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2. Genetic Control of Bordetella pertussis Infection: Identification of Susceptibility Loci Using Recombinant Congenic Strains of Mice

Author

H. A. Banus, Nico J. D. Nagelkerke, H. J. van Kranen, Barbara Hoebee, Frits R. Mooi, Tjeerd G. Kimman, and Peter Demant

Subjects
Genetic Markers, Bordetella pertussis, Genetic Linkage, Whooping Cough, Immunology, Congenic, Locus (genetics), Biology, Microbiology, Mice, Mice, Congenic, Genetic linkage, medicine, Animals, Genetic Predisposition to Disease, Lung, Gene, Chromosome 12, Whooping cough, Genetics, Chromosome Mapping, Bacterial Infections, biology.organism_classification, medicine.disease, Disease Models, Animal, Infectious Diseases, Genetic marker, Female, Parasitology, Lod Score
Abstract

Susceptibility to and severity of Bordetella pertussis infection in infants and children vary widely. The spectrum of clinical symptoms ranges from subclinical infection to mild disease, severe whooping cough, and death. The aims of this study were to examine genetic susceptibilities of mice to B. pertussis and to identify genetic loci in the mouse genome that are involved in susceptibility to B. pertussis infection. For this purpose we screened two sets of recombinant congenic strains (RCS) of mice, HcB and CcS, for differences in the numbers of bacteria in the lung 7 days after inoculation. For both CcS and in HcB mice, a wide range in numbers of bacteria in the lung was found, suggesting that the course of infection is under multigenic control. From both RCS sets of mice, we selected one strain to identify possible susceptibility loci in F 2 hybrid mice. The degree of lung colonization 7 days postinoculation in these F 2 mice was evaluated in relation to genetic markers by linkage analysis. We found three novel loci that are involved in the control of B. pertussis infection. One locus, designated B. pertussis susceptibility locus 1 ( Bps-1 ), was identified on chromosome 12. The presence of the C57BL/10 genome on this locus instead of the C3H genome significantly decreased the number of B. pertussis bacteria in the lung. Bps-1 has a dominant-positive effect on the clearance of B. pertussis from the lung. The function of most genes in this region is unknown. Two other loci, Bps-2 and Bps-3 , showed genetic interaction and are located on chromosomes 5 and 11. We aim to identify the gene(s) in these regions which modify susceptibility to B. pertussis .

Published
2005
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3. Smoking and the risk of prostate cancer in the European Prospective Investigation into Cancer and Nutrition

Author

Rudolf Kaaks, Kim Overvad, N. Larrañaga, Rosario Tumino, Paer Stattin, Antonio Agudo, Margareta Johansson, H. J. Van Kranen, Anders Bjartell, Anne Tjønneland, Antonia Trichopoulou, M-D Chirlaque, Domenico Palli, Hendriek C. Boshuizen, Jakob Linseisen, Aurelio Barricarte, H. B. Bueno-de-Mesquita, Elio Riboli, Pagona Lagiou, Dimitrios Trichopoulos, N. F. Johnsen, Heiner Boeing, Marc J. Gunter, Sabine Rohrmann, Vittorio Krogh, Tobias Pischon, David Ulmert, Fulvio Ricceri, Naomi E. Allen, Kay-Tee Khaw, Nicholas J. Wareham, M-J Sanchez, Birgit Teucher, Isabelle Romieux, Pietro Ferrari, Timothy J. Key, M. V. Argüelles Suárez, University of Zurich, and Rohrmann, S

Subjects
Male, Cancer Research, Nutrition and Disease, Epidemiology, Wiskundige en Statistische Methoden - Biometris, Prostate cancer, 0302 clinical medicine, Risk Factors, Surveys and Questionnaires, Voeding en Ziekte, follow-up, 1306 Cancer Research, Prospective Studies, Registries, 030212 general & internal medicine, Prospective cohort study, Smoking, Prostate Cancer, Cohort Study, Epic, Incidence, Incidence (epidemiology), cohort, Middle Aged, Prognosis, prostate cancer, 3. Good health, European Prospective Investigation into Cancer and Nutrition, Europe, Survival Rate, 030220 oncology & carcinogenesis, Cohort, 2730 Oncology, Life Sciences & Biomedicine, Cohort study, Adult, medicine.medical_specialty, recurrence, Nutritional Status, men, 610 Medicine & health, tobacco use, Risk Assessment, smoking, 03 medical and health sciences, Internal medicine, medicine, cohort study, Humans, ddc:610, Survival rate, Mathematical and Statistical Methods - Biometris, Gynecology, Science & Technology, health-professionals, prospective us, business.industry, cigarette-smoking, association, Prostatic Neoplasms, 10060 Epidemiology, Biostatistics and Prevention Institute (EBPI), medicine.disease, ONCOLOGY, mortality, business, EPIC, Follow-Up Studies
Abstract

Background:Smoking is not associated with prostate cancer incidence in most studies, but associations between smoking and fatal prostate cancer have been reported.Methods:During 1992 and 2000, lifestyle information was assessed via questionnaires and personal interview in a cohort of 145 112 European men. Until 2009, 4623 incident cases of prostate cancer were identified, including 1517 cases of low-grade, 396 cases of high grade, 1516 cases of localised, 808 cases of advanced disease, and 432 fatal cases. Multivariable Cox proportional hazards regression models were used to examine the association of smoking status, smoking intensity, and smoking duration with the risk of incident and fatal prostate cancer.Results:Compared with never smokers, current smokers had a reduced risk of prostate cancer (RR=0.90, 95% CI: 0.83-0.97), which was statistically significant for localised and low-grade disease, but not for advanced or high-grade disease. In contrast, heavy smokers (25+ cigarettes per day) and men who had smoked for a long time (40+ years) had a higher risk of prostate cancer death (RR=1.81, 95% CI: 1.11-2.93; RR=1.38, 95% CI: 1.01-1.87, respectively).Conclusion:The observation of an increased prostate cancer mortality among heavy smokers confirms the results of previous prospective studies.British Journal of Cancer advance online publication, 20 November 2012; doi:10.1038/bjc.2012.520www.bjcancer.com.

Published
2013
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4. Contribution of bi-allelic germline MUTYH mutations to early-onset and familial colorectal cancer and to low number of adenomatous polyps: case-series and literature review

Author

B. Jorritsma, Helga Westers, Renee C. Niessen, Carli M. J. Tops, H. J. van Kranen, Rolf H. Sijmons, C. L. E. Siezen, J. Varkevisser, Frederik J. Hes, Juul T. Wijnen, Alain Knopperts, R. C. Heine-Broring, Ellen Kampman, Maartje Nielsen, Yvonne J. Vos, Ethical, Legal, Social Issues in Genetics (ELSI), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Faculty of Psychology and Educational Sciences, Clinical sciences, and Medical Genetics

Subjects
Oncology, Male, Cancer Research, Nutrition and Disease, Colorectal cancer, gene-mutations, Gene mutation, Bioinformatics, Germline, DNA Glycosylases, Adenomatous Polyps, Familial, myh mutations, Voeding en Ziekte, Medicine, Genetics (clinical), Netherlands, medicine.diagnostic_test, Adenomatous Polyps/genetics, Middle Aged, Lynch syndrome, frequency, Female, Colorectal Neoplasms, Adult, MUTYH, medicine.medical_specialty, carriers, Bethesda criteria, Young Adult, Germline mutation, Internal medicine, Colorectal Neoplasms, Hereditary Nonpolyposis/genetics, Genetics, Humans, lynch-syndrome, Genetic Predisposition to Disease, consumption, Germ-Line Mutation, Molecular epidemiology Aetiology, screening and detection [NCEBP 1], Genetic testing, Aged, VLAG, colon, Young age, business.industry, Microsatellite instability, DNA Glycosylases/genetics, medicine.disease, Colorectal Neoplasms/genetics, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Mutation, identification, microsatellite instability, business, feasibility
Abstract

Item does not contain fulltext In the absence of a polyposis phenotype, colorectal cancer (CRC) patients referred for genetic testing because of early-onset disease and/or a positive family history, typically undergo testing for molecular signs of Lynch syndrome in their tumors. In the absence of these signs, DNA testing for germline mutations associated with other known tumor syndromes is usually not performed. However, a few studies in large series of CRC patients suggest that in a small percentage of CRC cases, bi-allelic MUTYH germline mutations can be found in the absence of the MUTYH-associated polyposis phenotype. This has not been studied in the Dutch population. Therefore, we analyzed the MUTYH gene for mutations in 89 patients with microsatellite-low or stable CRC cancer diagnosed before the age of 40 years or otherwise meeting the Bethesda criteria, all of them without a polyposis phenotype. In addition, we studied a series of 693 non-CRC patients with 1-13 adenomatous colorectal polyps for the MUTYH hotspot mutations Y179C, G396D and P405L. No bi-allelic MUTYH mutations were observed. Our data suggest that the contribution of bi-allelic MUTYH mutations to the development of CRC in Dutch non-polyposis patients that meet clinical genetic referral criteria, and to the development of low number of colorectal adenomas in non-CRC patients, is likely to be low.

Published
2013

5. Host Genetics of Bordetella pertussis Infection in Mice: Significance of Toll-Like Receptor 4 in Genetic Susceptibility and Pathobiology

Author

J. A. M. A. Dormans, H. de Ruiter, Frits R. Mooi, Rob J. Vandebriel, N. J. Nagelkerke, H. A. Banus, H. J. van Kranen, Tjeerd G. Kimman, and B. Hoebee

Subjects
Bordetella pertussis, Genetic Linkage, Whooping Cough, Immunology, Congenic, Microbiology, Mice, Inbred strain, Immunity, Genetic predisposition, medicine, Animals, Genetic Predisposition to Disease, Lung, Whooping cough, Host factor, Mice, Inbred BALB C, Mice, Inbred C3H, biology, Tumor Necrosis Factor-alpha, Bacterial Infections, biology.organism_classification, medicine.disease, Toll-Like Receptor 4, Infectious Diseases, TLR4, Cytokines, Parasitology
Abstract

The susceptibility to and the severity of Bordetella pertussis infections in infants and children varies widely, suggesting that genetic differences between individuals influence the course of infection. We have previously identified three novel loci that influence the severity of whooping cough by using recombinant congenic strains of mice: Bordetella pertussis susceptibility loci 1, 2, and 3 ( Bps1 , -2 , and -3 ). Because these loci could not account for all genetic differences between mice, we extended our search for additional susceptibility loci. We therefore screened 11 inbred strains of mice for susceptibility to a pertussis infection after intranasal infection. Susceptibility was defined by the number of bacteria in the lungs, being indicative of the effect between the clearance and replication of bacteria. The most resistant (A/J) and the most susceptible (C3H/HeJ) strains were selected for further genetic and phenotypic characterization. The link between bacterial clearance and chromosomal location was investigated with 300 F 2 mice, generated by crossing A/J and C3H/HeJ mice. We found a link between the delayed clearance of bacteria from the lung and a large part of chromosome 4 in F 2 mice with a maximum log of the odds score of 33.6 at 65.4 Mb, which is the location of Tlr4 . C3H/HeJ mice carry a functional mutation in the intracellular domain of Tlr4 . This locus accounted for all detectable genetic differences between these strains. Compared to A/J mice, C3H/HeJ mice showed a delayed clearance of bacteria from the lung, a higher relative lung weight, and increased body weight loss. Splenocytes from infected C3H/HeJ mice produced almost no interleukin-1β (IL-1β) and tumor necrosis factor alpha (TNF-α) upon ex vivo restimulation with B. pertussis compared to A/J mice and also showed a delayed gamma interferon (IFN-γ) production. TNF-α expression in the lungs 3 days after infection was increased fivefold compared to uninfected controls in A/J mice and was not affected in C3H/HeJ mice. In conclusion, Tlr4 is a major host factor explaining the differences in the course of infection between these inbred strains of mice. Functional Tlr4 is essential for an efficient IL-1-β, TNF-α, and IFN-γ response; efficient clearance of bacteria from the lung; and reduced lung pathology.

Published
2006

6. Tissue levels of fish fatty acids and risk of colorectal adenomas: a case-control study (Netherlands)

Author

M C, Busstra, C L E, Siezen, M J A L, Grubben, H J, van Kranen, F M, Nagengast, and P, van't Veer

Subjects
Adenoma, Adult, Male, Biopsy, Incidence, Fatty Acids, Fishes, Middle Aged, Dietary Fats, Diet, Adipose Tissue, Seafood, Case-Control Studies, Animals, Humans, Female, Tissue Distribution, Colorectal Neoplasms, Aged, Netherlands
Abstract

Epidemiological and animal studies have suggested that a high ratio of n-3 fish fatty acids to arachidonic acid (AA), might protect against colorectal carcinogenesis. Competition of n-3 and n-6 fatty acids, especially AA, for the enzyme cyclooxygenase-2 may be responsible for this effect. To examine the relation between fish intake and colorectal adenomas, data from a Dutch case-control study were analysed. All 52 cases and 57 controls filled out a food questionnaire, underwent a full colonic examination and have had a fat biopsy from the buttock. Intake of fish and fish fatty acids was inversely associated with colorectal adenomas although not statistically significant. For the ratio of fish fatty acids to AA, the ORs in the second and third tertile were 1.2 and 0.8 (p-trend = 0.78). Tissue levels of fish fatty acids were inversely associated and tissue levels of AA were positively associated with adenomas, although not statistically significant. However, the OR for the ratio of fish fatty acids to AA was 0.2 in the second and third tertile (p-trend = 0.002). In line with the hypothesis, a high ratio of fish fatty acids to AA in adipose tissue was associated with a lower risk of colorectal adenomas.

Published
2003

7. Early p53-positive foci as indicators of tumor risk in ultraviolet-exposed hairless mice: kinetics of induction, effects of DNA repair deficiency, and p53 heterozygosity

Author

H, Rebel, L O, Mosnier, R J, Berg, A, Westerman-de Vries, H, van Steeg, H J, van Kranen, and F R, de Gruijl

Subjects
Male, Mice, Knockout, Heterozygote, Mice, Hairless, Neoplasms, Radiation-Induced, Skin Neoplasms, DNA Repair, Ultraviolet Rays, RNA-Binding Proteins, Dose-Response Relationship, Radiation, Genes, p53, Xeroderma Pigmentosum Group A Protein, DNA-Binding Proteins, Kinetics, Mice, Risk Factors, Animals, Female, Tumor Suppressor Protein p53, Skin
Abstract

p53 mutations appear to be early events in skin carcinogenesis induced by chronic UVB irradiation. Clusters of epidermal cells that express p53 in mutant conformation ("p53 positive foci") are easily detected by immunohistochemical staining long before the appearance of skin carcinomas or their precursor lesions. In a hairless mouse model, we determined the dose-time dependency of the induction of these p53+ foci and investigated the relationship with the induction of skin carcinomas. The density of p53+ foci may be a good direct indicator of tumor risk. Hairless SKH1 mice were exposed to either of two regimens of daily UVB (500 or 250 J/m2 broadband UV from Philips TL12 lamps; 54% UVB 280-315 nm). With the high-dose regimen, the average number of p53+ foci in a dorsal skin area (7.2 cm2) increased rapidly from 9.0 +/- 2.1 (SE) at 15 days to 470 +/- 80 (SE) at 40 days. At half that daily dose, the induction of p53+ foci was slower by a factor of 1.49 +/- 0.15, very similar to a previously observed slower induction of squamous cell carcinomas by a factor of 1.54 +/- 0.02. In a double-log plot of the average number of p53 + foci versus time, the curves for the two exposure regimens ran parallel (slope, 3.7 +/- 0.7), similar to the curves for the number of tumors versus time (slope, 6.9 +/- 0.8). The difference in slopes (3.7 versus 6.9) is in line with the contention that more rate-limiting steps are needed to develop a tumor than a p53+ focus. By the time the first tumors appear (around 7-8 weeks with the high daily dose), the dorsal skin contains100 p53+ foci/cm2. To further validate the density of p53+ foci as a direct measure of tumor risk, we carried out experiments with transgenic mice with an enhanced susceptibility to UV carcinogenesis, homozygous Xpa knockout mice (deficient in nucleotide excision repair) and heterozygousp53 knockout mice (i.a. partially deficient in apoptosis). In both of these cancer-prone strains, the p53+ foci were induced at markedly increased rates, corresponding to increased rates of carcinoma formation. Therefore, the frequency of p53+ foci appears to correlate well with UVB-induced tumor risk.

Published
2001

8. Impact of global genome repair versus transcription-coupled repair on ultraviolet carcinogenesis in hairless mice

Author

R J, Berg, H, Rebel, G T, van der Horst, H J, van Kranen, L H, Mullenders, W A, van Vloten, and F R, de Gruijl

Subjects
Mice, Knockout, Mice, Hairless, Neoplasms, Radiation-Induced, Skin Neoplasms, Time Factors, DNA Repair, Papilloma, Transcription, Genetic, Ultraviolet Rays, Sunburn, Apoptosis, Exons, Parakeratosis, Mice, Mutation, Carcinoma, Squamous Cell, Animals, Epidermis
Abstract

The nucleotide excision repair (NER) system is comprised of two subpathways, i.e., transcription-coupled repair (TCR) and global genome repair (GGR). To establish the relative importance of TCR and GGR for UV effects on the skin, we have used hairless knockout mouse strain lacking either TCR (CSB -/-) or GGR (XPC -/-). In single exposure experiments, we found that CSB -/- mice have a 7-16 times higher susceptibility to sunburn than XPC -/- mice and than heterozygous (+/-) and wild-type (+/+) controls. Exposure to 80 J/m2 UV radiation (i.e., suberythemogenic in CSB -/-) on 10 consecutive days gives rise to epidermal hyperplasia in CSB -/- and XPC -/-, whereas repair-proficient controls do not show epidermal hyperplasia from these exposures. In addition, CSB -/- mice develop marked parakeratosis, whereas XPC -/- mice and controls do not. Under continued exposure to this daily dose, squamous cell carcinomas appear in CSB -/-, XPC -/-, and in the control groups, whereas only in the CSB -/- animals is a fairly high number of benign papillomas also found. The median latency time of squamous cell carcinomas (diametersor = 1 mm) is 84 days for the XPC -/- mice, 115 days for the CSB -/- mice, and 234-238 days for the heterozygous and wild-type control groups. These results indicate that GGR is more important than TCR in protection against UV-induced carcinomas of the skin but not against other UV effects such as sunburn, epidermal thickening, scaling of the stratum corneum, and development of papillomas. These results also indicate that GGR capacity may serve as a better predictor for skin cancer susceptibility than sensitivity to sunburn. The relative cancer susceptibilities of GGR- and TCR-deficient skin could well depend on the balance between an increased mutation rate and the presence (in CSB -/-) or lack (in XPC -/-) of a compensatory apoptotic response.

Published
2000

9. Balancing the risks and benefits of drinking water disinfection: disability adjusted life-years on the scale

Author

H J Van Kranen, A E De Hollander, J. F. M. Versteegh, Arie H. Havelaar, Peter Teunis, W Slob, J E Van Koten, and Evers Eg

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Health, Toxicology and Mutagenesis, Cost-Benefit Analysis, Population, Water supply, Cryptosporidiosis, Risk Assessment, Life Expectancy, Ozone, Water Supply, Environmental health, medicine, Animals, Humans, Disabled Persons, education, Child, Carcinoma, Renal Cell, Aged, Cryptosporidium parvum, education.field_of_study, Cost–benefit analysis, business.industry, Bromates, Risk of infection, Public health, Public Health, Environmental and Occupational Health, Infant, Newborn, Infant, Middle Aged, Kidney Neoplasms, Surgery, Quality-adjusted life year, Disinfection, Child, Preschool, Life expectancy, Female, Public Health, Quality-Adjusted Life Years, Risk assessment, business, Research Article
Abstract

To evaluate the applicability of disability adjusted life-years (DALYs) as a measure to compare positive and negative health effects of drinking water disinfection, we conducted a case study involving a hypothetical drinking water supply from surface water. This drinking water supply is typical in The Netherlands. We compared the reduction of the risk of infection with Cryptosporidium parvum by ozonation of water to the concomitant increase in risk of renal cell cancer arising from the production of bromate. We applied clinical, epidemiologic, and toxicologic data on morbidity and mortality to calculate the net health benefit in DALYs. We estimated the median risk of infection with C. parvum as 10(-3)/person-year. Ozonation reduces the median risk in the baseline approximately 7-fold, but bromate is produced in a concentration above current guideline levels. However, the health benefits of preventing gastroenteritis in the general population and premature death in patients with acquired immunodeficiency syndrome outweigh health losses by premature death from renal cell cancer by a factor of > 10. The net benefit is approximately 1 DALY/million person-years. The application of DALYs in principle allows us to more explicitly compare the public health risks and benefits of different management options. In practice, the application of DALYs may be hampered by the substantial degree of uncertainty, as is typical for risk assessment. Images Figure 1 Figure 2 Figure 3 Figure 4 Figure 5 Figure 6 Figure 7

Published
2000

10. Low incidence of p53 mutations in UVA (365-nm)-induced skin tumors in hairless mice

Author

H J, van Kranen, A, de Laat, J, van de Ven, P W, Wester, A, de Vries, R J, Berg, C F, van Kreijl, and F R, de Gruijl

Subjects
Male, Neoplasms, Radiation-Induced, Skin Neoplasms, Papilloma, Ultraviolet Rays, DNA Mutational Analysis, Mice, Inbred Strains, Genes, p53, Immunohistochemistry, Mice, Mutation, Carcinoma, Squamous Cell, Animals, Female
Abstract

Mutations with clear "UVB fingerprints" have been observed in the p53 gene of human nonmelanoma skin tumors and of experimentally UVB-induced murine skin tumors. Although UVA (315-400 nm) radiation is also a complete carcinogen, its contribution to sunlight-induced mutagenesis remains poorly characterized. There is experimental evidence that the production of reactive oxygen species plays a more dominant role with long-wave UVA than with UVB radiation. We have induced skin tumors (n = 42) in hairless SKH:HR1 mice (n = 14) by daily exposure to long-wave UVA (365-nm) radiation. The incidence of p53 alterations in these tumors is low compared to UVB-induced tumors; positive staining for the p53 protein was observed in only 50% of the tumors, and less than 15% of the tumors showed a mutation in one of the exons 5, 7, or 8 of the p53 gene. The pattern of p53 staining was more irregular and less dense compared to UVB, and the mutations (all C--T) were mainly (six of seven) located at codon 267. Besides a general p53 hotspot, this codon is also the main hotspot for UVB-induced skin tumors in these mice. No mutations specific for UVA, ie., mutations specific for reactive oxygen species, could be detected.

Published
1997

11. Chromosomal localization of the rat N-ras protooncogene by fluorescence in situ hybridization

Author

J M, de Stoppelaar, R F, Suijkerbuijk, H J, van Kranen, P, Faessen, G R, Mohn, and B, Hoebee

Subjects
Genes, ras, Restriction Mapping, Animals, Chromosome Mapping, Rats, Wistar, In Situ Hybridization, Fluorescence, Rats
Abstract

The rat N-ras protooncogene has been assigned to chromosome 2q34 by fluorescence in situ hybridization on rat metaphase chromosomes. This was accomplished using two recently isolated genomic clones with a length of 8.2 and 4.1 kb.

Published
1994

12. Absract

Author

Marietta Kaszkin, Volker Kinzel, Karl Maly, Irina Bichler, Florian Lang, Hans H. Grunicke, R. Pepperkok, R. Jakobi, P. Lorenz, W. Ansorge, W. Pyerin, P. Borowski, M. Harbers, A. Ludwig, T. Kischel, H. Hilz, K. Eckert, A. Granetzny, J. Fischer, R. Grosse, V. Manch, S. Wehner, B. Kornhuber, U. Ebener, K. Müller-Decker, G. Fürstenberger, I. Vogt, F. Marks, G. Graschew, A. Küsel, W. Hull, W. Lorenz, H. W. Thielmann, Gisela H. Degen, Alexius Freyberger, A. Müller, M. Linscheid, Ulrike Hindermeier, Ute Jorritsma, K. Golka, W. Föllmann, H. Peter, H. M. Bolt, S. Monnerjahn, D. N. Phillips, A. Never, A. Seidel, A. R. Glatt, K. Wiench, E. Frei, P. Schroth, M. Wiessler, T. Schäfer, M. Hergenhahn, E. Hecker, D. Proft, P. Bartholmes, R. S. Bagewadikar, B. Bertram, N. Frank, Hanno Leibersperger, Michael Gschwendt, Friedrich Marks, S. Fasco, Peter Plein, Karin Schiess, Lothar Seidler, T. Jacobi, E. Besemfelder, M. Stephan, W. D. Lehmann, M. Grell, B. Thoma, P. Scheurich, Markus Meyer, Hans Grunicke, G. Jaques, B. Wegmann, K. Ravemann, Odilia Popanda, Heinz Walter Thielmann, H. Voss, U. Wirkner, Dieter Werner, D. Strand, A. Kalmes, H. -P. Walther, B. Mechler, S. Volker Schirrmacher, V. Kinzel, R. Hess, H. -G. Hanagarth, C. Hässler, G. Brandner, Christian Ertel, B. Gückel, V. Schirrmacher, B. A. Kyewski, U. Bogdahn, P. Jachimczak, J. Schneider, W. Brysch, W. Schlingensiepen, D. Drenkard, C. Behl, J. Winkler, R. Apfel, J. Meixensberger, K. Stulle, P. Marquardt, H. P. Vollmers, J. Müller, H. -K. Müller-Hermelink, M. Schuermann, G. Seemann, Angelika Ptok, M. Ptok, T. E. Carey, M. Steffen, U. C. Nitz, B. Everding, F. Hölzel, G. Kantwerk-Funke, G. Boll, K. S. Zänker, P. Hölzel, J. Heymanns, C. Hennig, M. Rotsch, K. Havemann, Jürgen R. Fischer, Sabine Stehr, Harald Lahm, Peter Drings, Peter H. Krammer, M. Kirsch, A. Strubel, A. Kist, R. Hinn, H. Fischer, A. Buttler, G. Schackert, S. Friedenauer, D. Lindner, B. Marczynski, H. Karcls, H. W. Goergens, B. Epe, E. Müller, D. Schütze, S. Boiteux, E. Eder, C. Deininger, C. Hoffman, E. Scherer, E. Vermeulen, H. J. van Kranen, J. Bax, R. A. Woutersen, C. F. van Kreijl, B. Schurich, H. Hagedorn, E. Kamp, G. Eisenbrand, B. Spiegelhalder, U. Bolm-Audorff, H. G. Bienfait, R. Preussmann, C. -D. Wacker, H. Kehl, Z. Akkan, J. Ries, M. Meger, S. E. Shephard, D. Gunz, W. K. Lutz, A. R. Tricker, R. Kurnar, M. Siddiqi, P. Mende, B. Pfundstein, A. Scholl, C. Janzowski, D. Jacob, P. Goelzer, I. Henn, H. Zankl, K. -H. Zimlich, Barbara Gansewendt, Ricarda Thier, K. R. Schroeder, E. Hallier, G. Moeckel, W. Heiden, M. Waldherr-Teschner, J. Brickmann, H. Roeser, G. Krauter, G. Scherer, A. Krätschmer, H. Hauenstein, F. Adlkofer, R. C. Fernando, H. H. Schmeiser, W. Nicklas, Wolfgang Pfau, David H. Phillips, S. Scheckenbach, S. Cantoreggi, Monika Leutbecher, H. Ottenwälder, U. Föst, P. M. Baumgart, H. -C. Kliem, S. Data, C. Pfeiffer, A. Fuchs, P. Schmezer, F. Kuchenmeister, B. L. Pool-Zober, U. M. Liegibel, B. L. Pool-Zobel, L. Steeb, H. Friesel, Th. Schneider, H. R. Scherf, A. Buchmann, R. Bauer-Hofmann, J. Mahr, M. Schwarz, R. Schmidt, F. Rippmann, B. Steinbauer, P. Zlfu, B. Bunk, W. Hefter, K. Klinga, M. R. Berger, L. W. Robertson, G. Luebeck, S. Moolgavkar, U. Torsten, M. Kowalczyk-Wagner, H. Weitzel, Ch. Zechel, H. Peters, F. Anders, S. Ambs, T. Kirchner, H. -G. Neumann, C. Einig, E. Eigenbrodt, D. Oesterle, E. Deml, G. Weisse, U. Gerbracht, H. Stumpf, E. Filsingcr, P. Bannasch, W. Muster, P. Cikryt, P. Münzel, E. Röhrdanz, K. W. Bock, H. -P. Lipp, T. Wiesmüller, H. Hagenmaier, D. Schrenk, A. Karger, G. Bauer, P. Höfler, M. Götschl, E. Viesel, J. Jürgensmeier, D. Schaefer, G. Picht, J. Kiefer, P. Krieg, R. Schnapke, S. Feil, E. Wagner, U. Schleenbecker, A. Anders, M. M. Gross, S. Unger, E. J. Stanbridge, Petra Boukamp, Ulrich Pascheberg, Norbert E. Fusenig, H. Abken, U. H. Weidle, F. Grummt, K. Willecke, R. Schäfer, A. Hajnal, I. Balmer, R. Klemenz, P. E. Goretzki, H. 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Subjects
Cancer Research, Oncology, General Medicine
Published
1991
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