KIF1A is kinetically tuned to be a superengaging motor under hindering loads

Pyrpassopoulos, Serapion; Gicking, Allison M.; Zaniewski, Taylor M.; Hancock, William O.; Ostap, E. Michael

doi:10.1073/pnas.2216903120

Cited by 12 publications

(10 citation statements)

References 67 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We show that replacing KIF1A’s K-loop for loop-12 of the kinesin-3 motor, KIF14, which has only a single positively charged residue located close to the MT interface, results in a significant reduction of the run-length of the motor. This result is consistent with recent reports that show that KIF1A’s K-loop and its positively-charged residues are essential for KIF1A’s superprocessivity 74, 75 .…”

Section: Discussionsupporting

confidence: 94%

“…KIF1A, like other kinesin-3 family members, has an elongated Lys-rich loop-12 referred to as the K-loop. While it has been shown that the K-loop is important for KIF1A-MT binding [72][73][74][75] , how it interacts with MTs has not been clear as most of this loop is either disordered or not resolved in X-ray crystal structures of KIF1A and in lower resolution cryo-EM structures of KIF1A-MT complexes. Our high-resolution structures of KIF1A-MT complexes show the complete polypeptide path of the K-loop (Fig.…”

Section: Structure and Role Of The Kif1a-sepcific K-loopmentioning

confidence: 99%

“…The specific role of KIF1A's K-loop in MT binding has been previously established 57,[80][81][82] , yet its interaction mechanism with MTs has remained unclear. Previous X-ray crystallography and lower-resolution cryo-EM studies have not captured the conformation of this loop and how it interacts with MTs [65][66][67][68]70,71 .…”

Section: Structure and Role Of The Kif1a K-loopmentioning

confidence: 99%

See 2 more Smart Citations

Cryo-EM Unveils the Processivity Mechanism of Kinesin KIF1A and the Impact of its Pathogenic Variant P305L

Benoit

Rao

Asenjo

et al. 2023

Preprint

View full text Add to dashboard Cite

Mutations in the Kinesin-3 motor KIF1A, a microtubule (MT)-associated motor protein, cause devastating neurodevelopmental and neurodegenerative diseases termed KIF1A-associated neurological disorders (KAND). While the mechanism of KIF1A is increasingly understood, high resolution (<4 Å) structural information of KIF1A-MT complexes is lacking. Here, we present 2.7-3.4 Å resolution structures of dimeric MT-bound wild-type (WT) KIF1A and the pathogenic P305L mutant as a function of the nucleotide state. Our structures reveal that 1) the KIF1A dimer binds MTs in one- and two-heads-bound states, 2) that both MT-bound heads assume distinct conformations with tight inter-head connection, 3) the position and conformation of the class-specific loop 12 (the K-loop), and 4) that the P305L mutation causes structural changes in the K-loop that result in a weakly MT-bound state. Motivated by our structural insights, we performed structure-function studies that reveal that both the K-loop and head-head coordination are major determinants of KIF1A's superprocessive motility. Our work provides key insights into the mechanism of KIF1A and provides near-atomic structures of WT and mutant KIF1A for future structure-guided drug-design approaches to treat KAND.

show abstract

Section: Discussionsupporting

confidence: 94%

Section: Structure and Role Of The Kif1a-sepcific K-loopmentioning

confidence: 99%

Section: Structure and Role Of The Kif1a K-loopmentioning

confidence: 99%

See 1 more Smart Citation

Cryo-EM Unveils the Processivity Mechanism of Kinesin KIF1A and the Impact of its Pathogenic Variant P305L

Benoit

Rao

Asenjo

et al. 2023

Preprint

View full text Add to dashboard Cite

show abstract

“…It is worth mentioning that this type of behavior does not seem to be a generic feature of all kinesins. We recently studied the forces developed by KIF1A which is a member of the kinesin 3 family and we did not find such a variable type of behavior with microtubules in the three-bead assay [27]. However, in the single-bead assay the vertical force component Fz accelerated the detachment of KIF1A from the microtubule relative to the three-bead assay, which is in agreement with what we observed for KIF5B (kinesin 1) [27].…”

Section: A Surprising Discovery: Kinesin 1 and Microtubules Can Exhib...supporting

confidence: 89%

“…We recently studied the forces developed by KIF1A which is a member of the kinesin 3 family and we did not find such a variable type of behavior with microtubules in the three-bead assay [27]. However, in the single-bead assay the vertical force component Fz accelerated the detachment of KIF1A from the microtubule relative to the three-bead assay, which is in agreement with what we observed for KIF5B (kinesin 1) [27]. Since, as mentioned previously, the pair of opposing forces on the microtubule in the three-bead assay may apply in general along different protofilaments, the azimuthal angle  (cylindrical coordinates of the microtubule structure) between this pair of forces will be variable between different dumbbells (Fig.…”

Section: A Surprising Discovery: Kinesin 1 and Microtubules Can Exhib...mentioning

confidence: 91%

Manipulation of force geometry using optical tweezers reveals novel features of biomolecular interactions

Pyrpassopoulos,

Ostap,

Shuman

et al. 2023

Optical Trapping and Optical Micromanipulation XX

View full text Add to dashboard Cite

Optical tweezers have greatly impacted the development of mechanobiology by enabling high precision subpiconewton measurements of mechanical forces developed by force generating proteins, called molecular motors, at the single-molecule level. Molecular motors, such as kinesins hydrolyze ATP to generate force (10 pN) and transport in a directional manner intracellular cargoes along cytoskeletal filamentous tracks called microtubules. The force developed by kinesins have been mainly studied using the "single-bead" assay, where an optically trapped bead is pulled by a bead-attached kinesin molecule as it steps along a surface immobilized microtubule. This assay, besides forces parallel to the long axis of the filament on which the kinesin processes, forces perpendicular to the filament due to the bead interacting with the underlying microtubule. These perpendicular forces, which cannot be directly measured, can accelerate the detachment of the molecular motor from its filamentous track. An alternative approach is the "three-bead" assay, in which the vertical force component is minimized, and the total opposing force is mainly parallel to the microtubule. Experiments with kinesin show that microtubule attachment durations can be highly variable and up to 10-fold longer in the three-bead assay, compared to the single-bead. Thus, the ability of kinesin to bear mechanical load and remain attached to microtubules depends on the geometry of forces across the microtubule. Our work shows the importance for the development of optical trapping assays where the direction of the force vector can be very finely controlled and measured when studying the mechanical strength of biomolecular interactions.

show abstract

A Model for Chemomechanical Coupling of Kinesin-3 Motor

Xie

2024

Cel. Mol. Bioeng.

View full text Add to dashboard Cite

KIF1A is kinetically tuned to be a superengaging motor under hindering loads

Cited by 12 publications

References 67 publications

Cryo-EM Unveils the Processivity Mechanism of Kinesin KIF1A and the Impact of its Pathogenic Variant P305L

Cryo-EM Unveils the Processivity Mechanism of Kinesin KIF1A and the Impact of its Pathogenic Variant P305L

Manipulation of force geometry using optical tweezers reveals novel features of biomolecular interactions

A Model for Chemomechanical Coupling of Kinesin-3 Motor

Contact Info

Product

Resources

About