Engineered bacteria build microstructures on their own - C&EN Global

Inside the genomes of mollusks sit instructions on how to build their shells. Synthetic biologists want to learn how to write such genetic instruction...
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Science Concentrates MEDICINAL CHEMISTRY SYNTHETIC BIOLOGY

Microbes programmed to build Inside the genomes of mollusks sit instructions on how to build their shells. Synthetic biologists want to learn how to write such genetic instructions so they can program cells to construct novel inorganic structures for devices such as biosensors and self-healing electronics. Now, a team of researchers has engineered Escherichia coli to self-assemble gold-coated domes that can be used as simple pressure sensors (Nat. Biotechnol. 2017, DOI: 10.1038/ nbt.3978). Previous attempts to achieve engineered self-assembly have relied on researchers laying down molecular cues to coax microbes to construct patterns in desired shapes, says Megan N. McClean of the University of Wisconsin, Madison, who was not involved in the work. This group’s work, she says, demonstrates that “all of the information, in terms of how you want the community to develop into a spatial pattern, can be contained within individual cells themselves.” Lingchong You of Duke University and colleagues packed that information into a circuit of genes that controls production of a modified protein called curli, which self-assembles into fibers and binds gold nanoparticles. The researchers found that with the genetic circuit, the bacteria produced curli only at the exterior of their colonies, leading the microbes to construct a curli-based dome over themselves. Adding gold nanoparticles to the colonies produces domes that can be pressed together, top to top, to form a pressure sensor. Pushing on the domes increases their electrical connections, allowing the team to measure applied pressure via current flow between the domes.—MICHAEL TORRICE

Bryostatin advances Shorter synthesis promises to boost dwindling supply of bryostatin 1, and an analog fights hidden HIV The marine natural product bryostatin 1 has shown promise as a treatment for cancer, Alzheimer’s disease, and HIV. But neither the compound nor its analogs have become approved drugs. One of the problems that has dogged bryostatin 1 is its scarce supply. Now, chemists at Stanford University led by Paul A. Wender have developed a shortened synthesis of bryostatin 1 capable of supplying sufficient amounts of the compound for clinical trials. In the late 1980s, chemists at the National Cancer Institute took 12,700 kg of the tiny sea creature Bugula neritina—roughly the same weight as a school bus—and isolated from it just 18 g of bryostatin 1—not

gence, telescoped steps, a crystalline final compound—that augur well for developing an eventual manufacturing route.” Wender says there was no particular synthetic breakthrough that helped his group whittle down the synthesis of bryostatin 1, just clever chemistry and hard work. “It’s kind of like running a marathon,” he says. “What’s important is how you start, what the middle of the race looks like, and how you cross the finish line.” He is currently in discussions with potential partners to modestly scale up the synthesis using current Good Manufacturing Practices so the material can be used in the clinic. Bryostatin 1 has been given the go-ahead

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Bryostatin 1 enough to even fill a salt shaker. The lion’s share of that material has been used to supply more than three dozen clinical trials as a cancer chemotherapy, which ultimately didn’t pan out. Wender’s new 29-step synthesis of bryostatin 1, which nearly halves the number of steps in the only other synthesis of the compound, from Gary Keck’s lab at the University of Utah, could replenish supplies for clinical trials in other treatment areas where bryostatin 1 has proven promising (Science 2017, DOI: 10.1126/science. aan7969). “The recent work from the Wender group marks a significant advance in resolving supply issues that will enable full clinical evaluation of bryostatins as chemotherapeutic agents. Specifically, gram quantities of bryostatin 1 are now available by total synthesis,” notes Frank Fang, deputy president of Eisai’s Andover innovative Medicines Institute. “The route described has several attractive features—conver-

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SUW133 for testing in human clinical trials, but Wender still thinks many of the bryostatin analogs may ultimately be more useful than the natural product as drugs. In recent work with the University of California, Los Angeles’s Jerome A. Zack and colleagues, he has shown that the analog SUW133 can coax latent HIV out of cells and kill the virus more effectively than bryostatin 1 in an animal model (PLOS Path. 2017, DOI: 10.1371/journal.ppat.1006575). “Among the many findings of their work, two are especially relevant for the purpose of curing HIV: the absence of persistent immune activation after the reversal of HIV-1 latency by the drug, and the killing of a significant percentage of cells after the reactivation of latent HIV-1,” comments Santiago Moreno, an infectious disease expert at Madrid’s Ramón y Cajal Hospital. “If these results are confirmed in humans, apparently a single drug could do all the work needed.”—BETHANY

HALFORD OCTOBER 16, 2017 | CEN.ACS.ORG | C&EN

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