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1

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DNA methylation in various rat tissues by the esophageal carcinogen N-nitrosomethyl-n-amylamine and six of its positional isomers (1991)

Ji, Chuan ; Ludeke, Barbara I. ; Kleihues, Paul ; [et al.]

s.l. : American Chemical Society

Chemical research in toxicology 4 (1991), S. 77-81

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ISSN: 1520-5010

Source: ACS Legacy Archives

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1021/tx00019a010

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2

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Regionally Selective Inhibition of Cerebral Protein Synthesis in the Rat During Hypoglycemia and Recovery (1984)

Kiessling, Marika ; Xie, Yaxia ; Kleihues, Paul

Oxford, UK : Blackwell Publishing Ltd

Journal of neurochemistry 43 (1984), S. 0

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ISSN: 1471-4159

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: Regional cerebral protein synthesis was investigated in anesthetized, mechanically ventilated rats during progressive insulin-induced hypoglycemia and the recovery period following glucose infusion. Polysome profiles from precomatose animals with slow wave/polyspike EEG revealed a slight reduction of polyribosomes and a concurrent increase in monoribosomes, but autoradiographs showed a pattern of l-[3-3H]tyrosine incorporation indistinguishable from that of control rats. During the initial 30 min of insulin-induced isoelectric EEG (“coma”), autoradiographs showed a selective inhibition of protein synthesis in neurons and glial cells of the hippocampus and cerebral cortex, i.e., regions with high susceptibility for the development of hypoglycemic brain damage. Basal ganglia were less affected and areas with low vulnerability (hypothalamus, brainstem, and cerebellum) exhibited a normal pattern of amino acid incorporation. Using a flooding dose of l-[1-14C]valine (7.5 mmol/kg; 15 μCi/mmol), the rate of incorporation in cerebral cortex and cerebellum was found to be reduced to 2% and 80% of control values, respectively. Inhibition of protein synthesis was paralleled by a breakdown of polyribosomes and a concomitant increase in ribosomal subunits, indicating a block in peptide chain initiation. After 90 min of isoelectric EEG all brain structures with the exception of hypothalamus and area postrema showed an almost complete lack of amino acid incorporation. Glucose infusion after a 30-min period of hypoglycemic coma led to a partial restoration of cortical and hippocampal protein synthesis. Within 70–90 min of recovery, l-[1-14C]valine incorporation into neocortical and cerebellar proteins amounted to 47% and 125% of fasted controls. The very specialized patterns of regional impairment of cerebral protein synthesis during progressive hypoglycemia may reflect a selective vulnerability of some neuronal cell populations to hypoglycemic cell injury. Alternatively, the striking resistance of hypothalamus, brainstem, and cerebellum may be due to a more efficient glucose uptake at very low blood glucose levels.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1471-4159.1984.tb06070.x

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3

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DNA MODIFICATION AND REPAIR IN THE EXPERIMENTAL INDUCTION OF NERVOUS SYSTEM TUMORS BY CHEMICAL CARCINOGENS (1982)

Kleihues, Paul ; Patzschke, Karl ; Doerjer, Gerhard

Oxford, UK : Blackwell Publishing Ltd

Annals of the New York Academy of Sciences 381 (1982), S. 0

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ISSN: 1749-6632

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Natural Sciences in General

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1749-6632.1982.tb50393.x

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4

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Exhaustion and recovery of repair excision of O 6 -methylguanine from rat liver DNA (1976)

KLEIHUES, PAUL ; MARGISON, GEOFFREY P.

[s.l.] : Nature Publishing Group

Nature 259 (1976), S. 153-155

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ISSN: 1476-4687

Source: Nature Archives 1869 - 2009

Topics: Biology , Chemistry and Pharmacology , Medicine , Natural Sciences in General , Physics

Notes: [Auszug] In all experiments, female BD-1X rats (110-140 g) received an intravenous injection of lOmgkg"1 3H-MNU and were killed 6 h later. Liver DNA was isolated and purine bases were separated by Sephadex G-10 chromato-graphy of the acid hydrolysate11. After injection of 3H-MNU alone O6-3H-meG present in ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/259153a0

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5

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Single-dose toxicokinetics ofN-nitrosomethylethylamine andN-nitrosomethyl (2,2,2-trideuterioethyl)amine in the rat (1990)

Streeter, Anthony J. ; Nims, Raymond W. ; Anderson, Lucy M. ; [et al.]

Springer

Archives of toxicology 64 (1990), S. 109-115

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ISSN: 1432-0738

Keywords: N-Nitrosomethylethylamine ; Deuterium isotope effect ; N-Nitrosomethyl(2,2,2-trideuterioethyl)amine ; Toxicokinetics ; Rat

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract To investigate the origins of an organotropic shift toward increasing esophageal carcinogenicity and DNA alkylation caused by β-trideuteration of the hepatocarcinogen,N-nitrosomethylethylamine (NMEA), the single-dose toxicokinetics of NMEA andN-nitrosomethyl(2,2,2-trideuterioethyl)amine (NMEA-d 3) has been characterized in 8-week-old male Fischer 344 rats by analysis using high performance liquid chromatography of serial blood samples. An i.v. bolus dose of 0.6 μmol/kg to rats revealed biphasic first order elimination with a terminal half-life of 9.46 ± 0.69 min for unchanged NMEA and 28.9 ± 2.4 min for total radioactivity. Extensive conversion to polar metabolites was observed in the chromatograms. The systemic blood clearance and apparent steadystate volume of distribution for unchanged NMEA were 39.9 ± 4.6 ml/min/kg and 496 ± 36 ml/kg, respectively. There was negligible plasma protein binding and no detectable NMEA was excreted unchanged in the urine. Larger doses given by gavage indicated a systemic bioavailability of 25 ± 1%. Similar doses of NMEA-d 3 given to other groups of rats revealed no significant differences in any of the toxicokinetic parameters. NoN-nitrosomethyl (2-hydroxyethyl)amine was found as a detectable metabolite of NMEA or NMEA-d 3 in any of the blood or urine samples which were analyzed. When considered together, the data suggest that previously observed differences in organ specificity for the carcinogens, NMEA and NMEA-d 3, are not due to differences in the total amounts of nitrosamine reaching particular tissues, but may have other localized causes such as differences in the enzymes responsible for metabolism which are present in each tissue. Such differences may make too small a contribution to the total systemic clearance to be detectable in that parameter, but at the level of the fraction of a dose that alkylates DNA they may be important.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01974395

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6

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Preferential expression of Fas/APO1 (CD95) and apoptotic cell death in perinecrotic cells of glioblastoma multiforme (1996)

Tachibana, Osamu ; Lampe, Johannes ; Kleihues, Paul ; [et al.]

Springer

Acta neuropathologica 92 (1996), S. 431-434

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ISSN: 1432-0533

Keywords: Key words Fas ; Glioblastoma ; Astrocytoma ; Apoptosis ; Necrosis

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Fas/APO-1 (CD95)-mediated apoptosis is one of the major mechanisms of programmed cell death. We have previously shown by reverse transcriptase-polymerase chain reaction that Fas is frequently expressed in malignant gliomas [Tachibana et al. (1995) Cancer Res 55: 5528–5530]. In this study, we assessed Fas expression in astrocytomas using a polyclonal anti-Fas antibody. Immunoreactivity to Fas was detected in 1 out of 9 (11%) low-grade astrocytomas (WHO grade II), 2 of 11 (18%) anaplastic astrocytomas (WHO grade III) and in 13 of 15 (87%) glioblastomas (WHO grade IV). In glioblastomas, Fas expression was almost exclusively observed in glioma cells surrounding foci of necrosis. In these perinecrotic areas, there was also an accumulation of glioma cells undergoing apoptosis, as detected by in situ nick-end labeling. This suggests that Fas-mediated apoptosis may play a role in the pathogenesis of necrosis which constitutes a histological hallmark of glioblastoma multiforme.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s004010050542

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7

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p53 and PTEN gene mutations in gemistocytic astrocytomas (1998)

Watanabe, Kunihiko ; Peraud, Aurelia ; Gratas, Catherine ; [et al.]

Springer

Acta neuropathologica 95 (1998), S. 559-564

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ISSN: 1432-0533

Keywords: Key wordsPTEN mutation ; p53 mutation ; Gemistocytic astrocytoma

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The gemistocytic astrocytoma is a histological variant of diffuse astrocytomas and is characterised by the presence of large, GFAP-expressing neoplastic astrocytes (gemistocytes) and a tendency towards rapid progression to glioblastoma. In this study, we analyzed 28 gemistocytic astrocytomas (mean fraction of gemistocytes, 35.0 ± 9.9%) for mutations in the p53 and PTEN (MMAC1) tumour suppressor genes. Single strand conformation polymorphism (SSCP), followed by direct DNA sequencing of p53 exons 5–8, revealed a mutation in 23 of 28 (82%) cases. Regional analysis of four tumours revealed identical p53 mutations in gemistocytic and fibrillary tumour areas. In contrast, none of 15 gemistocytic astrocytomas (WHO Grade II) and only two of 11 (18%) anaplastic gemistocytic astrocytomas (WHO Grade III) contained a PTEN mutation. Of these, one was a 1 bp deletion in codon 345 and the other a 1 bp insertion in intron 4. Differential PCR did not reveal homozygous PTEN deletion in any of the tumours analysed. These results indicate that p53 mutations are a genetic hallmark of gemistocytic astrocytomas, whilst PTEN mutations are absent in low-grade and rare in anaplastic gemistocytic astrocytomas.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s004010050840

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8

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Long-term persistence of O 6 -methylguanine in rat brain DNA (1977)

KLEIHUES, PAUL ; BUCHELER, JOACHIM

[s.l.] : Nature Publishing Group

Nature 269 (1977), S. 625-626

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ISSN: 1476-4687

Source: Nature Archives 1869 - 2009

Topics: Biology , Chemistry and Pharmacology , Medicine , Natural Sciences in General , Physics

Notes: [Auszug] Adult female BD-IX rats (100-120 g) received a single intravenous injection of N- [3H] -methyl-N-nitrosourea (25.5 mCi mmol"1) at a dose of 10 mg per kg body weight. After time intervals ranging from 4h to 184 d, DNA was isolated by phenol extraction11 from the combined organs of two animals. ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/269625a0

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9

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Human astrocytic brain tumors express APO2L/TRAIL (1999)

Rieger, Johannes ; Ohgaki, Hiroko ; Kleihues, Paul ; [et al.]

Springer

Acta neuropathologica 97 (1999), S. 1-4

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ISSN: 1432-0533

Keywords: Key words APO2 ligand ; CD95 ligand ; Glioma

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract APO2 ligand (APO2L) is a CD95 ligand (CD95L)-related cytokine of the tumor necrosis factor family that interacts with agonistic (DR4, DR5) and antagonistic (DcR1, DcR2) receptors. Cultured malignant glioma cells preferentially express agonistic receptors and are susceptible to APO2L-induced apoptosis. Here, we report that 8 of 8 human glioma cell lines expressed APO2L mRNA and protein in vitro. Immunohistochemistry using a monoclonal antibody to APO2L revealed that all 23 primary astrocytic brain tumors analyzed, including low-grade astrocytomas and glioblastomas, express APO2L in vivo. With the exception of reactive astrocytes, non-neoplastic glia and neurons in the cerebrum lacked immunoreactivity of APO2L. Thus, in addition to the CD95/CD95L system, a second death ligand/death receptor pair may regulate susceptibility to apoptosis in human glial neoplasms.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s004010050948

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10

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Tumor induction by ras and myc oncogenes in fetal and neonatal brain: modulating effects of developmental stage and retroviral dose (1993)

Radner, Herbert ; El-Shabrawi, Yosuf ; Eibl, Robert H. ; [et al.]

Springer

Acta neuropathologica 86 (1993), S. 456-465

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ISSN: 1432-0533

Keywords: Retroviral vectors ; Oncogene-ras-myc ; Grafting ; Brain tumors

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Introduction into fetal rat brain cells of a replication-defective retroviral vector harboring v-Ha-ras and v-gag-myc rapidly causes the induction of highly malignant undifferentiated neuroectodermal tumors following transplantation into the brains of syngeneic hosts [Wiestler, et al. (1992) Cancer Res. 52: 3760–3767]. In the present study, we have investigated the modulating effect of the developmental stage of neural target cells and of the dose of the retroviral vector used in the grafting experiments. Exposure of fetal cells from embryonic day (E)12 or E14 produced a 100% incidence of malignant neuroectodermal tumors which led to the death of recipient animals after a median latency period of 32 days. A 100-fold reduction of the virus dose from 2.062×106 to 2.062×104 focus-forming units/ml resulted in a lower tumor incidence of 25%. Of six neural grafts exposed to v-Ha-ras and v-myc at E16, only one showed evidence of tumorigenesis (low-grade astrocytoma and hemangioma). All other transplants were morphologically normal for observation periods of 26 weeks, indicating a marked loss of transforming activity of ras and myc in more advanced stages of brain development. In retrovirus-exposed donor cells which caused the development of neural tumors in recipient rats, malignant transformation was also evident during culture in vitro, usually after 9–12 days. Oncogene complementation was also studied in the newborn rat brain. After microinjection of the retroviral vector into the brain at postnatal day (P)0, P1 and P3, 5 out of 20 animals (25%) developed a total of seven brain tumors. Histopathologically, three of these neoplasms were malignant neuroectodermal tumors which, in contrast to those induced in fetal brain transplants showed evidence of focal glial and/or neuronal differentiation. In addition, we observed one oligodendroglioma, two hemangiomas and a malignant hemangioendothelioma. These data indicate that neural precursor cells and endothelia of the rat brain represent the major target cells for the complementary action of ras and myc and that the use of target cells from later developmental stages (E16 and postnatal) leads to the induction of both primitive and more differentiated neoplasms.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00228580

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