The effect of copper deficiency and toxicity on the tumor suppressor protein p53

Tassabehji, Nadine M. Levenson, Cathy W.

January 2003

Thesis (M.S.)--Florida State University, 2003. / Advisor: Dr. Cathy Levenson, Florida State University, College of Human Sciences, Dept. of Nutrition, Food and Exercise Sciences. Title and description from dissertation home page (viewed 5/4/04). Includes bibliographical references.

Cancer cells Copper p53 protein.

Mammalian Reovirus Infection Changes the Expression of Bcl-xL Protein in H1299 Cell Line Independent of p53

Wang, Lou

22 September 2010

Mammalian reovirus (MRV) is a prototype virus of Reoviridae family. MRV virions are composed of two concentric protein capsids that surround a genome of 10 segments of dsRNA. It has been shown that MRV can manipulate host gene expression and further induce apoptosis and cell cycle arrest in various cell lines. However, the detailed molecular mechanisms by which MRV regulates the expression of host cells are largely unknown. P53 is an important transcriptional factor which modulates the expression of more than 130 genes controlled in cell stress-response. We aimed to examine the molecular mechanisms underlying the effect of MRV infection on the expression of host genes and the possible role of p53 in the interaction of MRV and host cells. Prototype serotype 3 reovirus strain Dearing (T3D) and serotype 1 strain Lang (T1L) were used to infect different cell lines, respectively, H1299 (p53-null and p53 positive), HT1080 (p53 mutant and p53 positive) and HCT116 (p21 deficient and 14-3-3σ deficient). By comparing the virus replication curve of T1L and T3D in these cell lines, we found that MRV can replicate with a similar pattern in both p53-defective and p53-positive cell lines which indicated that p53 does not have significant impact on MRV replication in these cell lines. We further found that the level of Bcl-xL protein, which has been shown to be able to inhibit apoptosis, was increased in H1299 cell lines (both p53-null and p53 positive) infected by T3D, but decreased in the same cell lines infected by T1L. A similar change of Bcl-xL protein was not observed In HCT116 and HT1080 cell lines with MRV infection. Fifty four T1L×T3D reassortants were used to map which gene or gene combination was responsible for the changes of Bcl-xL protein. We found that the expression of Bcl-xL protein in H1299 cell line infected by MRV was majorly controlled by the S1 gene segment which encodes the σ1 cell attachment protein and the σ1s non structural protein, while minorly controlled by L3 gene segment of MRV.

Reovirus

Bcl-xL

p53

H1299

Mammalian Reovirus Infection Changes the Expression of Bcl-xL Protein in H1299 Cell Line Independent of p53

Wang, Lou

22 September 2010

Mammalian reovirus (MRV) is a prototype virus of Reoviridae family. MRV virions are composed of two concentric protein capsids that surround a genome of 10 segments of dsRNA. It has been shown that MRV can manipulate host gene expression and further induce apoptosis and cell cycle arrest in various cell lines. However, the detailed molecular mechanisms by which MRV regulates the expression of host cells are largely unknown. P53 is an important transcriptional factor which modulates the expression of more than 130 genes controlled in cell stress-response. We aimed to examine the molecular mechanisms underlying the effect of MRV infection on the expression of host genes and the possible role of p53 in the interaction of MRV and host cells. Prototype serotype 3 reovirus strain Dearing (T3D) and serotype 1 strain Lang (T1L) were used to infect different cell lines, respectively, H1299 (p53-null and p53 positive), HT1080 (p53 mutant and p53 positive) and HCT116 (p21 deficient and 14-3-3σ deficient). By comparing the virus replication curve of T1L and T3D in these cell lines, we found that MRV can replicate with a similar pattern in both p53-defective and p53-positive cell lines which indicated that p53 does not have significant impact on MRV replication in these cell lines. We further found that the level of Bcl-xL protein, which has been shown to be able to inhibit apoptosis, was increased in H1299 cell lines (both p53-null and p53 positive) infected by T3D, but decreased in the same cell lines infected by T1L. A similar change of Bcl-xL protein was not observed In HCT116 and HT1080 cell lines with MRV infection. Fifty four T1L×T3D reassortants were used to map which gene or gene combination was responsible for the changes of Bcl-xL protein. We found that the expression of Bcl-xL protein in H1299 cell line infected by MRV was majorly controlled by the S1 gene segment which encodes the σ1 cell attachment protein and the σ1s non structural protein, while minorly controlled by L3 gene segment of MRV.

Reovirus

Bcl-xL

p53

H1299

Immunophenotypic and molecular approaches to the classification of diffuse large B cell lymphoma

Barrans, Sharon Louise

January 2001

No description available.

572.8

BCL6; BCL2; P53; FISH

Untersuchungen zur Expression p53-regulierter Gene nach Reduktion der zellulären Level des INHAT-Repressors NIR mittels RNA- Interferenztechnologie /

Dubois, Nicole.

January 2007

Zugl: Giessen, Universiẗat, Diss., 2007.

Untersuchungen zur Expression p53-regulierter Gene nach Reduktion der zellulären Level des INHAT-Repressors NIR mittels RNA-Interferenztechnologie

Dubois, Nicole

January 1900

Zugl.: Giessen, Univ., Diss., 2007

Ein Polymorphismus im Intron 3 des p53-Gens und erhöhtes Risiko für Ovarialkarzinom

Herzog, Raimund Ingo,

January 1998

Ulm, Univ., Diss., 1998.

Inhibition of human papilloma virus E6 oncogene function by mammalian lignans activates the p53 tumor suppressor protein and induces apoptosis in cervical cancer cells

Awad, Keytam Salem.

January 2007

Thesis (Ph.D.)--Kent State University, 2007. / Title from PDF t.p. (viewed July 8, 2009). Advisor: Angelo L. DeLucia. Keywords: human papilloma virus, mammalian lignans, p53, E6 oncogene. Includes bibliographical references (p. 133-149).

Untersuchungen zur Expression p53-regulierter Gene nach Reduktion der zellulären Level des INHAT Repressors NIR mittels RNA- Interferenztechnologie

Dubois, Nicole.

January 2007

Universiẗat, Diss., 2007--Giessen.

Biochemische Untersuchungen zur Rolle des Tumorsuppressorproteins P53 bei der Replikation und Reparatur der DNA

Hartmann, Hella.

Unknown Date

Universiẗat, Diss., 2001--Jena.

DNS-Reparatur. Replikation. Protein p53.