Abstract

SummaryMitochondria play fundamental roles within cells, including energy provision, calcium homeostasis, and the regulation of apoptosis. The transport of mitochondria by microtubule-based motors is critical for neuronal structure and function. This process allows local requirements for mitochondrial functions to be met and also facilitates recycling of these organelles [1, 2]. An age-related reduction in mitochondrial transport has been observed in neurons of mammalian and non-mammalian organisms [3, 4, 5, 6], and has been proposed to contribute to the broader decline in neuronal function that occurs during aging [3, 5, 6, 7]. However, the factors that influence mitochondrial transport in aging neurons are poorly understood. Here we provide evidence using the tractable Drosophila wing nerve system that the cyclic AMP/protein kinase A (cAMP/PKA) pathway promotes the axonal transport of mitochondria in adult neurons. The level of the catalytic subunit of PKA decreases during aging, and acute activation of the cAMP/PKA pathway in aged flies strongly stimulates mitochondrial motility. Thus, the age-related impairment of transport is reversible. The expression of many genes is increased by PKA activation in aged flies. However, our results indicate that elevated mitochondrial transport is due in part to upregulation of the heavy chain of the kinesin-1 motor, the level of which declines during aging. Our study identifies evolutionarily conserved factors that can strongly influence mitochondrial motility in aging neurons.

Highlights

  • Signaling pathways that increase lifespan are attractive candidates for exploring the regulation of axonal transport during aging [6, 10]

  • To shed light on the regulation of mitochondrial transport in aging neurons, we exploited a tractable system for imaging of axonal transport in an adult animal: the sensory neurons of the translucent Drosophila wing [5, 8, 9] (Figure 1A)

  • The decline in mitochondrial transport begins in the first week of adult life [5] and reflects reduced anterograde and retrograde movements (Figure S1B), equating to transport toward microtubule plus ends and minus ends, respectively [5]

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Summary

Introduction

Signaling pathways that increase lifespan are attractive candidates for exploring the regulation of axonal transport during aging [6, 10]. Cyclic AMP (cAMP) is an important second messenger in intracellular signaling, and elevation of its concentration can extend lifespan in Drosophila and mice [11, 12]. We investigated whether cAMP influences axonal transport of mitochondria in aged flie

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