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An astronomical waltz reveals a sextuplet of planets

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An astronomical waltz reveals a sextuplet of planets


An international collaboration between astronomers using the CHEOPS and TESS space satellites, including NCCR PlanetS members from the University of Bern and the University of Geneva, have found a key new system of six transiting planets orbiting a bright star in a harmonic rhythm. This rare property enabled the team to determine the planetary orbits which initially appeared as an unsolvable riddle.

CHEOPS is a joint mission by ESA and Switzerland, under the leadership of the University of Bern in collaboration with the University of Geneva. Thanks to a collaboration with scientists working with data from NASA’s satellite TESS, the international team could uncover the planetary system orbiting the nearby star HD110067. A very distinctive feature of this system is its chain of resonances: the planets orbit their host star in perfect harmony. Part of the research team are researchers from the University of Bern and the University of Geneva who are also members of the National Center of Competence in Research (NCCR) PlanetS. The findings have just been published in Nature.

The planets in the HD110067 system revolve around the star in a very precise waltz. When the closest planet to the star makes three full revolutions around it, the second one makes exactly two during the same time. This is called a 3:2 resonance. “Amongst the over 5000 exoplanets discovered orbiting other stars than our Sun, resonances are not rare, nor are systems with several planets. What is extremely rare though, is to find systems where the resonances span such a long chain of six planets” points out Dr. Hugh Osborn, CHEOPS fellow at the University of Bern, leader of CHEOPS observation programme involved in the study, and co-author of the publication. This is precisely the case of HD110067 whose planets form a so-called “resonant chain” in successive pairs of 3:2, 3:2, 3:2, 4:3, and 4:3 resonances, resulting in the closest planet completing six orbits while the outer-most planet does one.

A seemingly unsolvable puzzle

Although multiple planets were initially detected thanks to their transits, the exact arrangement of the planets was unclear at first. However, the precise gravitational dance enabled the scientists’ team to solve the puzzle of HD110067. Prof. Adrien Leleu from the University of Geneva, in charge of analysing the orbital resonances, and co-author of the study, explains: “A transit occurs when a planet, from our point of view, passes in front of its host star, blocking a minute fraction of the starlight, creating an apparent dip of its brightness.” From the first observations carried out by NASA’s TESS satellite, it was possible to determine that the two inner planets called ‘b’ and ‘c’ have orbital periods of 9 and 14 days respectively. However, no conclusions could be drawn for the other four detected planets as two were seen to transit once in 2020 and once in 2022 with a large 2-year gap in the data, and the other two transited only once in 2022.

The solution to the puzzle for those four additional planets finally began to emerge thanks to observations with the CHEOPS space telescope. While TESS aims at scanning all of the sky bit by bit to find short-period exoplanets, CHEOPS is a targeted mission, focusing on a single star at a time with exquisite precision. “Our CHEOPS observations enabled us to find that the period of planet ‘d’ is 20.5 days. Also, it ruled out multiple possibilities for the remaining three outer planets, ‘e’, ‘f’ and ‘g’,” reveals Osborn.

Predicting the precise waltz of the planets

That is when the team realized that the three inner planets of HD110067 are dancing in a precise 3:2, 3:2 chain of resonances: when the innermost planet revolves nine times around the star, the second revolves six times and the third planet four times.

The team then considered the possibility that the three other planets could also be part of the chain of resonances. “This led to dozens of possibilities for their orbital period,” explains Leleu, “but combining existing observational data from TESS and CHEOPS, with our model of the gravitational interactions between the planets, we could exclude all solutions but one: the 3:2, 3:2, 3:2, 4:3, 4:3 chain.” The scientists could therefore predict that the outer three planets (‘e’, ‘f’ and ‘g’) have orbital periods of 31, 41 days, and 55 days.

This prediction allowed to schedule observations with a variety of ground-based telescopes. Further transits of planet ‘f’ were observed, revealing it was precisely where theory predicted it based on the resonant-chain. Finally, reanalysis of the data from TESS revealed two hidden transits, one from each of planets ‘f’ and ‘g’, exactly at the times expected by the predictions, confirming the periods of the six planets. Additional CHEOPS observations of each planet, and in particular planet ‘e’ are scheduled in the near future.

A key system for the future

From the handful of resonant-chain systems found so far, CHEOPS has highly contributed to the understanding of not only HD110067, but also of TOI-178. Another well-known example of a resonant-chain system is the TRAPPIST-1 system which hosts seven rocky planets. However, TRAPPIST-1 is a small and incredibly faint star which makes any additional observations very difficult. HD110067, on the other hand, is more than 50 times brighter than TRAPPIST-1.

“The fact that the planets in the HD110067 system have been detected by the transit method is key. While they pass in front of the star, light also filters through the planetary atmospheres” points out Jo Ann Egger, PhD student at the University of Bern, who computed the composition of the planets using CHEOPS data, and co-author of the study. This property is allowing astronomers to determine the chemical composition and other properties of the atmospheres. Since a lot of light is required, the bright star HD110067 and its orbiting planets are an ideal target for further studies to charachterize the planetary atmospheres. “The sub-Neptune planets of the HD110067 system appear to have low masses, suggesting they may be gas- or water-rich. Future observations, for example with the James Webb Space Telescope (JWST), of these planetary atmospheres could determine whether the planets have rocky or water-rich interior structures,” concludes Egger.



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‘Dancing molecules’ heal cartilage damage

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In November 2021, Northwestern University researchers introduced an injectable new therapy, which harnessed fast-moving “dancing molecules,” to repair tissues and reverse paralysis after severe spinal cord injuries.

Now, the same research group has applied the therapeutic strategy to damaged human cartilage cells. In the new study, the treatment activated the gene expression necessary to regenerate cartilage within just four hours. And, after only three days, the human cells produced protein components needed for cartilage regeneration.

The researchers also found that, as the molecular motion increased, the treatment’s effectiveness also increased. In other words, the molecules’ “dancing” motions were crucial for triggering the cartilage growth process.

The study was published today (July 26) in the Journal of the American Chemical Society.

“When we first observed therapeutic effects of dancing molecules, we did not see any reason why it should only apply to the spinal cord,” said Northwestern’s Samuel I. Stupp, who led the study. “Now, we observe the effects in two cell types that are completely disconnected from one another — cartilage cells in our joints and neurons in our brain and spinal cord. This makes me more confident that we might have discovered a universal phenomenon. It could apply to many other tissues.”

An expert in regenerative nanomedicine, Stupp is Board of Trustees Professor of Materials Science and Engineering, Chemistry, Medicine and Biomedical Engineering at Northwestern, where he is founding director of the Simpson Querrey Institute for BioNanotechnology and its affiliated center, the Center for Regenerative Nanomedicine. Stupp has appointments in the McCormick School of Engineering, Weinberg College of Arts and Sciences and Feinberg School of Medicine. Shelby Yuan, a graduate student in the Stupp laboratory, was primary author of the study.

Big problem, few solutions

As of 2019, nearly 530 million people around the globe were living with osteoarthritis, according to the World Health Organization. A degenerative disease in which tissues in joints break down over time, osteoarthritis is a common health problem and leading cause of disability.

In patients with severe osteoarthritis, cartilage can wear so thin that joints essentially transform into bone on bone — without a cushion between. Not only is this incredibly painful, patients’ joints also can no longer properly function. At that point, the only effective treatment is a joint replacement surgery, which is expensive and invasive.

“Current treatments aim to slow disease progression or postpone inevitable joint replacement,” Stupp said. “There are no regenerative options because humans do not have an inherent capacity to regenerate cartilage in adulthood.”

What are ‘dancing molecules’?

Stupp and his team posited that “dancing molecules” might encourage the stubborn tissue to regenerate. Previously invented in Stupp’s laboratory, dancing molecules are assemblies that form synthetic nanofibers comprising tens to hundreds of thousands of molecules with potent signals for cells. By tuning their collective motions through their chemical structure, Stupp discovered the moving molecules could rapidly find and properly engage with cellular receptors, which also are in constant motion and extremely crowded on cell membranes.

Once inside the body, the nanofibers mimic the extracellular matrix of the surrounding tissue. By matching the matrix’s structure, mimicking the motion of biological molecules and incorporating bioactive signals for the receptors, the synthetic materials are able to communicate with cells.

“Cellular receptors constantly move around,” Stupp said. “By making our molecules move, ‘dance’ or even leap temporarily out of these structures, known as supramolecular polymers, they are able to connect more effectively with receptors.”

Motion matters

In the new study, Stupp and his team looked to the receptors for a specific protein critical for cartilage formation and maintenance. To target this receptor, the team developed a new circular peptide that mimics the bioactive signal of the protein, which is called transforming growth factor beta-1 (TGFb-1).

Then, the researchers incorporated this peptide into two different molecules that interact to form supramolecular polymers in water, each with the same ability to mimic TGFb-1. The researchers designed one supramolecular polymer with a special structure that enabled its molecules to move more freely within the large assemblies. The other supramolecular polymer, however, restricted molecular movement.

“We wanted to modify the structure in order to compare two systems that differ in the extent of their motion,” Stupp said. “The intensity of supramolecular motion in one is much greater than the motion in the other one.”

Although both polymers mimicked the signal to activate the TGFb-1 receptor, the polymer with rapidly moving molecules was much more effective. In some ways, they were even more effective than the protein that activates the TGFb-1 receptor in nature.

“After three days, the human cells exposed to the long assemblies of more mobile molecules produced greater amounts of the protein components necessary for cartilage regeneration,” Stupp said. “For the production of one of the components in cartilage matrix, known as collagen II, the dancing molecules containing the cyclic peptide that activates the TGF-beta1 receptor were even more effective than the natural protein that has this function in biological systems.”

What’s next?

Stupp’s team is currently testing these systems in animal studies and adding additional signals to create highly bioactive therapies.

“With the success of the study in human cartilage cells, we predict that cartilage regeneration will be greatly enhanced when used in highly translational pre-clinical models,” Stupp said. “It should develop into a novel bioactive material for regeneration of cartilage tissue in joints.”

Stupp’s lab is also testing the ability of dancing molecules to regenerate bone — and already has promising early results, which likely will be published later this year. Simultaneously, he is testing the molecules in human organoids to accelerate the process of discovering and optimizing therapeutic materials.

Stupp’s team also continues to build its case to the Food and Drug Administration, aiming to gain approval for clinical trials to test the therapy for spinal cord repair.

“We are beginning to see the tremendous breadth of conditions that this fundamental discovery on ‘dancing molecules’ could apply to,” Stupp said. “Controlling supramolecular motion through chemical design appears to be a powerful tool to increase efficacy for a range of regenerative therapies.”



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New understanding of fly behavior has potential application in robotics, public safety

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Why do flies buzz around in circles when the air is still? And why does it matter?

In a paper published online July 26, 2024 by the scientific journal Current Biology, University of Nevada, Reno Assistant Professor Floris van Breugel and Postdoctoral Researcher S. David Stupski respond to this up-until-now unanswered question. And that answer could hold a key to public safety — specifically, how to better train robotic systems to track chemical leaks.

“We don’t currently have robotic systems to track odor or chemical plumes,” van Breugel said. “We don’t know how to efficiently find the source of a wind-borne chemical. But insects are remarkably good at tracking chemical plumes, and if we really understood how they do it, maybe we could train inexpensive drones to use a similar process to find the source of chemicals and chemical leaks.”

A fundamental challenge in understanding how insects track chemical plumes — basically, how does the fly find the banana in your kitchen? — is that wind and odors can’t be independently manipulated.

To address this challenge, van Breugel and Stupski used a new approach that makes it possible to remotely control neurons — specifically the “smell” neurons — on the antennae of flying fruit flies by genetically introducing light-sensitive proteins, an approach called optogenetics. These experiments, part of a $450,000 project funded through the Air Force Office of Scientific Research, made it possible to give flies identical virtual smell experiences in different wind conditions.

What van Breugel and Stupski wanted to know: how do flies find an odor when there’s no wind to carry it? This is, after all, likely the wind experience of a fly looking for a banana in your kitchen. The answer is in the Current Biology article, “Wind Gates Olfaction Driven Search States in Free Flight.” The print version will appear in the Sept. 9 issue.

Flies use environmental cues to detect and respond to air currents and wind direction to find their food sources, according to van Breugel. In the presence of wind, those cues trigger an automatic “cast and surge” behavior, in which the fly surges into the wind after encountering a chemical plume (indicating food) and then casts — moves side to side — when it loses the scent. Cast-and-surge behavior long has been understood by scientists but, according to van Breugel, it was fundamentally unknown how insects searched for a scent in still air.

Through their work, van Breugel and Stupski uncovered another automatic behavior, sink and circle, which involves lowering altitude and repetitive, rapid turns in a consistent direction. Flies perform this innate movement consistently and repetitively, even more so than cast-and-surge behavior.

According to van Breugel, the most exciting aspect of this discovery is that it shows flying flies are clearly able to assess the conditions of the wind — its presence, and direction — before deploying a strategy that works well under these conditions. The fact that they can do this is actually quite surprising — can you tell if there is a gentle breeze if you stick your head out of the window of a moving car? Flies aren’t just reacting to an odor with the same preprogrammed response every time like a simple robot, they are responding in context-appropriate manner. This knowledge potentially could be applied to train more sophisticated algorithms for scent-detecting drones to find the source of chemical leaks.

So, the next time you try to swat a fly in your home, consider the fact that flies might actually be a little more aware of some of their natural surroundings than you are. And maybe just open a window to let it out.



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New drug shows promise in clearing HIV from brain

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An experimental drug originally developed to treat cancer may help clear HIV from infected cells in the brain, according to a new Tulane University study.

For the first time, researchers at Tulane National Primate Research Center found that a cancer drug significantly reduced levels of SIV, the nonhuman primate equivalent of HIV, in the brain by targeting and depleting certain immune cells that harbor the virus.

Published in the journal Brain, this discovery marks a significant step toward eliminating HIV from hard-to-reach reservoirs where the virus evades otherwise effective treatment.

“This research is an important step in tackling brain-related issues caused by HIV, which still affect people even when they are on effective HIV medication,” said lead study author Woong-Ki Kim, PhD, associate director for research at Tulane National Primate Research Center. “By specifically targeting the infected cells in the brain, we may be able to clear the virus from these hidden areas, which has been a major challenge in HIV treatment.”

Antiretroviral therapy (ART) is an essential component of successful HIV treatment, maintaining the virus at undetectable levels in the blood and transforming HIV from a terminal illness into a manageable condition. However, ART does not completely eradicate HIV, necessitating lifelong treatment. The virus persists in “viral reservoirs” in the brain, liver, and lymph nodes, where it remains out of reach of ART.

The brain has been a particularly challenging area for treatment due to the blood-brain barrier — a protective membrane that shields it from harmful substances but also blocks treatments, allowing the virus to persist. In addition, cells in the brain known as macrophages are extremely long-lived, making them difficult to eradicate once they become infected.

Infection of macrophages is thought to contribute to neurocognitive dysfunction, experienced by nearly half of those living with HIV. Eradicating the virus from the brain is critical for comprehensive HIV treatment and could significantly improve the quality of life for those with HIV-related neurocognitive problems.

Researchers focused on macrophages, a type of white blood cell that harbors HIV in the brain. By using a small molecule inhibitor to block a receptor that increases in HIV-infected macrophages, the team successfully reduced the viral load in the brain. This approach essentially cleared the virus from brain tissue, providing a potential new treatment avenue for HIV.

The small molecule inhibitor used, BLZ945, has previously been studied for therapeutic use in amyotrophic lateral sclerosis (ALS) and brain cancer, but never before in the context of clearing HIV from the brain.

The study, which took place at the Tulane National Primate Research Center, utilized three groups to model human HIV infection and treatment: an untreated control group, and two groups treated with either a low or high dose of the small molecule inhibitor for 30 days. The high-dose treatment lead to a notable reduction in cells expressing HIV receptor sites, as well as a 95-99% decrease in viral DNA loads in the brain .

In addition to reducing viral loads, the treatment did not significantly impact microglia, the brain’s resident immune cells, which are essential for maintaining a healthy neuroimmune environment. It also did not show signs of liver toxicity at the doses tested.

The next step for the research team is to test this therapy in conjunction with ART to assess its efficacy in a combined treatment approach. This could pave the way for more comprehensive strategies to eradicate HIV from the body entirely.

This research was funded by the National Institutes of Health, including grants from the National Institute of Mental Health and the National Institute of Neurological Disorders and Stroke, and was supported with resources from the Tulane National Primate Research Center base grant of the National Institutes of Health, P51 OD011104.



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