Title : p53 Mediated regulation of smar1 and their coordinated role in tumorigenesis through modulation of nfκb and tgfβ target gene expression

Bibliographic Details
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Type of Material:	Thesis
Title:	p53 Mediated regulation of smar1 and their coordinated role in tumorigenesis through modulation of nfκb and tgfβ target gene expression
Researcher:	Singh, Kamini
Guide:	Chattopadhyay, Samit
Department:	National Centre for Cell Science
Publisher:	Savitribai Phule Pune University
Place:	Pune
Year:	June 2007
Language:	English
Subject:	Nuclear matrix
Subject:	Tumorigenesis
Dissertation/Thesis Note:	PhD
Fulltext:	Shodhganga

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001 447305
003 IN-AhILN
005 2023-07-07 13:54:16
008 __ 230707t2007||||ii#||||g|m||||||||||eng||
035 __ |a(IN-AhILN)th_447305
040 __ |aPUNE_411007|dIN-AhILN
041 __ |aeng
100 __ |aSingh, Kamini|eResearcher
110 __ |aNational Centre for Cell Science|bSavitribai Phule Pune University|dPune|ein
245 __ |ap53 Mediated regulation of smar1 and their coordinated role in tumorigenesis through modulation of nfκb and tgfβ target gene expression
260 __ |aPune|bSavitribai Phule Pune University|cJune 2007
300 __ |a153p.|dDVD
500 __ |aBibliography p.130-150
502 __ |bPhD
520 __ |aNuclear matrix and matrix binding proteins play important role in regulating various cellular processes. Association of Matrix Attachment Regions (MARs) with Matrix Attachment Region Binding Proteins (MARBPs) maintains the chromatin architecture and matrix topology. Altered chromatin structure and function is observed during tumorigenesis due to dysregulation of MARBPs. SMAR1 is initially identified from T-cell and is been characterized as a MARBP Smar1 gene is present at 16q24.3 locus and its tumor suppressor role is recently been highlighted. SMAR1 is also established as negative regulator of transcription at TCRβ locus and Cyclin D1 promoter. The present study focuses on understanding the mechanism of SMAR1 regulation and its in depth role in regulating the transcription and signaling pathways pertinent to breast cancer. Our study shows that SMAR1 transcription is directly regulated by another tumor suppressor MARBP, p53 upon DNA damage through its response element. Further in human breast cancer sample
653 __ |aNuclear matrix
653 __ |aTumorigenesis
700 __ |aChattopadhyay, Samit|eGuide
856 __ |uhttp://shodhganga.inflibnet.ac.in/handle/10603/2454|yShodhganga
905 __ |afromsg

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000	00000ntm a2200000ua 4500
001	447305
003	IN-AhILN
005	2023-07-07 13:54:16
008	__	230707t2007\|\|\|\|ii#\|\|\|\|g\|m\|\|\|\|\|\|\|\|\|\|eng\|\|
035	__	\|a(IN-AhILN)th_447305
040	__	\|aPUNE_411007\|dIN-AhILN
041	__	\|aeng
100	__	\|aSingh, Kamini\|eResearcher
110	__	\|aNational Centre for Cell Science\|bSavitribai Phule Pune University\|dPune\|ein
245	__	\|ap53 Mediated regulation of smar1 and their coordinated role in tumorigenesis through modulation of nfκb and tgfβ target gene expression
260	__	\|aPune\|bSavitribai Phule Pune University\|cJune 2007
300	__	\|a153p.\|dDVD
500	__	\|aBibliography p.130-150
502	__	\|bPhD
520	__	\|aNuclear matrix and matrix binding proteins play important role in regulating various cellular processes. Association of Matrix Attachment Regions (MARs) with Matrix Attachment Region Binding Proteins (MARBPs) maintains the chromatin architecture and matrix topology. Altered chromatin structure and function is observed during tumorigenesis due to dysregulation of MARBPs. SMAR1 is initially identified from T-cell and is been characterized as a MARBP Smar1 gene is present at 16q24.3 locus and its tumor suppressor role is recently been highlighted. SMAR1 is also established as negative regulator of transcription at TCRβ locus and Cyclin D1 promoter. The present study focuses on understanding the mechanism of SMAR1 regulation and its in depth role in regulating the transcription and signaling pathways pertinent to breast cancer. Our study shows that SMAR1 transcription is directly regulated by another tumor suppressor MARBP, p53 upon DNA damage through its response element. Further in human breast cancer sample
653	__	\|aNuclear matrix
653	__	\|aTumorigenesis
700	__	\|aChattopadhyay, Samit\|eGuide
856	__	\|uhttp://shodhganga.inflibnet.ac.in/handle/10603/2454\|yShodhganga
905	__	\|afromsg