A Noninvasive Approach to Optogenetics Using Focused Ultrasound Blood Brain Barrier Disruption for the Delivery of Radioluminescent Particles

Rich, Megan; Zhang, Eric; Dickey, Ashley; Jones, Haley W.; Cannon, Kelli E.; Bandera, Yuriy; Foulger, Stephen H.; Lubin, Farah D.; Bolding, Mark

doi:10.1101/2020.08.20.248302

Cited by 3 publications

(6 citation statements)

References 34 publications

(41 reference statements)

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“…Radioluminescent nanoparticles have been shown to persist in brain tissue for at least 72 h after injection [54], enabling repeated experiments over multiple days. Radioluminescent nanoparticles can also be delivered into the brain using focused ultrasound to open the blood brain barrier [22], avoiding the damage of intracranial injection. X-ray activation of RLPs is therefore a potentially viable method for noninvasive optogenetics.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, LSO:Ce is nonhygroscopic, biologically inert, and can be synthesized at the nanoscale level [76,77]. While we used microparticles in this study, LSO:Ce nanoparticles could be used to increase their likelihood of passing through the blood-brain barrier, especially if used together with focused ultrasound to increase BBB permeability [22]. We previously demonstrated that LSO:Ce microparticles are non-toxic to neurons and had very minor effects on synaptic transmission [21].…”

Section: Discussionmentioning

confidence: 99%

“…The use of RLPs would allow the light to be generated locally, overcoming the issue of light attenuation and the need for high power intensities. Additionally, inorganic scintillators can be noninvasively delivered to specific brain regions using focused ultrasound [22]. A common inorganic scintillator is Ceriumdoped lutetium oxyorthosilicate (LSO:Ce).…”

Section: Introductionmentioning

confidence: 99%

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Feasibility of cerium-doped LSO particles as a scintillator for x-ray induced optogenetics

Bartley¹,

Fischer²,

Bagley³

et al. 2021

J. Neural Eng.

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Optogenetics is a widely used tool for studying neural circuits. However, non-invasive methods for light delivery in the brain are needed to avoid physical damage typically caused by intracranial insertion of light guides. An innovative strategy could employ X-ray activation of radioluminescent particles (RLPs) to emit localized light. We previously reported that RLPs composed of cerium doped lutetium oxyorthosilicate (LSO:Ce), an inorganic scintillator that emits blue light, are biocompatible with neuronal function and synaptic transmission. However, little is known about the consequences of acute X-ray exposure on synaptic function and long-term plasticity. Furthermore, modulation of neuronal or synaptic function by X-ray induced radioluminescence from RLPs has not yet been demonstrated. Here we show that 30 minutes of X-ray exposure at a rate of 0.042 Gy/second caused no change in the strength of basal glutamatergic transmission during extracellular dendritic field recordings in mouse hippocampal slices. Additionally, long-term potentiation (LTP), a robust measure of synaptic integrity, was able to be induced after X-ray exposure and expressed at a magnitude not different from control conditions (absence of X-rays). This is important as synaptic plasticity is critical to learning and memory. Next, we used molecular and electrophysiological approaches to determine if X-ray dependent radioluminescence emitted from RLPs can activate light sensitive proteins. We found that X-ray stimulation of RLPs elevated cAMP levels in HEK293T cells expressing OptoXR, a chimeric opsin receptor that combines the extracellular lightsensitive domain of channelrhodopsin-2 (ChR2) with an intracellular second messenger signaling cascade. This demonstrates that X-ray radioluminescence from LSO:Ce particles can activate OptoXR. Next, we tested whether X-ray activation of the RLPs can enhance synaptic activity in whole-cell recordings from hippocampal neurons expressing ChR2, both in cell culture and acute hippocampal slices. Importantly, Xray radioluminescence caused an increase in the frequency of spontaneous excitatory postsynaptic currents (sEPSCs) in both systems, indicating activation of ChR2 and excitation of neurons. Together, our results show that X-ray activation of LSO:Ce particles can heighten cellular and synaptic function. The combination of LSO:Ce inorganic scintillators and X-rays is therefore a viable method for optogenetics as an alternative to more invasive light delivery methods.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Feasibility of cerium-doped LSO particles as a scintillator for x-ray induced optogenetics

Bartley¹,

Fischer²,

Bagley³

et al. 2021

J. Neural Eng.

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show abstract

“…Recently, Rich et al (2020) reported successful non-invasive delivery of light-emitting radio luminescent X-ray sensitive particles (RLPs) to the hippocampus of rats using magnetic resonance imaging (MRI)-guided focused ultrasound (FUS). Crucially, MRI-guided FUS can be used to deliver both RLPs and viral vectors for light-sensitive channel expression as demonstrated by Wang et al (2017).…”

Section: Reply To Objections About Potential Therapeutic Applicabilit...mentioning

confidence: 99%

Personality and Authenticity in Light of the Memory-Modifying Potential of Optogenetics: A Reply to Objections about Potential Therapeutic Applicability of Optogenetics

Adamczyk

Zawadzki

2021

AJOB Neuroscience

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“…In contrast, findings of recent years have shown that the prospect of providing measures to selectively deactivate the targeted memory can be actually realized with the use of an emerging MMT-optogenetics [35][36][37]. Although making optogenetic system operable to control neural activity underlying the memory still involves invasive manipulations, i.e., inserting opsin genes via viral infection and implanting optical fibers, less invasive optogenetic-systems are currently under development (see [38][39][40][41][42] for recent advancements in making optogenetics less or even non-invasive). While it may take years to make optogenetics or optogeneticlike technology a therapeutic memory-modifying measure, 2 if ever to be realized, 3 the fact that MMT has been shown to be effective in deactivating specific memories makes it timely and important to consider potential philosophical 4…”

Section: Introductionmentioning

confidence: 99%

The Ethics of Memory Modification: Personal Narratives, Relational Selves and Autonomy

Zawadzki

2022

Neuroethics

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For nearly two decades, ethicists have expressed concerns that the further development and use of memory modification technologies (MMTs)—techniques allowing to intentionally and selectively alter memories—may threaten the very foundations of who we are, our personal identity, and thus pose a threat to our well-being, or even undermine our “humaneness.” This paper examines the potential ramifications of memory-modifying interventions such as changing the valence of targeted memories and selective deactivation of a particular memory as these interventions appear to be at the same time potentially both most promising clinically as well as menacing to identity. However, unlike previous works discussing the potential consequences of MMTs, this article analyzes them in the context of the narrative relational approach to personal identity and potential issues related to autonomy. I argue that such a perspective brings to light the ethical aspects and moral issues arising from the use of MMTs that have been hidden from previously adopted approaches. In particular, this perspective demonstrates how important the social context in which an individual lives is for the ethical evaluation of a given memory-modifying intervention. I conclude by suggesting that undertaking memory modifications without taking into account the social dimension of a person’s life creates the risk that she will not be able to meet one of the basic human needs—the autonomous construction and maintenance of personal identity. Based on this conclusion, I offer some reflections on the permissibility and advisability of MMTs and what these considerations suggest for the future.

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A Noninvasive Approach to Optogenetics Using Focused Ultrasound Blood Brain Barrier Disruption for the Delivery of Radioluminescent Particles

Cited by 3 publications

References 34 publications

Feasibility of cerium-doped LSO particles as a scintillator for x-ray induced optogenetics

Feasibility of cerium-doped LSO particles as a scintillator for x-ray induced optogenetics

Personality and Authenticity in Light of the Memory-Modifying Potential of Optogenetics: A Reply to Objections about Potential Therapeutic Applicability of Optogenetics

The Ethics of Memory Modification: Personal Narratives, Relational Selves and Autonomy

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