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• W56784355 endingPage "3747" @default.
• W56784355 startingPage "3737" @default.
• W56784355 abstract "Abstract Fanconi anemia (FA) is an autosomal recessive cancer susceptibility syndrome. The phenotype includes developmental defects, bone marrow failure, and cell cycle abnormalities. At least eight complementation groups (A-H) exist, and although three of the corresponding complementation group genes have been cloned, they lack recognizable motifs, and their functions are unknown. We have isolated a binding partner for the Fanconi anemia group C protein (FANCC) by yeast two-hybrid screening. We show that the novel gene, FAZF, encodes a 486 amino acid protein containing a conserved amino terminal BTB/POZ protein interaction domain and three C-terminal Krüppel-like zinc fingers. FAZF is homologous to the promyelocytic leukemia zinc finger (PLZF) protein, which has been shown to act as a transcriptional repressor by recruitment of nuclear corepressors (N-CoR, Sin3, and HDAC1 complex). Consistent with a role in FA, BTB/POZ-containing proteins have been implicated in oncogenesis, limb morphogenesis, hematopoiesis, and proliferation. We show that FAZF is a transcriptional repressor that is able to bind to the same DNA target sequences as PLZF. Our data suggest that the FAZF/FANCC interaction maps to a region of FANCC deleted in FA patients with a severe disease phenotype. We also show that FAZF and wild-type FANCC can colocalize in nuclear foci, whereas a patient-derived mutant FANCC that is compromised for nuclear localization cannot. These results suggest that the function of FANCC may be linked to a transcriptional repression pathway involved in chromatin remodeling." @default.
• W56784355 created "2016-06-24" @default.
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• W56784355 date "1999-12-01" @default.
• W56784355 modified "2023-10-18" @default.
• W56784355 title "A Novel BTB/POZ Transcriptional Repressor Protein Interacts With the Fanconi Anemia Group C Protein and PLZF" @default.
• W56784355 cites W1411619184 @default.
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• W56784355 cites W1553544241 @default.
• W56784355 cites W1572138865 @default.
• W56784355 cites W1598192021 @default.
• W56784355 cites W16620579 @default.
• W56784355 cites W1870470978 @default.
• W56784355 cites W188006079 @default.
• W56784355 cites W1903792504 @default.
• W56784355 cites W1951809136 @default.
• W56784355 cites W1964106952 @default.
• W56784355 cites W1964274155 @default.
• W56784355 cites W1966322170 @default.
• W56784355 cites W1966971933 @default.
• W56784355 cites W1972710550 @default.
• W56784355 cites W1981859725 @default.
• W56784355 cites W1982342754 @default.
• W56784355 cites W1982640053 @default.
• W56784355 cites W1984565556 @default.
• W56784355 cites W1991311051 @default.
• W56784355 cites W1992567175 @default.
• W56784355 cites W1995204178 @default.
• W56784355 cites W1996719010 @default.
• W56784355 cites W1996904533 @default.
• W56784355 cites W1999725652 @default.
• W56784355 cites W2003618279 @default.
• W56784355 cites W2005404159 @default.
• W56784355 cites W2006741975 @default.
• W56784355 cites W2006881752 @default.
• W56784355 cites W2010117150 @default.
• W56784355 cites W2013743651 @default.
• W56784355 cites W2036503229 @default.
• W56784355 cites W2038499121 @default.
• W56784355 cites W2044329004 @default.
• W56784355 cites W2046045770 @default.
• W56784355 cites W2055043387 @default.
• W56784355 cites W2065417936 @default.
• W56784355 cites W2071716563 @default.
• W56784355 cites W2074499201 @default.
• W56784355 cites W2075079030 @default.
• W56784355 cites W2076218188 @default.
• W56784355 cites W2079604568 @default.
• W56784355 cites W2079722920 @default.
• W56784355 cites W2082172922 @default.
• W56784355 cites W2083034560 @default.
• W56784355 cites W2086567214 @default.
• W56784355 cites W2094646101 @default.
• W56784355 cites W2095184701 @default.
• W56784355 cites W2101143531 @default.
• W56784355 cites W2106004899 @default.
• W56784355 cites W2110098007 @default.
• W56784355 cites W2110542977 @default.
• W56784355 cites W2112087352 @default.
• W56784355 cites W2117816178 @default.
• W56784355 cites W2118904153 @default.
• W56784355 cites W2121637532 @default.
• W56784355 cites W2133442371 @default.
• W56784355 cites W2136144485 @default.
• W56784355 cites W2137232000 @default.
• W56784355 cites W2140716445 @default.
• W56784355 cites W2142946131 @default.
• W56784355 cites W2158714788 @default.
• W56784355 cites W2159480680 @default.
• W56784355 cites W2167194725 @default.
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• W56784355 cites W2387074628 @default.
• W56784355 cites W308204182 @default.
• W56784355 cites W3117462546 @default.
• W56784355 cites W36484103 @default.
• W56784355 cites W4235275114 @default.
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• W56784355 doi "https://doi.org/10.1182/blood.v94.11.3737" @default.
• W56784355 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/10572087" @default.
• W56784355 hasPublicationYear "1999" @default.
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