Your search keyword '"Ianari, A"' showing total 5 results

1. Systematic profiling of conditional degron tag technologies for target validation studies.

Author

Bondeson, Daniel P., Mullin-Bernstein, Zachary, Oliver, Sydney, Skipper, Thomas A., Atack, Thomas C., Bick, Nolan, Ching, Meilani, Guirguis, Andrew A., Kwon, Jason, Langan, Carly, Millson, Dylan, Paolella, Brenton R., Tran, Kevin, Wie, Sarah J., Vazquez, Francisca, Tothova, Zuzana, Golub, Todd R., Sellers, William R., and Ianari, Alessandra

Subjects

CHIMERIC proteins, DRUG target, COMMUNITY life

Abstract

Conditional degron tags (CDTs) are a powerful tool for target validation that combines the kinetics and reversible action of pharmacological agents with the generalizability of genetic manipulation. However, successful design of a CDT fusion protein often requires a prolonged, ad hoc cycle of construct design, failure, and re-design. To address this limitation, we report here a system to rapidly compare the activity of five unique CDTs: AID/AID2, IKZF3d, dTAG, HaloTag, and SMASh. We demonstrate the utility of this system against 16 unique protein targets. We find that expression and degradation are highly dependent on the specific CDT, the construct design, and the target. None of the CDTs leads to efficient expression and/or degradation across all targets; however, our systematic approach enables the identification of at least one optimal CDT fusion for each target. To enable the adoption of CDT strategies more broadly, we have made these reagents, and a detailed protocol, available as a community resource. Conditional Degron Tags are a valuable tool to validate and study novel therapeutic targets. Here, the authors compared 5 orthogonal tags across 16 unique proteins and provide a panel of vectors for users to systematically screen the tags with their own protein of interest. [ABSTRACT FROM AUTHOR]

Published

2022

2. Differential regulation of E2F1 apoptotic target genes in response to DNA damage.

Author

Pediconi, Natalia, Ianari, Alessandra, Costanzo, Antonio, Belloni, Laura, Gallo, Rita, Cimino, Letizia, Porcellini, Antonio, Screpanti, Isabella, Balsano, Clara, Alesse, Edoardo, Gulino, Alberto, and Levrero, Massimo

Subjects

GENETIC regulation, TRANSCRIPTION factors, DNA damage

Abstract

E2F1, a member of the E2F family of transcription factors, in addition to its established proliferative effect[SUP1], has also been implicated in the induction of apoptosis through p53-dependent and p53-independent pathways[SUP2]. Several genes involved in the activation or execution of the apoptotic programme have recently been shown to be upregulated at the transcriptional level by E2F1 overexpression, including the genes encoding INK4a/ARF, Apaf-1, caspase 7 and p73 (refs 3-5). E2F1 is stabilized in response to DNA damage[SUP6,7] but it has not been established how this translates into the activation of specific subsets of E2F target genes. Here, we applied a chromatin immunoprecipitation approach to show that, in response to DNA damage, E2F1 is directed from cell cycle progression to apoptotic E2F target genes. We identify p73 as an important E2F1 apoptotic target gene in DNA damage response and we show that acetylation is required for E2F1 recruitment on the P1p73 promoter and for its transcriptional activation. [ABSTRACT FROM AUTHOR]

Published

2003

3. Concordance rate for Type II diabetes mellitus in monozygotic twins: actuarial analysis.

Author

Medici, F., Hawa, M., Ianari, A., Pyke, D. A., and Leslie, R. D. G

Abstract

To determine the concordance rate for Type II (non-insulin-dependent) diabetes mellitus in monozygotic twin pairs, initially ascertained discordant for diabetes, we carried out a prospective study on 44 non-diabetic subjects, each of whom had a sibling twin with diabetes (21 men, 23 women, median age 55 years, interquartile range 47–65). The subjects were referred as discordant for Type II diabetes. The twin pairs were part of the British Diabetic Twin Study and ascertained between May 1968 and January 1998. These subjects underwent an OGTT at time of referral and periodically thereafter. The mean follow-up was 8 years (range 0–18 years) and data were collected until January 1996. The percentage of twins who developed Type II diabetes was assessed by standard actuarial life-table methods and the pairwise concordance rate, that is the proportion of concordant pairs over the sum of concordant and discordant pairs, was calculated. The observed rates of concordance for Type II diabetes at 1, 5, 10, and 15 years follow-up were 17, 33, 57, and 76 %, respectively. The concordance rate for any abnormality of glucose metabolism (either Type II diabetes or impaired glucose tolerance) at 15 years follow-up was 96 %. The concordance rate for Type II diabetes in monozygotic twins is very high even in twins initially ascertained discordant for diabetes. [Diabetologia (1999) 42: 146–150] [ABSTRACT FROM AUTHOR]

Published

1999

4. DON’T TELL ME I CAN’T… …take up netball.

Author

HANMAN, JAMES and IANARI, LUCIANA

Published

2018

5. Cell death or survival: The complex choice of the retinoblastoma tumor suppressor protein.

Author

Ianari, Alessandra and Gulino, Alberto

Published

2010