A high affinity Sybody blocks Cofilin-1 binding to F-actin in vitro and in cancer cells

Paraschiakos, Themistoklis; Scholz, Jonas; Li, Jing; Pogenberg, Vivian; Faix, Jan; Windhorst, Sabine; Deckers, Markus; Han, Soo-Ji

doi:10.1016/j.bcp.2025.116866

Journal Article

PUBDB-2025-04113

A high affinity Sybody blocks Cofilin-1 binding to F-actin in vitro and in cancer cells

Paraschiakos, T. ; Li, J. ; Scholz, J. ; Han, S.-J. ; Deckers, M. ; Pogenberg, V. ; Faix, J. ; Windhorst, S. (Corresponding author)

2025
Elsevier Science Amsterdam [u.a.]

Biochemical pharmacology 236, 116866 - (2025) [10.1016/j.bcp.2025.116866]

This record in other databases:

Please use a persistent id in citations: doi:10.1016/j.bcp.2025.116866

Abstract: Upregulation of the actin-severing protein Cofilin-1 is implicated in enhancing malignancy of various cancer types by promoting actin turnover and increasing cellular motility. Despite the importance of targeting Cofilin-1, currently there is a lack of inhibitors specifically targeting its actin-severing activity. To address this issue, we generated synthetic anti-Cofilin-1 nanobodies (Sybodies) that interfere with human Cofilin-1 binding to filamentous actin. We identified four high affinity Sybodies against human Cofilin-1 with dissociation constants (KD) in the nanomolar range that inhibited G-actin sequestration, and actin-severing activity of Cofilin-1 in vitro. Notably, Sybody B12, with the lowest KD of approximately 27 nM, competitively blocked actin binding to Cofilin-1, and also inhibited G-actin sequestration of murine Cofilin-1. The crystal structure of the Sybody-B12-Cofilin-1 complex, resolved at 1.8 Å, revealed that Sybody B12 binds to the G-actin binding site of Cofilin-1, showing that Sybody B12 engages the same binding site on Cofilin-1 as actin. Consistently, transient expression of mPlum-tagged Sybody B12 in human H1299 lung cancer cells inhibited the formation of enhanced green fluorescent protein (EGFP)-Cofilin-actin rods. Notably, stable expression of Sybody B12 did not affect viability of H1299 cells, and no compensatory up-regulation of Cofilin-2 or actin-depolymerization factor (ADF) mRNA were detectable in Sybody B12 expressing H1299 cells. Together, these findings suggest that Sybody B12 exhibits a strong potential as tool for inhibiting the interaction of Cofilin-1 with actin. In addition, it could serve as a promising lead structure for designing Cofilin-1 inhibitors in silico.

Classification:

ddc:610

Contributing Institute(s):

EMBL-User (EMBL-User)

Research Program(s):

6G3 - PETRA III (DESY) (POF4-6G3) (POF4-6G3)

Experiment(s):

PETRA Beamline P14 (PETRA III)

Database coverage:
Medline

; BIOSIS Previews ; Biological Abstracts ; Clarivate Analytics Master Journal List ; Current Contents - Life Sciences ; Ebsco Academic Search ; Essential Science Indicators ; IF >= 5 ; JCR ; Nationallizenz

; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection

Click to display QR Code for this record

The record appears in these collections:
Document types > Articles > Journal Article
Private Collections > >EMBL > EMBL-User
Documents in process
Public records

Record created 2025-09-26, last modified 2025-09-26

Similar records

Restricted:

PDF

PDF (PDFA)
External link:

Fulltext

Rate this document:

(Not yet reviewed)

Add to personal basket
Export as Author List with IDs BibTeX (UTF-8), EndNote XML, EndNote Text, RIS, MARC, Print MARC, MARCXML, DC,
Request correction
Submit fulltext

guest :: login PUBDB
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help