Tag Archives: cryo-electron microscopy (cryo-EM)

Visualization of RNA structures at near-atomic resolution enabled by nanotechnology

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The illustration that accompanies the research is both fascinating and baffling as its caption,

Caption: This illustration is inspired by the Paleolithic rock painting in the Lascaux cave, signifying the acronym of our method, ROCK. Figuratively, the patterns of the rock art in the background (brown) are the 2D projections of the engineered dimeric construct of the Tetrahymena group I intron, while the main object in the front (blue) is the reconstructed 3D cryo-EM map of the dimer, with one monomer in focus and refined to the high resolution that allowed the collaborators to build an atomic model of the RNA. Credit: Wyss Institute at Harvard University

This May 2, 2022 news item on ScienceDaily announces the research into RNA molecules made possible by ROCK (the technology being illustrated in the above),

We live in a world made and run by RNA [ribonucleic acid], the equally important sibling of the genetic molecule DNA. In fact, evolutionary biologists hypothesize that RNA existed and self-replicated even before the appearance of DNA and the proteins encoded by it. Fast forward to modern day humans: science has revealed that less than 3% of the human genome is transcribed into messenger RNA (mRNA) molecules that in turn are translated into proteins. In contrast, 82% of it is transcribed into RNA molecules with other functions many of which still remain enigmatic.

To understand what an individual RNA molecule does, its 3D structure needs to be deciphered at the level of its constituent atoms and molecular bonds. Researchers have routinely studied DNA and protein molecules by turning them into regularly packed crystals that can be examined with an X-ray beam (X-ray crystallography) or radio waves (nuclear magnetic resonance). However, these techniques cannot be applied to RNA molecules with nearly the same effectiveness because their molecular composition and structural flexibility prevent them from easily forming crystals.

Now, a research collaboration led by Wyss Core Faculty member Peng Yin, Ph.D. at the Wyss Institute for Biologically Inspired Engineering at Harvard University, and Maofu Liao, Ph.D. at Harvard Medical School (HMS), has reported a fundamentally new approach to the structural investigation of RNA molecules. ROCK, as it is called, uses an RNA nanotechnological technique that allows it to assemble multiple identical RNA molecules into a highly organized structure, which significantly reduces the flexibility of individual RNA molecules and multiplies their molecular weight. Applied to well-known model RNAs with different sizes and functions as benchmarks, the team showed that their method enables the structural analysis of the contained RNA subunits with a technique known as cryo-electron microscopy (cryo-EM). Their advance is reported in Nature Methods.

A May 2, 2022 Wyss Institute for Biologically Inspired Engineering at Harvard University news release (also on EurekAlert) by Benjamin Boettner, which originated the news item, delves further into the imaging technology, Note: Links have been removed,

“ROCK is breaking the current limits of RNA structural investigations and enables 3D structures of RNA molecules to be unlocked that are difficult or impossible to access with existing methods, and at near-atomic resolution,” said Yin, who together with Liao led the study. “We expect this advance to invigorate many areas of fundamental research and drug development, including the burgeoning field of RNA therapeutics.” Yin also is a leader of the Wyss Institute’s Molecular Robotics Initiative and Professor in the Department of Systems Biology at HMS.

Gaining control over RNA

Yin’s team at the Wyss Institute has pioneered various approaches that enable DNA and RNA molecules to self-assemble into large structures based on different principles and requirements, including DNA bricks and DNA origami. They hypothesized that such strategies could also be used to assemble naturally occurring RNA molecules into highly ordered circular complexes in which their freedom to flex and move is highly restricted by specifically linking them together. Many RNAs fold in complex yet predictable ways, with small segments base-pairing with each other. The result often is a stabilized “core” and “stem-loops” bulging out into the periphery. 

“In our approach we install ‘kissing loops’ that link different peripheral stem-loops belonging to two copies of an identical RNA in a way that allows a overall stabilized ring to be formed, containing multiple copies of the RNA of interest,” said Di Liu, Ph.D., one of two first-authors and a Postdoctoral Fellow in Yin’s group. “We speculated that these higher-order rings could be analyzed with high resolution by cryo-EM, which had been applied to RNA molecules with first success.”

Picturing stabilized RNA

In cryo-EM, many single particles are flash-frozen at cryogenic temperatures to prevent any further movements, and then visualized with an electron microscope and the help of computational algorithms that compare the various aspects of a particle’s 2D surface projections and reconstruct its 3D architecture. Peng and Liu teamed up with Liao and his former graduate student François Thélot, Ph.D., the other co-first author of the study. Liao with his group has made important contributions to the rapidly advancing cryo-EM field and the experimental and computational analysis of single particles formed by specific proteins.

“Cryo-EM has great advantages over traditional methods in seeing high-resolution details of biological molecules including proteins, DNAs and RNAs, but the small size and moving tendency of most RNAs prevent successful determination of RNA structures. Our novel method of assembling RNA multimers solves these two problems at the same time, by increasing the size of RNA and reducing its movement,” said Liao, who also is Associate Professor of Cell Biology at HMS. “Our approach has opened the door to rapid structure determination of many RNAs by cryo-EM.” The integration of RNA nanotechnology and cryo-EM approaches led the team to name their method “RNA oligomerization-enabled cryo-EM via installing kissing loops” (ROCK).

To provide proof-of-principle for ROCK, the team focused on a large intron RNA from Tetrahymena, a single-celled organism, and a small intron RNA from Azoarcus, a nitrogen-fixing bacterium, as well as the so-called FMN riboswitch. Intron RNAs are non-coding RNA sequences scattered throughout the sequences of freshly-transcribed RNAs and have to be “spliced” out in order for the mature RNA to be generated. The FMN riboswitch is found in bacterial RNAs involved in the biosynthesis of flavin metabolites derived from vitamin B2. Upon binding one of them, flavin mononucleotide (FMN), it switches its 3D conformation and suppresses the synthesis of its mother RNA.  

“The assembly of the Tetrahymena group I intron into a ring-like structure made the samples more homogenous, and enabled the use of computational tools leveraging the symmetry of the assembled structure. While our dataset is relatively modest in size, ROCK’s innate advantages allowed us to resolve the structure at an unprecedented resolution,” said Thélot. “The RNA’s core is resolved at 2.85 Å [one Ångström is one ten-billions (US) of a meter and the preferred metric used by structural biologists], revealing detailed features of the nucleotide bases and sugar backbone. I don’t think we could have gotten there without ROCK – or at least not without considerably more resources.” 

Cryo-EM also is able to capture molecules in different states if they, for example, change their 3D conformation as part of their function. Applying ROCK to the Azoarcus intron RNA and the FMN riboswitch, the team managed to identify the different conformations that the Azoarcus intron transitions through during its self-splicing process, and to reveal the relative conformational rigidity of the ligand-binding site of the FMN riboswitch.

“This study by Peng Yin and his collaborators elegantly shows how RNA nanotechnology can work as an accelerator to advance other disciplines. Being able to visualize and understand the structures of many naturally occurring RNA molecules could have tremendous impact on our understanding of many biological and pathological processes across different cell types, tissues, and organisms, and even enable new drug development approaches,” said Wyss Founding Director Donald Ingber, M.D., Ph.D., who is also the Judah Folkman Professor of Vascular Biology at Harvard Medical School and Boston Children’s Hospital, and Professor of Bioengineering at the Harvard John A. Paulson School of Engineering and Applied Sciences.

The study was also authored by Joseph Piccirilli, Ph.D., an expert in RNA chemistry and biochemistry and Professor at The University of Chicago. It was supported by the National Science Foundation (NSF; grant# CMMI-1333215, CCMI-1344915, and CBET-1729397), Air Force Office of Scientific Research (AFOSR; grant MURI FATE, #FA9550-15-1-0514), National Institutes of Health (NIH; grant# 5DP1GM133052, R01GM122797, and R01GM102489), and the Wyss Institute’s Molecular Robotics Initiative.

Here’s a link to and a citation for the paper,

Sub-3-Å cryo-EM structure of RNA enabled by engineered homomeric self-assembly by Di Liu, François A. Thélot, Joseph A. Piccirilli, Maofu Liao & Peng Yin. Nature Methods (2022) DOI: https://doi.org/10.1038/s41592-022-01455-w Published: 02 May 2022

This paper is behind a paywall.

Two new Canada Excellence Research Chairs (CERC) at the University of British Columbia (Canada) bring bioproducts and precision medicine skills

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This is very fresh news. One of these chairs has not yet been listed (at the time of this writing) as a member of the institute that he will be leading. Here’s the big picture news from an
April 17, 2019 University of British Columbia (UBC) news release, Note: Links have been removed,

Two internationally recognized researchers join the University of British Columbia as Canada Excellence Research Chairs, bringing international talent in the fields of forest bioproducts and precision cancer drug design.

Orlando Rojas has accepted the Canada Excellence Research Chair in Forest Bioproducts, while Sriram Subramaniam will hold the Gobind Khorana Canada Excellence Research Chair in Precision Cancer Drug Design—named after late Nobel Prize-winning UBC biochemistry professor Har Gobind Khorana.

“We are delighted to welcome Dr. Rojas and Dr. Subramaniam to UBC,” said UBC President and Vice-Chancellor, Professor Santa J. Ono. “Thanks to the CERC program and the generous support of our partners, including VGH & UBC Hospital Foundation, we have an opportunity to continue to build on UBC’s reputation as a global leader in these vitally important research fields.”

The Canada Excellence Research Chairs (CERC) program was established by the federal government in 2008 to attract top research talent from abroad to Canada. UBC will receive up to $10 million over seven years to support each chair and their research teams. In addition, a philanthropic gift of $18 million made to VGH & UBC Hospital Foundation will support cancer drug design that will be carried out by Subramaniam in close partnership with UBC and the Vancouver Prostate Centre at VGH.

“VGH & UBC Hospital Foundation is honoured to announce an $18 million gift from Aqueduct Foundation on behalf of an anonymous donor that will increase capacity for discovering and testing new life-saving cancer treatments right here in B.C. This funding will specifically support the design of precise, targeted and cost-effective drugs for cancer in work led by Dr. Sriram Subramaniam in close partnership with UBC and the Vancouver Prostate Centre at VGH and other research centres,” says Barbara Grantham, president and CEO of VGH & UBC Hospital Foundation.

Bioproducts

The April 17, 2019 UBC news release, goes on to describe the two new chairs,

Breaking new ground in forest bioproducts

Orlando Rojas comes to UBC from Aalto University [Finland], where he directs with VTT, the Technical Research Centre of Finland, a scientific cluster to advance the Finnish materials bio-economy. A recipient of the Anselme Payen Award—one of the highest international recognitions in the area of cellulose and renewable materials—and an elected member of the American Chemical Society and the Finnish Academy of Science and Letters, Rojas is recognized as a worldwide leader in the area of nanocelluloses.

“I’m thrilled to join an already stellar team of researchers at UBC’s BioProducts Institute,” said Rojas. “My research is aimed at uncovering solutions that can be found in nature to fulfill our material needs by using sustainably, readily available bio-resources. I hope to break new grounds to create positive societal impacts and to better our quality of life.”

As the CERC in Forest Bioproducts, Rojas will establish a world-class research program in genomics, synthetic biology, materials science and engineering. Together with his team and by applying cutting-edge nano- and biotechnologies, he will discover new strategies to isolate and transform biomass components—non-fossil organic materials derived from plants (including wood)—as well as side-streams and residuals from forestry and agriculture, oils and biomolecules. The work will lead to the generation of new bio-based precursors and advanced materials critical to the future bioeconomy. Rojas will be the scientific director of the UBC BioProducts Institute, synergizing a distinguished group of professors and researchers across campus who will conduct multi- and cross-disciplinary research that will position UBC at the forefront in the area.

As climate change continues to be the greatest threat to our world, the need to transition toward a more sustainable bio-based circular economy is critical. Rojas’ research is vital in understanding the role of forest and other plant-based resources in facilitating the transition to renewable materials and bioproducts.

As I noted earlier, Rojas has yet to be added to the UBC BioProducts Institute roster but I did find a listing of his published papers on Google Scholar and noted a number of them are focused on nanocellulose with at least one study on cellulose nanocrystals (CNC),

  • Cellulose nanocrystals: chemistry, self-assembly, and applications [by] Y Habibi, LA Lucia, OJ Rojas Chemical reviews 110 (6), 3479-3500

The University of British Columbia was the site for much of the early work in Canada and internationally on cellulose nanocrystals. After the provincial government lost interest in supporting it, the researchers at FPInnovations (I think it was a university spin-off organization) moved their main headquarters (leaving a smaller group in British Columbia) to the province of Québec where they receive significant support . In turn, FPInnovations spun-off a company, CelluForce which produces CNC from forest products.This news about Roja’s appointment would seem to make for an interesting development in Canada’s nanocellulose story.

Precision medicine with cryo-electron microscopy

Now for the second CERC appointment, from the April 17, 2019 UBC news release,

Putting Canada at the forefront of precision medicine

Sriram Subramaniam is recognized as a global leader in the emerging field of cryo-electron microscopy, or cryo-EM, a technology that has sparked a revolution in imaging of protein complexes. Subramaniam and his team demonstrated that proteins and protein-bound drugs could be visualized at atomic resolution with cryo-EM, paving the way for this technology to be used in accelerating drug discovery.

Subramaniam comes to UBC’s faculty of medicine from the US National Cancer Institute (NCI) at the National Institutes of Health (NIH) where he led a research team that made seminal advances in molecular and cellular imaging using electron microscopy, including work on advancing vaccine design for viruses such as HIV. Subramaniam is also founding director of the National Cryo-EM Program at NCI, NIH.

As the Gobind Khorana Canada Excellence Research Chair in Precision Cancer Drug Design, Subramaniam will establish and direct a laboratory located at UBC, aimed at bringing about transformative discoveries in cancer, neuroscience and infectious disease. Subramaniam is appointed both in the department of urologic sciences and in biochemistry and molecular biology at UBC, and is linked to the precision cancer drug design program at the Vancouver Prostate Centre at VGH.

His research is supported by a philanthropic gift of $18 million made to VGH & UBC Hospital Foundation. He will work in close partnership with the Vancouver Prostate Centre at VGH.

“We would not be able to undertake this path aimed at leveraging advances in imaging technology to improve patient outcomes if it weren’t for the generous support of the donor, the Canadian government, and VGH & UBC Hospital Foundation,” said Subramaniam. “I am proud to be part of a team of outstanding researchers here in Vancouver, and working together to harness the true potential of cryo-EM to accelerate drug design. Our work has the potential to establish VGH, UBC and Canada at the forefront of the emerging era of precision medicine.”

I was not able to find much in the way of additional information about Subramaniam—other than this (from the High Resolution Electron Microscopy Lab Members webpage),

Sriram Subramaniam received his Ph.D. in Physical Chemistry from Stanford University and completed postdoctoral training in the Departments of Chemistry and Biology at M.I.T. [Massachusetts Institute of Technology] He is chief of the Biophysics Section in the Laboratory of Cell Biology at the Center for Cancer Research, National Cancer Institute. He holds a visiting faculty appointment at the Johns Hopkins University School of Medicine.

Welcome to both Orlando J. Rohas and Sriram Subramaniam!