Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
Author
Journal
IF	>30 >20 >10 >5 all

Title	Amyloid Fibrillation of a Ninjurin-1-Derived α-Helical Peptide: Structural Insights into Conformational Transition.
Journal, issue, pages	ACS Nano, Vol. 19, Issue 40, Page 35977-35991, Year 2025
Publish date	Oct 14, 2025
Authors	Meijiao Wang / Wencheng Xia / Dan Zhao / Zhaoyi Zhai / Rongjing Chen / Xue Bai / Zhe Zhang / Hao Fan / Jian-Ping Zhang / Cong Liu / Fang Jiao /
PubMed Abstract	Amyloid fibrils, defined by their cross-β architecture, are central to both disease and function, yet the molecular principles governing their formation remain incompletely understood. Ninjurin-1 ...Amyloid fibrils, defined by their cross-β architecture, are central to both disease and function, yet the molecular principles governing their formation remain incompletely understood. Ninjurin-1 (NINJ1), a membrane protein essential for plasma membrane rupture (PMR) during cell death, contains an N-terminal amphipathic α-helix. Here, we investigate a key peptide fragment of this region (residues 40-69, HE30) and uncover its membrane-disruptive activity, self-assembly, and structural transitions. Monomeric HE30 reorganizes lipids to induce membrane thinning while undergoing an environmentally responsive α-helix-to-β-sheet transition that drives amyloid fibril formation. Fibrils formed at physiological temperatures are predominantly nontwisted, but elevated temperatures induce left-handed twisted structures with variable pitches and lengths, and even result in high-order superhelical bundles. We further resolved the twisted fibril structures of HE30 by cryo-EM, revealing two distinct fibril polymorphs stabilized by both hydrophobic and electrostatic interactions. Consistently, salts inhibit HE30 fibrillation, emphasizing the role of electrostatic interactions in stabilizing fibrils. Moreover, acidic conditions (∼pH 4.4) promote fibril formation, whereas alkaline conditions lead to disassembly into α-helical monomers in a reversible manner. AFM tracking reveals the asymmetric growth of fibrils, where one end elongates faster and the opposite end exhibits slower growth or complete inhibition. Functionally, HE30 fibrils are nontoxic and act as scaffolds for the temperature-controlled assembly of gold nanoparticle (AuNPs) superstructures. These findings not only advance our understanding of NINJ1-induced PMR but also provide a detailed structural basis for HE30 fibril formation via α-helix to β-sheet transitions and underscore their potential as building blocks for fibril-based biomaterials.
External links	ACS Nano / PubMed:41037056
Methods	EM (helical sym.)
Resolution	2.9 - 3.2 Å
Structure data	62179 9k8s EMDB-62179, PDB-9k8s: Cryo-EM structure of HE30 polymorph 1 Method: EM (helical sym.) / Resolution: 2.9 Å 62180 9k8t EMDB-62180, PDB-9k8t: Cryo-EM structure of HE30 polymorph 2 Method: EM (helical sym.) / Resolution: 3.2 Å
Source	homo sapiens (human)
Keywords	PROTEIN FIBRIL / helical fibril