Literature DB >> 27751944

Hippocampal to basal forebrain transport of Mn2+ is impaired by deletion of KLC1, a subunit of the conventional kinesin microtubule-based motor.

Christopher S Medina1, Octavian Biris2, Tomas L Falzone3, Xiaowei Zhang4, Amber J Zimmerman1, Elaine L Bearer5.   

Abstract

Microtubule-based motors carry cargo back and forth between the synaptic region and the cell body. Defects in axonal transport result in peripheral neuropathies, some of which are caused by mutations in KIF5A, a gene encoding one of the heavy chain isoforms of conventional kinesin-1. Some mutations in KIF5A also cause severe central nervous system defects in humans. While transport dynamics in the peripheral nervous system have been well characterized experimentally, transport in the central nervous system is less experimentally accessible and until now not well described. Here we apply manganese-enhanced magnetic resonance (MEMRI) to study transport dynamics within the central nervous system, focusing on the hippocampal-forebrain circuit, and comparing kinesin-1 light chain 1 knock-out (KLC-KO) mice with age-matched wild-type littermates. We injected Mn2+ into CA3 of the posterior hippocampus and imaged axonal transport in vivo by capturing whole-brain 3D magnetic resonance images (MRI) in living mice at discrete time-points after injection. Precise placement of the injection site was monitored in both MR images and in histologic sections. Mn2+-induced intensity progressed along fiber tracts (fimbria and fornix) in both genotypes to the medial septal nuclei (MSN), correlating in location with the traditional histologic tract tracer, rhodamine dextran. Pairwise statistical parametric mapping (SPM) comparing intensities at successive time-points within genotype revealed Mn2+-enhanced MR signal as it proceeded from the injection site into the forebrain, the expected projection from CA3. By region of interest (ROI) analysis of the MSN, wide variation between individuals in each genotype was found. Despite this statistically significant intensity increases in the MSN at 6h post-injection was found in both genotypes, albeit less so in the KLC-KO. While the average accumulation at 6h was less in the KLC-KO, the difference between genotypes did not reach significance. Projections of SPM T-maps for each genotype onto the same grayscale image revealed differences in the anatomical location of significant voxels. Although KLC-KO mice had smaller brains than wild-type, the gross anatomy was normal with no apparent loss of septal cholinergic neurons. Hence anatomy alone does not explain the differences in SPM maps. We conclude that kinesin-1 defects may have only a minor effect on the rate and distribution of transported Mn2+ within the living brain. This impairment is less than expected for this abundant microtubule-based motor, yet such defects could still be functionally significant, resulting in cognitive/emotional dysfunction due to decreased replenishments of synaptic vesicles or mitochondria during synaptic activity. This study demonstrates the power of MEMRI to observe and measure vesicular transport dynamics in the central nervous system that may result from or lead to brain pathology.
Copyright © 2016 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Axonal transport; Hippocampal-forebrain circuit; Kinesin light chain-1; Kinesin-1; Manganese-enhanced magnetic resonance imaging (MEMRI); Statistical parametric mapping

Mesh:

Substances:

Year:  2016        PMID: 27751944      PMCID: PMC5457905          DOI: 10.1016/j.neuroimage.2016.09.035

Source DB:  PubMed          Journal:  Neuroimage        ISSN: 1053-8119            Impact factor:   6.556


  81 in total

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Authors:  Karen D B Smith; Richard Paylor; Robia G Pautler
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6.  Cloning mammalian genes by expression selection of genetic suppressor elements: association of kinesin with drug resistance and cell immortalization.

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Journal:  Proc Natl Acad Sci U S A       Date:  1994-04-26       Impact factor: 11.205

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Authors:  Elaine L Bearer; Xiaowei Zhang; Russell E Jacobs
Journal:  Neuroimage       Date:  2007-05-18       Impact factor: 6.556

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Journal:  Brain Res       Date:  2007-04-06       Impact factor: 3.252

9.  Defective kinesin heavy chain behavior in mouse kinesin light chain mutants.

Authors:  A Rahman; A Kamal; E A Roberts; L S Goldstein
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  7 in total

1.  Automated Computational Processing of 3-D MR Images of Mouse Brain for Phenotyping of Living Animals.

Authors:  Christopher S Medina; Brett Manifold-Wheeler; Aaron Gonzales; Elaine L Bearer
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2.  Alterations of functional circuitry in aging brain and the impact of mutated APP expression.

Authors:  Elaine L Bearer; Brett C Manifold-Wheeler; Christopher S Medina; Aaron G Gonzales; Frances L Chaves; Russell E Jacobs
Journal:  Neurobiol Aging       Date:  2018-06-28       Impact factor: 4.673

3.  Studying Axonal Transport in the Brain by Manganese-Enhanced Magnetic Resonance Imaging (MEMRI).

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Journal:  Methods Mol Biol       Date:  2022

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5.  Herpes Simplex Virus, Alzheimer's Disease and a Possible Role for Rab GTPases.

Authors:  Elaine L Bearer; Chengbiao Wu
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Review 6.  Manganese-Enhanced Magnetic Resonance Imaging: Application in Central Nervous System Diseases.

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Journal:  Front Neurol       Date:  2020-02-25       Impact factor: 4.003

7.  Decoupling the Effects of the Amyloid Precursor Protein From Amyloid-β Plaques on Axonal Transport Dynamics in the Living Brain.

Authors:  Christopher S Medina; Taylor W Uselman; Daniel R Barto; Frances Cháves; Russell E Jacobs; Elaine L Bearer
Journal:  Front Cell Neurosci       Date:  2019-12-03       Impact factor: 5.505

  7 in total

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