FEDERICA CANNISTRÀ

PhD Graduate

PhD program:: XXXVIII

advisor: Isabella Saggio

Thesis title: Role of the nuclear envelope in physiological and pathological conditions

Background: During “open” mitosis, the nuclear envelope disassembles to allow chromosome segregation and reassembles around daughter nuclei. The Endosomal Sorting Complex Required for Transport (ESCRT) mediates this process. While ESCRT-III proteins drive this process and are recruited by upstream factors such as BAF, the involvement of other ESCRT proteins remains unclear. AKTIP is a novel ESCRT-I-associated protein. It shows similarities with the ESCRT-I TSG101, it localizes at the midbody during abscission together with the ESCRT-I and ESCRT-III components. Intriguingly, AKTIP also localizes at the nuclear rim in interphase cells. Aim: We therefore asked whether AKTIP contributes to nuclear envelope reformation by coordinating ESCRT-III organization and maintaining post-mitotic nuclear integrity. Methods: To investigate the role of AKTIP in nuclear envelope dynamics, HeLa cells were depleted of AKTIP using lentiviral transduction. Immunofluorescence microscopy was used to examine AKTIP localization during mitosis, its co-distribution with BAF and IST1. The effects of AKTIP loss on the distribution of ESCRT-III components IST1 and CHMP2A was assessed. The role of AKTIP in nuclear integrity was also evaluated by analyzing cGAS foci, laminB1 discontinuities, and micronuclei formation. Results: Data obtained during the PhD show that AKTIP localizes at chromatin discs during anaphase, where it colocalizes with the ESCRT-III-associated protein IST1. AKTIP depletion impaired proper ESCRT-III localization at this stage. During pro-metaphase, AKTIP assembled into a ring-like structure on nascent microtubule spindles, colocalizing with BAF; notably, BAF depletion disrupted AKTIP localization during mitosis. Functional analyses revealed that loss of AKTIP led to increased nuclear abnormalities, including laminB1 discontinuities, cGAS-positive foci, and micronuclei formation. Conclusions: Our findings identify AKTIP as a crucial regulator of ESCRT-III organization during nuclear envelope reformation. Its recruitment begins as early as pro-metaphase, likely through a cooperative mechanism with BAF that links chromatin anchoring to membrane remodeling. AKTIP dysfunction compromises nuclear architecture, highlighting its potential relevance in aging and cancer biology.

Research products

11573/1752676 - 2025 - The Dynamics of the ESCRT Machinery in Open Mitosis from Physiology to Pathology

La Torre, Mattia; Cannistrà, Federica; Burla, Romina; Saggio, Isabella - 01g Articolo di rassegna (Review)

paper: CELLS (Basel: mdpi-Molecular Diversity Preservation International) pp. - - issn: 2073-4409 - wos: WOS:001612421500001 (0) - scopus: 2-s2.0-105021431610 (0)

11573/1726443 - 2024 - Analysis of rapidly mutating Y-STRs enables almost complete discrimination of unrelated and related males from the African continent

Barni, Filippo; Ralf, Arwin; Della Rocca, Chiara; Cannistrà, Federica; Gigliucci, Marco; Trombetta, Beniamino; Berti, Andrea; Kayser, Manfred; Cruciani, Fulvio - 01f Lettera, Nota

paper: FORENSIC SCIENCE INTERNATIONAL: GENETICS (Elsevier) pp. - - issn: 1872-4973 - wos: WOS:001316544700001 (3) - scopus: 2-s2.0-85202786549 (3)

11573/1691923 - 2023 - Impact of diffused versus vasculature targeted DNA damage on the heart of mice depleted of telomeric factor Ft1

La Torre, Mattia; Centofante, Eleonora; Nicoletti, Carmine; Burla, Romina; Giampietro, Alessandro; Cannistrà, Federica; Schirone, Leonardo; Valenti, Valentina; Sciarretta, Sebastiano; Musarò, Antonio; Saggio, Isabella - 01a Articolo in rivista

paper: AGING CELL (-MALDEN:WILEY-BLACKWELL PUBLISHING, INC. -Oxford : Blackwell, 2002-) pp. 1-16 - issn: 1474-9718 - wos: WOS:001104818700001 (1) - scopus: 2-s2.0-85176915477 (1)