age or sex of the patient, tumour localization, histologic grade, DNA ploidy pattern, HLA-DR staining pattern, or survival. Samples from 5 different localizations in 7 carcinomas showed identical K-ras mutation pattern, as did 19 recurrences/ metastases originating from 11 carcinomas.When present, the primary tumour shows homogeneous distribution of K-ras mutation, and the mutation follows the carcinoma in the secondary deposit, regardless of lymphogenous or hematogenous spread. The presence of K-ras mutation does not seem to have prognostic significance for the patient, and the precise nucleotide change is furthermore not predictive of tumour behaviour.

Published
1997

182. High frequency of fusion transcripts involving TCF7L2 in colorectal cancer: novel fusion partner and splice variants

Author

Torfinn, Nome, Andreas M, Hoff, Anne Cathrine, Bakken, Torleiv O, Rognum, Arild, Nesbakken, and Rolf I, Skotheim

Subjects
Oncogene Proteins, Fusion, RNA Splicing, Molecular Sequence Data, Gene Identification and Analysis, Gene Splicing, Molecular Genetics, Gastrointestinal Tumors, Genetics, Cancer Genetics, Humans, RNA, Messenger, Biology, Gene Rearrangement, Base Sequence, Genome, Human, Reproducibility of Results, Computational Biology, Cancers and Neoplasms, Exons, Genomics, HCT116 Cells, Oncology, Genetic Loci, Medicine, RNA Splice Sites, Colorectal Neoplasms, Transcription Factor 7-Like 2 Protein, Research Article
Abstract

VTI1A-TCF7L2 was reported as a recurrent fusion gene in colorectal cancer (CRC), found to be expressed in three out of 97 primary cancers, and one cell line, NCI-H508, where a genomic deletion joins the two genes [1]. To investigate this fusion further, we analyzed high-throughput DNA and RNA sequencing data from seven CRC cell lines, and identified the gene RP11-57H14.3 (ENSG00000225292) as a novel fusion partner for TCF7L2. The fusion was discovered from both genome and transcriptome data in the HCT116 cell line. By triplicate nested RT-PCR, we tested both the novel fusion transcript and VTI1A-TCF7L2 for expression in a series of 106 CRC tissues, 21 CRC cell lines, 14 normal colonic mucosa, and 20 normal tissues from miscellaneous anatomical sites. Altogether, 42% and 45% of the CRC samples expressed VTI1A-TCF7L2 and TCF7L2-RP11-57H14.3 fusion transcripts, respectively. The fusion transcripts were both seen in 29% of the normal colonic mucosa samples, and in 25% and 75% of the tested normal tissues from other organs, revealing that the TCF7L2 fusion transcripts are neither specific to cancer nor to the colon and rectum. Seven different splice variants were detected for the VTI1A-TCF7L2 fusion, of which three are novel. Four different splice variants were detected for the TCF7L2-RP11-57H14.3 fusion. In conclusion, we have identified novel variants of VTI1A-TCF7L2 fusion transcripts, including a novel fusion partner gene, RP11-57H14.3, and demonstrated detectable levels in a large fraction of CRC samples, as well as in normal colonic mucosa and other tissue types. We suggest that the fusion transcripts observed in a high frequency of samples are transcription induced chimeras that are expressed at low levels in most samples. The similar fusion transcripts induced by genomic rearrangements observed in individual cancer cell lines may yet have oncogenic potential as suggested in the original study by Bass et al.

Published
2013

189. The doctors' role in cases of suspected child abuse.

Author

STRAY-PEDERSEN, ARNE, MØLLER, CLAUS, DE LANGE, CHARLOTTE, DUE-TØNNESSEN, BERNT J., GRØGAARD, JENS B., HAUGEN, OLAV H., HIKMAT, OMAR, MAHESPARAN, RUBY, MÜLLER, LIL-SOFIE ORDING, MYHRE, ARNE KRISTIAN, MYHRE, MIA CATHRINE, NEDREGAARD, BÅRD, NORDHOV, SOLVEIG MARIANNE, ROGNUM, TORLEIV OLE, ROSENDAHL, KAREN, SØRBØ, TOMAS, JO VOLLMER-SANDHOLM, MARY, and AUKLAND, STEIN MAGNUS

Published
2018
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190. Fatal Accident Resulting from Methyl Bromide Poisoning after Fumigation of a Neighbouring House; Leakage through Sewage Pipes

Author

Sverre Langård, Øystein Fløtterød, Torleiv Rognum, and Vidar Skaug

Subjects
Male, medicine.medical_specialty, Fumigation, Sewage, Autopsy, Infant, Premature, Diseases, Toxicology, chemistry.chemical_compound, Bromide, medicine, Humans, Cause of death, Inhalation, business.industry, Infant, Newborn, Pneumonia, Police, Hydrocarbons, Brominated, Surgery, chemistry, Anesthesia, Toxicity, Vomiting, Female, medicine.symptom, business, Infant, Premature
Abstract

An intoxication after using methyl bromide (CH3Br) in fumigation is reported. The accident resulted in the death of a newborn infant within 12-13 h after exposure, as well as clinical intoxication of the infant's parents. The concentration of bromide ion in the infant's blood was 170 mg l-1 and in the parents blood it was 130 and 110 mg l-1. Autopsy showed that the cause of death was acute pneumonia due to aspiration, most likely resulting from vomiting and aspiration after inhalation of CH3Br. The clinical symptoms of the parents are reported, as well as a brief survey on the kinetics and CH3Br toxicity in animals and humans. Reconstruction of the events prior to the intoxication revealed that the sewage pipes serving the two houses had been sucked empty only 1-2 h prior to the start of fumigation, resulting in an open sewage connection between the houses and permitting CH3Br to leak from the treated house into the house of the affected family.

Published
1996

191. K-ras mutations and HLA-DR expression in large bowel adenomas

Author

Torleiv O. Rognum, Jarle Breivik, Gunn Iren Meling, Gustav Gaudernack, Eiliv Lund, Ole Petter F. Clausen, Tone Løvig, Aasa R. Schjølberg, Frøydis Langmark, S. Norheim Andersen, and O. Fausa

Subjects
Adenoma, Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Molecular Sequence Data, Biology, medicine.disease_cause, Epithelium, Antigen, medicine, HLA-DR, Humans, Aged, Aged, 80 and over, Mutation, Base Sequence, Point mutation, Single-strand conformation polymorphism, HLA-DR Antigens, Middle Aged, medicine.disease, Up-Regulation, Genes, ras, Oncology, Dysplasia, Cancer research, Immunohistochemistry, Female, Colorectal Neoplasms, Research Article
Abstract

A total of 72 sporadic colorectal adenomas in 56 patients were studied for the presence of point mutations in codons 12 and 13 of the K-ras gene and for HLA-DR antigen expression related to clinicopathological variables. Forty K-ras mutations in 39 adenomas were found (54%): 31 (77%) in codon 12 and nine (23%) in codon 13. There was a strong relationship between the incidence of K-ras mutations and adenoma type, degree of dysplasia and sex. The highest frequency of K-ras mutations was seen in large adenomas of the villous type with high-grade dysplasia. Fourteen out of 15 adenomas obtained from 14 women above 65 years of age carried mutations. HLA-DR positivity was found in 38% of the adenomas, large tumours and those with high-grade dysplasia having the strongest staining. Coexpression of K-ras mutations and HLA-DR was found significantly more frequently in large and highly dysplastic adenomas, although two-way analysis of variance showing size and grade of dysplasia to be the most important variable. None of the adenomas with low-grade dysplasia showed both K-ras mutation and HLA-DR positivity (P = 0.004). K-ras mutation is recognised as an early event in colorectal carcinogenesis. The mutation might give rise to peptides that may be presented on the tumour cell surface by class II molecules, and thereby induce immune responses against neoplastic cells. Images Figure 3 Figure 4 Figure 5 Figure 6

Published
1996

192. Beta-endorphin immunoreactivity levels in CSF after laryngeal chemoreflex activation correlate with apnoea duration in piglets

Author

Lauritz Stoltenberg, Hanne Storm, Ola Didrik Saugstad, Karl L Reichelt, and Torleiv O. Rognum

Subjects
Male, medicine.medical_specialty, Narcotic antagonists, Time Factors, Apnea, Swine, Narcotic Antagonists, Radioimmunoassay, Blood Pressure, Random Allocation, Reflex, Bradycardia, medicine, Animals, Humans, Gynecology, Random allocation, Naloxone, business.industry, beta-Endorphin, Obstetrics and Gynecology, Animals, Newborn, Pediatrics, Perinatology and Child Health, Female, Respiratory control, Larynx, business
Abstract

L'activation du reflexe humoral larynge provoquant un reflux gastro-oesophagien, peut constituer un mecanisme pathogenique de l'apnee en liaison avec un risque pour la vie et le SIDS. Les enfants souffrant de reflux gastro-oesophagique et d'apnee presentent un taux accru d'immuno-reactivite de la β-endorphine dans le plasma. La β-endorphine peut inhiber la respiration et induire la bradycardie. La naloxone est un antagoniste de la β-endorphine et il a ete etabli qu'elle peut etre utilisee avec succes pour soigner les enfants souffrant d'apnee et presentant un niveau accru d'immuno-reactivite de β-endorphine du liquide cephalo-rachidien. Dans le but de determiner si la β-endorphine du liquide cephalo-rachidien augmentait avec le reflexe humoral larynge induisant l'apnee chez le porcelet, nous avons provoque un reflexe humoral larynge avec et sans pre-traitement a la naloxone et nous avons mesure l'immuno-reactivite de la β-endorphine dans le liquide cephalo-rachidien avant et apres l'episode d'apnee. Nous avons pris des porcelets de t a 10 jours qui avaient suivi une premedication a l'azaperone et auxquels nous avons administre de la metomidate jusqu'a etablissement d'une anesthesie adequate. Les porcelets ont subi une ventilation mecanique jusqu'a 60 min apres l'intervention, apres quoi ils respiraient spontanement. Nous avons enregistre le rythme respiratoire, le volume minute et le volume courant. Pendant l'intervention, nous avons place une sonde vesicale dans l'espace subglottal pour insuffler le larynx avec l'air sature d'ammoniaque destine a stimuler le reflexe humoral larynge. Nous avons aussi place un catheter arteriel pour enregistrer la pression sanguine. La pouls etait enregistre par electrodes sur la peau. Nous avons administre a un groupe de porcelets 100 microgrammes/kg de naloxone i. v. 5 minutes avant le reflexe humoral larynge induisant l'apnee (n = 6) tandis que l'autre groupe n'etait pas traite (n = 7). Le liquide cephalo-rachidien a ete preleve avant et apres chaque episode d'apnee par ponction sous-occipitale. Les taux de β-endorphine ont ete mesures par dosage immuno-radiologique du liquide cephalo-rachidien. Les surnageants de l'examen immuno-radiologique ont ete transferes a une HPLC pour verifier que la β-endorphine avait ete mesuree. Nous avons applique le test Mann-Whitney U pour comparer les deux groupes et, pour les examens de correlation, nous nous sommes servi du coefficient de correlation des rangs de Spearman. Nous avons constate que la duree moyenne des episodes e'apnee chez les porcelets traites a la naloxone etait nettement plus courte que chez les porcelets non traites (n = 0,02) avec respectivement 12 sec (plage de 0 a 20) et de 28 sec (plage de 10 a 40). Pour le reste, l'accroissement de la pression sanguine et le ralentissement du rythme cardiaque pendant le reflexe humoral larynge provoquant l'apnee chez les porcelets traites a la naloxone ne presentait aucune difference significative par rapport aux porcelets non traites. Le niveau d'immuno-reactivite de la β-endorphine du liquide cephalo-rachidien avant l'apnee etait inferieur a 4,3 fmol/ml SCF. Le niveau moyen d'immuno-reactivite de la β-endorphine du liquide cephalo-rachidien apres l'apnee les porcelets traites a la naloxone ne presentait pas de difference statistiquement pertinente par rapport aux porcelets non traites avec respectivement 615 fmol/ ml CSF (plage de 93 a 1090) et 984 fmol/ml CSF (plage de 380 a 2400) (figure 1). Apres transfert du materiel d'immuno-reactivite de la β-endorphine du dosage immuno-radiologique a la HPLC, nous avons du demontrer l'identite avec la )-endorphine ajoutee. Nous avons aussi mis en relation le niveau d'immuno-r

Published
1996

193. Somatic mutations in the hMSH2 gene in microsatellite unstable colorectal carcinomas

Author

Ragnhild A. Lothe, Lipford J, Michael F. Kane, Sigrid Lystad, Torleiv O. Rognum, Anne Lise Børresen, Gunn Iren Meling, Paul T. Morrison, and Richard D. Kolodner

Subjects
Adult, DNA Repair, Somatic cell, Molecular Sequence Data, DNA, Satellite, Biology, medicine.disease_cause, Germline, Fungal Proteins, Germline mutation, Genetics, medicine, Humans, Amino Acid Sequence, Molecular Biology, Gene, Germ-Line Mutation, Genetics (clinical), Aged, Aged, 80 and over, Mutation, Polymorphism, Genetic, Base Sequence, Microsatellite instability, DNA, Neoplasm, General Medicine, Middle Aged, medicine.disease, DNA-Binding Proteins, MutS Homolog 2 Protein, Cancer research, Microsatellite, DNA mismatch repair, Colorectal Neoplasms
Abstract

Microsatellite instability is frequently seen in tumors from patients with hereditary nonpolyposis colorectal cancer (HNPCC). Germline mutations in the mismatch repair gene hMSH2 account for approximately 50% of these cases. Tumors from sporadic cases also exhibit this microsatellite instability phenotype, although at a lower frequency, and very few somatically derived mutations have so far been reported in such tumors. In this study DNA from 23 primary colorectal carcinomas (four familial and 19 sporadic cases) exhibiting microsatellite instability were screened for mutations in the hMSH2 gene using constant denaturant gel electrophoresis (CDGE). Among the sporadic cases, five (26%) were found to have somatically derived mutations. One tumor revealed two different mutations, possibly leading to a homozygous inactivation of the gene. One of the four familial cases was classified as having HNPCC, and a germline as well as a somatic mutation were found in this tumor. These results demonstrate that a considerable proportion of sporadic colorectal cancers with microsatellite instability, have somatic mutations in the hMSH2 gene.

Published
1995

194. β-Endorphin May Be a Mediator of Apnea Induced by the Laryngeal Chemoreflex in Piglets

Author

Ola Didrik Saugstad, Stephanie Øyasæter, Karl L Reichelt, Hanne Storm, Lauritz Stoltenberg, and Torleiv O. Rognum

Subjects
Blood Glucose, Male, Aging, medicine.medical_specialty, Apnea, Swine, Pilot Projects, Cisterna magna, Injections, Hemoglobins, chemistry.chemical_compound, Internal medicine, Cisterna Magna, Reflex, medicine, Animals, Respiratory system, Hypoxanthine, business.industry, Body Weight, beta-Endorphin, Hypoxia (medical), Vitreous Body, Blood pressure, Endocrinology, Hematocrit, chemistry, Hypoxanthines, Anesthesia, Pediatrics, Perinatology and Child Health, Female, Larynx, medicine.symptom, business, Respiratory minute volume
Abstract

To determine whether β-endorphin is involved in the laryngeal chemoreflex. we initially injected 0.01 1 mg of β-endorphin into the cisterna magna (i.c.m.) and registered the respiralory and cardiovascular patterns in 5–10-d-old piglets. From 0.1 to 1 mg of β-cndorphin i.c.m. induced a decrease in the minute volume, hearl rate, and blood pressure within 15 min. Within the next 30 min respiratory pauses accompanied by blood pressure increases and reductions in heart ratc developed, similar to the respiratory and cardiovascular pattern of the induced laryngcal chemoreflex. Based on these initial data, we decided to induce a laryngeal chemoreflex in piglets pretreated with 0.1 mg of β-endorphin i.c.m (n = 6), 0.2 mg of β-endorphin i.c.m. (n = 6), 0.1 mg of β-endorphin i.c.m. and 100 μg/kg naloxone i.v. (n = 6), 100 μg/kg naloxonc i.v. (n - 6). or water i.c.m. (n = 6). Because clevated levels of hypoxanthine in the vitreous humor may indicate hypoxia before death, we therefore measured the postmortem hypoxanthine levels in the vitreous humor. The laryngeal chemoreflex-induced apnea was shortenec in the piglet group pretreated with water i.c.m and naloxone i.v. (p < 0.01) and in the piglet group pictreated with 0.1 mg of β-endorphin i.c.m and naloxone i.v. (p < 0.05), but not significantly prolonged in the piglet groups pretreated with 0.1 or 0.2 mg of β-endorphin i.c.m. when compared with the piglcts prerreated with water i.c.m. The hypoxanthine levels in the vitreous humor were found increased after death only in piglets prctreated with 0.2 mg of β-endorphin i.c.m. before the laryngeal chemorefltex was induced (p < 0.05). We conclude that β-cndorphin is probably a mediator of apnca induced by the laryngenl chemoreflex in piglets.

Published
1995

195. A K-ras 13GLY → ASP mutation is recognized by HLA-DQ7 restricted T cells in a patient with colorectal cancer. Modifying effect of DQ7 on established cancers harbouring this mutation?

Author

Torbjørn Hansen, Erik Thorsby, Tobias Gedde-Dahl, Gustav Gaudernack, Beate Fossum, Jarle Breivik, Gunn Iren Meling, Torleiv O. Rognum, and Ingebjørg Knutsen

Subjects
CD4-Positive T-Lymphocytes, Cancer Research, Cellular immunity, Colorectal cancer, Molecular Sequence Data, Biology, Epitope, HLA-DQ Antigens, medicine, Humans, Amino Acid Sequence, Receptor, Conserved Sequence, HLA-DQ7, Haplotype, Middle Aged, medicine.disease, Genes, ras, Oncology, Mutation, Mutation (genetic algorithm), Immunology, Cancer research, Adenocarcinoma, Female, Colorectal Neoplasms
Abstract

We have characterized and described in detail 2 CD4+ T-lymphocyte clones (TLC) from a colonic cancer patient. These TLC specifically recognize a K-ras-derived peptide carrying the 13Asp mutation commonly found in adenocarcinomas of the colon. The TLC were independently derived, as they carried 2 different T-cell receptors. The TLC recognized partly overlapping epitopes within the 13Asp peptide, presented by HLA-DQ7 molecules, suggesting that this molecule might confer some protective immunity against the mutation. On the basis of analysis of 251 colonic carcinomas, the presence of HLA-DQ7 did not seem to protect against the establishment of carcinomas carrying the 13Asp mutation, since the frequency of the DQ7 haplotype was not decreased among patients having this mutation. A modifying effect of DQ7 on the development of carcinomas with a 13Asp mutation was, however, observed, resulting in fewer tumours reaching advanced Dukes stages when DQ7 was present.

Published
1994

196. Up-regulated Epithelial Expression of HLA-DR and Secretory Component in Salivary Glands: Reflection of Mucosal Immunostimulation in Sudden Infant Death Syndrome

Author

P. S. Thrane, Per Brandtzaeg, and Torleiv O. Rognum

Subjects
Pathology, medicine.medical_specialty, medicine.diagnostic_test, Salivary gland, business.industry, Secretory component, Human leukocyte antigen, Sudden infant death syndrome, Immunofluorescence, Sudden death, medicine.anatomical_structure, Antigen, Pediatrics, Perinatology and Child Health, Immunology, medicine, HLA-DR, business
Abstract

Human parotid glands from 55 forensic autopsy subjects, 1–12 mo of age, were examined by immunohistochemistry without knowledge about the cause of death. Various combinations of monoclonal or polyclonal antibody reagents of the following specificities were applied in two-color immunofluorescence analyses: HLA class I or II (DR, DP, or DQ); pan-T cell (CD3); leukocyte common antigen (CD45); and secretory component (poly-Ig receptor). Sudden infant death syndrome victims (n = 17) were shown to have significantly increased numbers of CD45+ stromal leukocytes and intensified epithelial expression of HLA-DR and secretory component as well as increased endothelial expression of both HLA class I and II (DR, DP, and DQ) determinants compared with controls (n = 31) who had died from noninfectious causes. Seven overtly infectious subjects (bronchopneumonia) showed still more up-regulated expression. This result suggested that enhanced stimulation of the local immune system exists in sudden infant death syndrome, with release of certain cytokines that are known to up-regulate epithelial expression of HLA-DR and secretory component.

Published
1994

197. Inverse relationship between beta-endorphin immunoreactivity in cerebrospinal fluid and nucleus tractus solitarius in sudden infant death

Author

Karl L Reichelt, Hanne Storm, and Torleiv O. Rognum

Subjects
Male, medicine.medical_specialty, Radioimmunoassay, Neuropeptide, Peptide hormone, Sudden death, chemistry.chemical_compound, Cerebrospinal fluid, Internal medicine, Solitary Nucleus, Humans, Medicine, Respiratory system, Chromatography, High Pressure Liquid, business.industry, Solitary nucleus, beta-Endorphin, Infant, Endocrinology, nervous system, chemistry, Postmortem Changes, Pediatrics, Perinatology and Child Health, Female, business, Sudden Infant Death
Abstract

In nucleus tractus solitarius (NTS) beta-endorphin (BEND) induces bradycardia and respiratory depression which have been reported to precede death in sudden infant death (SID). Of SID victims, 50% have elevated levels of beta-endorphin immunoreactivity (BENDI) in the cerebrospinal fluid (CSF), and 50% had undetectable levels. We therefore investigated the relationship of BENDI in the CSF to BENDI levels in the NTS area. This study included SID victims (CSF from n = 47, brain stem from n = 16), borderline SID victims (CSF and brain stem from n = 2), sudden death in childhood (CSF and brain stem from n = 1), and controls (CSF from n = 32, brain stem from n = 11). BEND in CSF and NTS area, after extraction, was measured by radioimmunoassay. High performance liquid chromatography was used for closer identification of BENDI. We found that the SID victims divided into two subpopulations, one having a relatively high BENDI level in CSF and one having no detectable level (P < 0.01). Furthermore, an inverse relationship was found between BENDI level in CSF and BENDI level in NTS area in the SID victims (P < 0.05). We conclude that increased BENDI level in CSF is associated with low BENDI level in the NTS area in 50% of SID victims. The low BENDI level in the NTS area may be due to increased release of BEND.

Published
1994

198. In-depth evaluation of real-world car collisions: fatal and severe injuries in children are predominantly caused by restraint errors and unstrapped cargo

Author

Torleiv O. Rognum, Pål Aksel Næss, Inggard Lereim, Arne Stray-Pedersen, Marianne Skjerven-Martinsen, and Trond Boye Hansen

Subjects
Engineering, Adolescent, Poison control, Crash, Suicide prevention, Occupational safety and health, Risk Factors, Injury prevention, medicine, Forensic engineering, Humans, Child, Child Restraint Systems, Cause of death, Trauma Severity Indices, business.industry, Norway, Medical record, Public Health, Environmental and Occupational Health, Accidents, Traffic, Human factors and ergonomics, Infant, medicine.disease, Child, Preschool, Wounds and Injuries, Medical emergency, business, human activities, Safety Research
Abstract

Major improvements have taken place in the development of child restraint systems and in-car safety in general, but motor vehicle accidents remain the leading cause of death and disability in children. An interdisciplinary study was therefore performed to investigate the injury mechanisms in car collisions involving children.Motor vehicle collisions (MVCs) resulting in death or serious injuries to the drivers or their passengers in the southeastern part of Norway in the period 2007-2009 were included in the study if children less than 16 years of age were passengers. An investigation team examined the crash scene within 24 h of the accident. The internal and external environment of the vehicle was investigated, with particular focus on safety equipment and registration of child occupant contact points. Information was collected from witnesses, crash victims, the police, road authority reports, and medical records. Clinical or postmortem examinations were performed on the child occupants.Fifteen high-impact car crashes involving 27 child occupants were investigated: 7 children died (median [range] age 8 (0-15) years), 8 were severely injured (8 [5-13] years), and 12 sustained minor or no injuries (3.5 [0-14] years). Fourteen out of 15 fatalities or severe injuries (MAIS ≥3) were found to be due to various safety errors: harness straps or seat belts incorrectly routed (5/15) or poorly adjusted (4/15), unstrapped luggage (4/15), or technical errors (1/15). All 7 of the fatally injured children died at the crash scene, and 6 died due to head/upper neck trauma. No safety errors were found among the 12 children with either minor or no injuries. No association was found between the instantaneous change in velocity (ΔV) and the injury severity.The risk of child passengers being severely or fatally injured in MVCs is significantly higher when they are incorrectly restrained or exposed to unsecured heavy luggage. Appropriate crash investigations may provide important information regarding the injury mechanisms, which will be necessary for the implementation of preventive measures to reduce future fatalities.

Published
2011

199. SPG20, a novel biomarker for early detection of colorectal cancer, encodes a regulator of cytokinesis

Author

Torleiv O. Rognum, Arild Nesbakken, Harald Stenmark, Stine A. Danielsen, Geir Hoff, Guro Elisabeth Lind, Ragnhild A. Lothe, Espen Thiis-Evensen, and Camilla Raiborg

Subjects
Male, Cancer Research, Colorectal cancer, Down-Regulation, Cell Cycle Proteins, cytokinesis, Mouse model of colorectal and intestinal cancer, Biology, Feces, Cell Line, Tumor, Genetics, Carcinoma, medicine, Biomarkers, Tumor, Humans, Promoter Regions, Genetic, early detection, Molecular Biology, Spartin, Cancer, Proteins, Methylation, DNA Methylation, Middle Aged, medicine.disease, Gene Expression Regulation, Neoplastic, DNA methylation, Cancer cell, Cancer research, Biomarker (medicine), Female, Original Article, methylation, SPG20, Colorectal Neoplasms, colorectal neoplasia
Abstract

Colorectal cancer is a common disease with high mortality. Suitable biomarkers for detection of tumors at an early curable stage would significantly improve patient survival. Here, we show that the SPG20 (spastic paraplegia-20) promoter, encoding the multifunctional Spartin protein, is hypermethylated in 89% of colorectal carcinomas, 78% of adenomas and only 1% of normal mucosa samples. SPG20 methylation was also present in a pilot series of stool samples and corresponding tumors from colorectal cancer patients. SPG20 promoter hypermethylation resulted in loss of mRNA expression in various cancer types and subsequent depletion of Spartin. We further showed that Spartin downregulation in cancer cells resulted in cytokinesis arrest, which was reversed when SPG20 methylation was inhibited. The present study identifies SPG20 promoter hypermethylation as a biomarker suitable for non-invasive detection of colorectal cancer, and a possible mechanism for cytokinesis arrest in colorectal tumorigenesis.

Published
2011

200. Transcriptome instability in colorectal cancer identified by exon microarray analyses: Associations with splicing factor expression levels and patient survival

Author

Trude H. Ågesen, Torleiv O. Rognum, Rolf Inge Skotheim, Arild Nesbakken, Ragnhild A. Lothe, and Anita Sveen

Subjects
Genetics, Research, Alternative splicing, Microsatellite instability, Biology, medicine.disease, Exon skipping, Transcriptome, Splicing factor, Exon, Chromosome instability, RNA splicing, medicine, Molecular Medicine, Genetics(clinical), Molecular Biology, Genetics (clinical)
Abstract

Background Colorectal cancer (CRC) is a heterogeneous disease that, on the molecular level, can be characterized by inherent genomic instabilities; chromosome instability and microsatellite instability. In the present study we analyze genome-wide disruption of pre-mRNA splicing, and propose transcriptome instability as a characteristic that is analogous to genomic instability on the transcriptome level. Methods Exon microarray profiles from two independent series including a total of 160 CRCs were investigated for their relative amounts of exon usage differences. Each exon in each sample was assigned an alternative splicing score calculated by the FIRMA algorithm. Amounts of deviating exon usage per sample were derived from exons with extreme splicing scores. Results There was great heterogeneity within both series in terms of sample-wise amounts of deviating exon usage. This was strongly associated with the expression levels of approximately half of 280 splicing factors (54% and 48% of splicing factors were significantly correlated to deviating exon usage amounts in the two series). Samples with high or low amounts of deviating exon usage, associated with overall transcriptome instability, were almost completely separated into their respective groups by hierarchical clustering analysis of splicing factor expression levels in both sample series. Samples showing a preferential tendency towards deviating exon skipping or inclusion were associated with skewed transcriptome instability. There were significant associations between transcriptome instability and reduced patient survival in both sample series. In the test series, patients with skewed transcriptome instability showed the strongest prognostic association (P = 0.001), while a combination of the two characteristics showed the strongest association with poor survival in the validation series (P = 0.03). Conclusions We have described transcriptome instability as a characteristic of CRC. This transcriptome instability has associations with splicing factor expression levels and poor patient survival.

Published
2011

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