was privileged to deliver the opening keynote at this month’s FediForum, a conference for people building and supporting the open social web. My talk touched on what’s happening now, drew on my experiences building Elgg and Known and investing at Matter Ventures, and gave participants three important questions to ask themselves as they build platforms and serve communities.
Here’s the talk in its entirety, courtesy of FediForum. The transcript [is on the page.]
Miss Major Griffin-Gracy, a legendary transgender activist who had been in the movement since Stonewall, died Monday at age 78.
Her death was announced by the House of GG—Griffin-Gracy Retreat and Educational Center, which she founded. She died “in the comfort of her home and surrounded by loved ones in Little Rock, Arkansas,” says a statement from the center. “Her enduring legacy is a testament to her resilience, activism, and dedication to creating safe spaces for Black trans communities and all trans people — we are eternally grateful for Miss Major’s life, her contributions and how deeply she poured into those she loved.”
Miss Major had suffered from health problems for some time and had recently begun receiving hospice care.She spent more than 50 years fighting for the “trans, gender-nonconforming, and LGB community — especially for Black trans women, trans women of color and those who have survived incarceration and police brutality,” the statement continues. Major’s fierce commitment and intersectional approach to justice brought her to care directly for people with HIV/AIDS in New York in the early 1980s, and later to drive San Francisco’s first mobile needle exchange. As director of the TGI Justice Project, she’d return to prisons as a mentor to her ‘gurls’ inside.”
She founded House of GG in 2019 as “a space for our community to take a break, swim, enjoy good food, laugh, listen to music, watch movies, and recharge for the ongoing fight for our lives,” the statement goes on. “Miss Major fought tirelessly for her people, her love as vast and enduring as the universe she knew herself to be a part of. She was a world builder, a visionary, and unwavering in her devotion to making freedom possible for Black, trans, formerly and currently incarcerated people as well as the larger trans and LGB community. Because of her, countless new possibilities have been made for all of us to thrive — today and for generations to come. She affirmed that our lives hold meaning and that we stand on the shoulders of giants like her, whose courageous love and relentless fight assured our right to live with dignity. We will forever honor her memory, her steadfast presence, and her enduring commitment to our collective liberation.” (snip-MORE good history and story on the page)
As I’ve said before, please feel free to use my cartoons for your posters (just no altering text or images, please). Contact me either in the comments or email for the hi-res file (atelnaes@anntelnaes.com) . Here’s also a few suggestions from my archives if you don’t have a particular one in mind.
Stay safe and be loud with your First Amendment Rights.
UPDATE: Thank you for all your requests and my apologies for not being able to respond to your added kind messages. Even if you’re only getting the attached file, I’ve read and appreciated them all.
***Liza Donnelly and Steve Brodner are both offering their excellent editorial cartoons to download for posters.
(Well, the Science and Art parts, anyway! This is originally a year-old story, republished by Cosmos today. I scouted around for some sort of an update, but didn’t find one. I still thought this is interesting, and at least now we know another area in which A.I. might be applied. I think that’s good to know, since A.I. does make mistakes, as noted below.)
This artwork of an origami bird holds AlphaFold 3 predictions of a complex of two proteins (ScpA and ScpB) in its beak. The protein complex is important during cell division in bacteria. Top: ScpA is cyan and ScpB is green. Bottom: Confidence measures, where dark blue is very high confidence, light blue is confident, yellow is low confidence, and orange is very low confidence in the structural prediction. Credit: AlphaFold 3, Katie Michie.
A protein is made from of a chain of amino acids strung together like beads on a necklace. This chain spontaneously folds, like origami, into intricate pleats, folds, and loops through interactions between its amino acids. The resulting unique 3D structure largely determines its vital function within the lifeform. Solving the structure allows biologists to better understand how the protein works and design experiments to affect and modify it.
The smallest known protein, TAL, influences development of the fruit fly Drosophila melanogaster and has just 11 amino acids. The largest, Titin, is found in human muscle cells and is made up of roughly 35,000.
Proteins are far too tiny to inspect under a regular microscope. For decades researchers used complex experimental techniques, such as X-ray crystallography, nuclear magnetic resonance (NMR) spectroscopy, and cryogenic electron microscopy (cryo-EM) to solve their structures. It’s painstaking, time-consuming work that takes specialised skill and sometimes hundreds of thousands of dollars. And, as Kate Michie can attest, success is not always guaranteed.
“I spent four years trying to solve the crystal structure of a complex of two human proteins and got scooped. You know, I got nothing out of four years. I worked really hard at it, and it was a really difficult project. AlphaFold can calculate those in a few hours,” says Michie, who is chief scientist of the Structural Biology Facility at the Mark Wainwright Analytical Centre, of the University of New South Wales Sydney.
On 8 May 2024 Nature dropped a paper introducing the third and latest iteration of the artificial intelligence (AI) system AlphaFold, which predicts the 3D structure of proteins from their amino acid sequences. Google DeepMind and Isomorphic Labs, both subsidiaries of Alphabet, co-developed the new model. They say AlphaFold 3 (AF3) is “a revolutionary model that can predict the structure and interactions of all life’s molecules with unprecedented accuracy”. But, while AF3 has generated significant interest since its release, it has simultaneously sparked criticism among those in the scientific community.
Let’s take a closer look at how AI is changing the world of structural biology.
A revolution in protein structure
AF3’s predecessor, AlphaFold 2, was released as open source code in July 2021 and immediately changed the game in structural biology.
“I contacted the high-performance computation people and said, ‘we really need to get this piece of code running’. And then I asked my colleague, ‘Do you have any structures that you never submitted to the Protein Data Bank?’” says Michie.
The Protein Data Bank (PDB) is the global archive of all the experimentally solved structures for large biological molecules. As of June 2024, its estimated to include more than 220,000 proteins, which sounds like a lot until you consider the number of proteins we know of exceeds 200 million.
“My colleague sent me a sequence of a small protein he never submitted to the PDB, I ran it, and I just sent him the result. His email response to me was: ‘My mind is blown!’ And he said, ‘I immediately thought someone else must have solved the structure.’”
But they hadn’t, AF2 had accurately predicted the 3D structure of the protein from its amino acid sequence alone. What had taken years to describe experimentally had been done in just a few hours.
AF2 is a deep learning algorithm. In the world of AI that means it simulates the neural networks found in human brains. First, it takes the protein sequence of interest and searches several databases for similar proteins. By comparing these sequences, it can identify areas of similarity and difference to understand how the protein has changed across evolution.
For instance, if two amino acids are in close contact in 3D space then a mutation in one will usually be accompanied by a mutation in the other (to conserve the structure of the protein). But if they are far apart then they tend to evolve independently from each other. Using this to work out the relative positions of the amino acids, AF2 then takes its training on PDB structural data and iteratively constructs a 3D model of the protein’s structure with relatively high accuracy.
Scientists can take advantage of that predicted structure to accelerate their science by doing smarter, more strategic experiments in the laboratory right off the bat. “I’ve done work with some scientists working with immune complexes, and the models coming out of AlphaFold enable them to really trim down the number of animal experiments they do,” says Michie. “So instead of making say 20 CRISPR mice, they only might make two.”
As seen in AlphaFold 3, a structural prediction of Fos and Jun transcription factors with the DNA sequence they bind. The top panel shows the model and confidence data, and the green chart shows the high confidence of them binding to each other. Credit: AlphaFold 3, Katie Michie.
Crystal clues
An accurate AlphaFold structure can also be the crucial missing piece of the puzzle that allows researchers to experimentally solve the structure using X-ray crystallography.
“One of my other colleagues is virologist and he’d been working on a protein that had eluded structural elucidation for 20–30 years. It was from the world’s first known retrovirus,” says Michie.
“The trick of crystallography is you need to know two components of the maths to solve them,” she continues. The diffraction data provided by X-ray crystallography gives you one of those components, but you don’t have the other: the phase.
Traditional methods of obtaining phase information had proved unsuccessful, until Michie suggested using AlphaFold instead.
“Immediately the structure came out. AlphaFold helped him get the crystals but then actually enabled him to phase the structure. It told us that the Alpha Fold model was very good, but it also fixed up this problem in structural biology.”
To Michie, AlphaFold represents a massive step forward: “it’s genuinely the biggest scientific advance in my career”.
“The Alpha Fold model was very good, but it also fixed up this problem in structural biology.”
Predicting the structures of life’s molecules
Proteins don’t exist in a vacuum. They move around, bind to and modify each other, and even form large, complicated complexes.
Peter Czabotar, joint head of the Structural Biology Division at WEHI, the oldest medical research institute in Australia, says one of the early limitations of AF2 was you could only ever get structural predictions of one protein, alone. “Often what you’re interested in is how different proteins will interact with each other. For example, we work on proteins that are involved with cell death and the interactions between those proteins will dictate whether a cell will live or die.”
The gap has since been bridged by other research groups adapting and building upon AF2’s open source code, and with the AlphaFold-Multimer extension in October 2021.
The newest version, AF3, extends upon this capability by predicting interactions of multiple proteins, and nucleic acids (DNA and RNA). It can predict the impact of ions and post-translational modifications – the addition of chemical groups to amino acids – on these molecular systems too. AF3 can also be used to predict how a selection of small molecules called ligands bind to proteins, though this is restricted to ligands that have high-quality experimental data available in the PDB.
“But where the real power is, something that we do a lot of, is in the drug discovery world,” says Czabotar. “And it is extremely powerful for that, potentially, but they haven’t enabled that in the way that it’s released. We’ve done drug discovery against cell death proteins, for example. I can’t take one of the drugs that we’ve worked with and see how it interacts with my target protein, I can only use the [ligands] that they’ve enabled us to use.”
That capability to predict the structure of novel drug molecules interacting with target proteins seems to be restricted to Isomorphic Labs, which was launched in 2021 to pursue commercial drug discovery.
AF3 uses a very different approach for this new suit of predictions: generative AI. After processing the sequence inputs, it assembles its predictions using a diffusion network, the likes of which power AI image generators. According to Isomorphic Labs’ website: “the diffusion process starts with a cloud of atoms, and over many steps converges on its final, most accurate molecular structure”. Diffusion has been applied to protein structure prediction before, for example, in the seminal RoseTTAFold diffusion (RFdiffusion) by the Baker Laboratory at the Institute for Protein Design, the University of Washington.
But generative AI is not without its limitations. AF3 will occasionally produce structures with overlapping atoms (this is physically impossible) or replace a detail of the structure with its mirror image (chemically impossible). As a generative model, it is also prone to hallucinations in which it invents plausible-looking structures – particularly in disordered regions of the protein that lack a stable 3D structure – similarly to how a text to image AI struggles to create realistic-looking hands. In-built confidence measures help to identify when AF3 isn’t so sure about its structural prediction, but ultimately it takes a scientist with understanding of the underlying structural biology to come along and identify what’s gone wrong, and why.
“It’s very, very powerful. But it doesn’t exclude the need to necessarily confirm things experimentally. Whether that is by solving structures themselves or by, for example, testing the structures in some way in an experiment,” says Czabotar.
Concerns about code
In a major departure from AF2, access to the newest iteration of AlphaFold is limited to a web server and for non-commercial research only. “We have various structure-based drug discovery projects and some of them are purely academic, as students, PhDs and honours projects. But we also have had commercial partnerships, because that’s a way to push your discoveries into a clinical setting,” says Czabotar. “So generally, anything that is going to make an impact is done by an academic lab in a commercial partnership. Now, I guess it puts us in a bit of an awkward situation. Even if we could look at our compounds bound to the target [protein], there’s some projects where we won’t be able to do it because, you know, we’ve ticked a box.”
AF3’s accompanying Nature paper was also published without the source code, but with a ‘pseudocode’ instead – a detailed description of what the code can do and how it works. This prompted an open letter to the Editors of Nature, published 16 May and endorsed by more than 1,000 scientists as of June.
The letter raised concerns that “the absence of available code compromises peer review” and that the pseudocode released would “require months of effort to turn into workable code that approximates the performance, wasting valuable time and resources”. Access to the web server was also initially capped at 10 predictions per day, which the letter stated, “restricts the scientific community’s capacity to verify the broad claims of the findings or apply the predictions on a large scale”.
The sentiments appear to have hit home. Shortly after the letter’s release, DeepMind’s Vice President of research, Pushmeet Kohli announced via X that they would double the daily job limit to 20 and are “working on releasing the AF3 model (incl weights) for academic use … within 6 months”.
On 22 May Nature responded in an editorial, stating its reasoning for publishing the paper without code: “the private sector funds most global research and development, and many of the results of such work are not published in peer-reviewed journals. We at Nature think it’s important that journals engage with the private sector and work with its scientists so they can submit their research for peer review and publication.”
In the meantime, other researchers won’t be sitting idly by until the code release at the end of 2024. Already, multiple teams are racing to develop their own open source versions of AlphaFold 3, without any strings attached.
Following public outcry, the Department of Education has reversed its decision to cut funding for students who have both hearing and vision loss, opting instead to reroute grants to an organization that will provide funding to these students.
Following public outcry, the U.S. Department of Education has restored funding for students who have both hearing and vision loss, about a month after cutting it.
But rather than sending the money directly to the four programs that are part of a national network helping students who are deaf and blind, a condition known as deafblindness, the department has instead rerouted the grants to a different organization that will provide funding for those vulnerable students.
The Trump administration targeted the programs in its attacks on diversity, equity and inclusion; a department spokesperson had cited concerns about “divisive concepts” and “fairness” in explaining the decision to withhold the funding.
ProPublica and other news organizations reported last month on the canceled grants to agencies that serve these students in Oregon, Washington and Wisconsin, as well as in five states that are part of a New England consortium.
Programs then appealed to the Education Department to retain their funding, but the appeals were denied. Last week, the National Center on Deafblindness, the parent organization of the agencies that were denied, told the four programs that the Education Department had provided it with additional grant money and the center was passing it on to them.
“This will enable families, schools, and early intervention programs to continue to … meet the unique needs of children who are deafblind,” according to the letter from the organization to the agencies, which was provided to ProPublica. Education Department officials did not respond to questions from ProPublica; automatic email replies cited the government shutdown. (snip-MORE)
The American Federation of Labor (AFL) voted to boycott all German-made products as a protest against Nazi antagonism to organized labor within Germany.
This morning, I was in the backseat of an Uber ride and absentmindedly playing with my lips in the quiet way it’s socially acceptable for grown adults to do (or, perhaps, that’s me rationalizing) when, to my surprise, I accidentally forced too much air through the aperture of my mouth, creating a sound that could understandably be perceived by the driver as a fart.
Mildly panicked, I leapt into action by recreating the sound a few more times in quick succession in order to non-verbally (?) communicate to the driver:
Haha, see? That totally wasn’t what you thought it was! I accidentally made that sound with my lips! I’m now doing it again two or three more times to show that it’s just me playing with my mouth and not doing something very rude right behind you! Actually, making that sound is rude, too — look, I promise I am not blasting ass in the backseat of your car, okay?!
I am 39-years-old today. It’s my final year in this decade. It’s been a doozy.
I turned 30 a little over three weeks before the 2016 election. (I know. We won’t get into that because you already get it.)
All my life, I’ve heard of folks in their late-30s just dreading the big FOUR ZERO, and it’s not my place to judge them. I’m sure they had their reasons.
But me? I’m so ready for my 40s. If I could snap my fingers and make it happen now, I would have turned 40 today. Maybe I’ll just lie and say I’m 40 moving forward.
Being in your 40s sounds awesome. Being in your 50s and 60s sounds even better. I wanna fast-forward and get there already. I want the accumulated wisdom and experience and memories right now. I want that whole toolbox immediately.
Sadly, I cannot have it immediately. That is earned. I must brave the final year of my 30s in our oh-so-stable world to get a little closer to the benefits of being older and wiser.
To that end, I’m gonna make this a great Year 39. I plan to treat it like a final dress rehearsal for the second half of my life.
I’d like y’all to help me get things off to a great start.
Every year, for the past decade, I’ve hosted a birthday fundraiser for my favorite organization Running Start, a non-profit that trains young women in high school and college to run for office someday.
These programs are wide-ranging: from one-day workshops on college campuses (Elect Her) to congressional fellowships to the HBCU Women’s Leadership Summit, thousands of young women have been equipped with necessary skills to go on and do great things in politics, law, advocacy, and media.
I’ve served on the Board of Running Start since 2021, working harmoniously alongside my colleagues—Democrats and Republicans and independents—to ensure the next generation of young women get an exceptional head start toward leading our country someday.
In that time, I have seen a huge, diverse network of alums directly benefit from these programs and then watch as their campuses and communities benefit from them, too.
And believe me, I get it, everyone and their mother and their cousin is hitting y’all up for money right now — for that campaign or that non-profit or that candidate or that cause and on and on.
Thus, I am grateful for the consideration. It means a lot. I am thankful.
As always, those making very generousdonations ($250 or more) should know you’ll be getting a phone call from me to thank you for your generosity, and if you really wanna go above and beyond ($1000 or more), that’ll mean coffee over zoom OR me treating you to lunch here in D.C. (or wherever you live if we can make it happen — no kidding, we will find a way.)
But also: everyone donating will get a personal email from me thanking them because every donation, no matter how much, means something to me and the young women who benefit from Running Start’s programs.
In the meantime, please wish me luck on this final lap of my 30s, and if you could offer up a prayer that I’ll avoid embarrassing sounds in cars, I’d appreciate that, too.
October 12, 1492 Natives of islands off the Atlantic shore of North America came upon Italian explorer Christopher Columbus, who was searching for a water route to India for Spanish Queen Isabella.
October 12, 1945 Pfc. Desmond Doss became the first conscientious objector ever to be awarded the Congressional Medal of Honor. Doss, a Seventh Day Adventist, enlisted in 1942 but refused to carry a rifle or train on Saturdays. On the island of Okinawa, under heavy Japanese fire, he saved the lives of 75 sick and wounded soldiers by lowering them, one by one, down a 400-foot cliff. The guest house at Walter Reed Army Medical Center is Doss Memorial Hall in his honor. Read more (includes movie trailer)
October 12, 1958 A Reform Jewish Temple in Atlanta (the city’s oldest) was firebombed with fifty sticks of dynamite in retaliation for Jewish support of local black civil rights activists. The Temple’s Rabbi, Jacob Rothschild, was outspoken in his support of civil rights and integration, and was a friend of Reverend Martin Luther King, Jr. before he became well known nationally. From Georgia PBS
October 12, 1967 British zoologist Desmond Morris stunned the world with his book, “The Naked Ape,” a frank study of human behavior from a zoologist’s perspective. Morris had earlier studied the artistic abilities of apes and was appointed Curator of Mammals at the London Zoo. Read more
October 12, 1967 “A Call to Resist Illegitimate Authority” appeared in The Nation and the New York Review of Books. 20,000 signed it, including academics, clergymen, writers. It urged “that every free man has a legal right and a moral duty to exert every effort to end this war [Vietnam], to avoid collusion with it, and to encourage others to do the same.” This document became the main basis for the federal government’s criminal prosecution (for encouraging draft evasion) of five of the signers: Dr. Benjamin Spock, Marcus Raskin, Mitchell Goodman, Michael Ferber, and the Reverend William Sloane Coffin. Read the Call
October 12, 1970 Lt. William Calley was court-martialled for the massacre of 102 civilians in the Vietnamese village of My Lai; far more actually died during the incident. The full sad story Lt. Calley
October 12, 1977 “Regents of the University of California v. Bakke” was argued in front of the U.S. Supreme Court. The question: Did the University of California violate the Fourteenth Amendment’s equal protection clause, and the Civil Rights Act of 1964, by practicing an affirmative action policy that resulted in the repeated rejection of Bakke’s application for admission to its medical school? Read more
Scottie's Playtime 