In vivo photocontrol of microtubule dynamics and integrity, migration and mitosis, by the potent GFP-imaging-compatible photoswitchable reagents SBTubA4P and SBTub2M

Gao, Li; Meiring, Joyce; Varady, Adam; Ruider, Iris E; Heise, Constanze; Wranik, Maximilian; Velasco, Cecilia D.; Taylor, Jennifer A.; Terni, Beatrice; Standfuss, Jörg; Cabernard, Clemens; Llobet, Artur; Steinmetz, Michel O.; Bausch, Andreas R.; Distel, Martin; Ahlfeld, Julia; Akhmanova, Anna; Thorn‐Seshold, Oliver

doi:10.1101/2021.03.26.437160

Cited by 11 publications

(31 citation statements)

References 59 publications

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“…The most powerful SBTubs are the highly potent cosolvent-requiring SBTub2M, and slightly less potent but buffersoluble SBTubA4P [9]. These replace first generation SBTub3 and SBTub3P [7].…”

Section: Choosing Inhibitors For Photoswitching-based Optical Control Of Mtsmentioning

confidence: 99%

“…Drug Scaffolds: Pharmaceuticals that have already been used as part of MT-inhibiting photopharmaceuticals include taxol [14] and epothilone [13] for MT-stabilising photopharmaceuticals AzTax and STEpo; and colchicinoids (analogues of colchicine-binding-site drugs like colchicine, colcemid, nocodazole or combretastatin) have been used in MT-destabilising photopharmaceuticals e.g. PST, SBTub and PHTub (Fig 5) [2,7,9,15,23,24]. where the photoswitchable bond is inside the overall binding motif.…”

Section: Notesmentioning

confidence: 99%

“…5-10 min presumably due to hindered access to the medium. SBTubs have been used also for temporally precise blockage of development in frog; and cell-precise targeting of anti-migration and antimitotic effects over 24 hours in organoid cultures in a matrix [9]. SBTubs have shown some ability to apply subcellularly-localised effects in large neurons [7].…”

Section: Note 13 Uses Of Sbtubs and Psts In Vivomentioning

confidence: 99%

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Photocontrolling Microtubule Dynamics with Photoswitchable Chemical Reagents

Thorn‐Seshold

Meiring²

2021

Preprint

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Microtubule dynamics can be inhibited with sub-second temporal resolution and cellular-scale spatial resolution, by using precise illuminations to optically pattern where and when photoswitchable microtubule-inhibiting chemical reagents exert their latent bioactivity. The recently-available reagents (SBTub, PST, STEpo, AzTax, PHTub) now enable researchers to use light to reversibly modulate microtubule-dependent processes in eukaryotes, in 2D and 3D cell culture as well as in vivo, across a variety of model organisms: with applications in fields from cargo transport to cell migration, cell division, and embryonic development. However, a wide knowledge gap has remained in the literature, which has blocked further translation of these and many other classes of photopharmaceuticals. No generally-applicable procedures or workflows to establish biological assays using photopharmaceuticals have been published. Accordingly, the rate of adoption of photopharmaceutical tools in the broader chemical biology community (beyond the original chemical developers of the tools) has remained very low. Vital information about assay benchmarking for photoconversion, testing for isomer solubility, proving the retention of mechanism of action, estimating the limits of phototoxicity etc has either simply not been formalised in the literature, or has remained buried in diverse reports without being unified and codified for an audience beyond that of synthetic organic chemists. Here we have developed a robust four-step assay establishment procedure to optimise assay parameters for achieving reliable photocontrol over microtubule dynamics, that is applicable to diverse families of photoswitchable inhibitors. This procedure also controls for these common sources of irreproducibility and includes numerous troubleshooting steps. We also collect together the relevant information for non-chemist "users" such as microscopists and biologists, to introduce the theory of small molecule photoswitching; the unique features, usage requirements, and limitations that photoswitchable chemical reagents have; and the specific performance features of the major classes of photoswitchable microtubule inhibitors that are currently available; to highlight their properties that suit them to different applications. The generally-applicable workflows that we present allow establishing cellular assays optically controlling microtubule dynamics in a temporally reversible fashion with spatial specificity down to a single selected cell within a field of view. These workflows and methods also equip the reader to tackle advanced uses of photoswitchable chemical reagents for general protein targets, in 3D culture and in vivo, and can represent an important bridge to reach the high-value biological applications that photopharmacology can promise.

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“…The most powerful SBTubs are the highly potent cosolvent-requiring SBTub2M, and slightly less potent but buffersoluble SBTubA4P [9]. These replace first generation SBTub3 and SBTub3P [7].…”

Section: Choosing Inhibitors For Photoswitching-based Optical Control Of Mtsmentioning

confidence: 99%

Section: Notesmentioning

confidence: 99%

Section: Note 13 Uses Of Sbtubs and Psts In Vivomentioning

confidence: 99%

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Photocontrolling Microtubule Dynamics with Photoswitchable Chemical Reagents

Thorn‐Seshold

Meiring²

2021

Preprint

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“…GFP-orthogonality is also needed to keep imaging channels free for the multiplexed readouts that are increasingly standard in cutting-edge research. 23 (2) The SBT's C=C chromophore is ideally situated for efficient photoswitching at 405 nm or 442 nm, so matching the typical photoactivation lasers installed in microscope -again a crucial feature for practical impact. (3) SBT is highly metabolically stable, and avoids biochemical photoswitch scission.…”

Section: Introductionmentioning

confidence: 99%

“…Taken together, these advantages of the SBTs proved crucial in allowing SBTubs to succeed as MT photoswitches in tissue and animal applications across a variety of animal models, while photopharmaceuticals based on the other photoswitches have not generally succeeded in moving beyond 2D cell culture or early embryo applications. 23 We were therefore motivated to bring the powerful advantages of the SBT photoswitch to bear on the attractive class of microtubule stabilisers, to generate novel optically-controlled MT-stabilisers with improved practical applicability and scope. We now report the development of such GFP-orthogonal photopharmaceutical MT stabilisers, based on epothilone (Fig 1b).…”

Section: Introductionmentioning

confidence: 99%

Photoswitchable epothilone-based microtubule stabilisers allow GFP-imaging-compatible, optical control over the microtubule cytoskeleton

Gao

Meiring

Heise

et al. 2021

Preprint

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Optical methods to modulate microtubule stability and dynamics are promising approaches to reach the micron- and millisecond-scale resolution needed to decrypt the diverse roles of the microtubule cytoskeleton in biology. However, such optical methods have until now focussed nearly exclusively on microtubule destabilisation. Here, we introduce "STEpos" as light-responsive epothilone reagents, designed to photoswitchably bind to tubulin and stabilise lateral contacts in the microtubule lattice. Using a novel styrylthiazole photoswitch, designed to allow the hydrogen-bonding that is key to epothilone potency, we have created the first set of GFP-orthogonal photoswitchable microtubule stabilisers. The STEpos can photocontrol microtubule polymerisation, cell division, and cellular microtubule dynamics with micron- and second-scale spatiotemporal precision. STEpos offer substantial improvements of potency, solubility, and ease-of-use compared to the only previous photopharmaceuticals for microtubule stabilisation. The intriguing structure-photoswitching activity relationship insights from this work will also assist future developments of improved STEpo reagents, and we anticipate that these will contribute greatly to high-precision cytoskeleton research across the fields of biophysics, cargo transport, cell motility, cell division, development, and neuroscience.

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Photoswitchable Cytotoxins

Thorn‐Seshold

2022

Molecular Photoswitches

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In vivo photocontrol of microtubule dynamics and integrity, migration and mitosis, by the potent GFP-imaging-compatible photoswitchable reagents SBTubA4P and SBTub2M

Cited by 11 publications

References 59 publications

Photocontrolling Microtubule Dynamics with Photoswitchable Chemical Reagents

Photocontrolling Microtubule Dynamics with Photoswitchable Chemical Reagents

Photoswitchable epothilone-based microtubule stabilisers allow GFP-imaging-compatible, optical control over the microtubule cytoskeleton

Photoswitchable Cytotoxins

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