Sound off: with RNA interference, gene silencing roars into labs.Although you don't hear a thing, there is a raucous party going on inside each one of your cells. Each minute of every day, molecules are murmuring information from one to the next in an ancient version of the game of telephone. DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. , the genetic party host, starts each round by whispering a message to its chemical cousin RNA RNA: see nucleic acid. RNA in full ribonucleic acid One of the two main types of nucleic acid (the other being DNA), which functions in cellular protein synthesis in all living cells and replaces DNA as the carrier of genetic . Keeping the game going, RNA passes this communication to the ribosomes Ribosomes Small particles, present in large numbers in every living cell, whose function is to convert stored genetic information into protein molecules. , the cell's amino acid-linking machines. They, in turn, spit out Verb 1. spit out - spit up in an explosive manner splutter, sputter cough out, cough up, expectorate, spit up, spit out - discharge (phlegm or sputum) from the lungs and out of the mouth 2. a protein translation of the original message. The proteins that result from this string of chatter fulfill all the cell's vital functions--and keep it going for countless more rounds of telephone throughout its life. But what would happen if someone put a molecular muzzle on one of these players, disrupting a round of the game? It would muffle the influence of a particular gene. Such a tool would be a tremendous boon to scientists looking to discover that gene's function. Researchers could infer, by omission, the gene's role in a cell. Shushing unwanted messages could also provide medical researchers with a means to rid cells of proteins that cause diseases. Scientists have spent decades searching for such a tool. One method, antisense RNA antisense RNA an RNA sequence which is complementary to a functional RNA. technology, proved to be unreliable. Another, engineering animals to lack a specific gene, can take at least a year. What's more, genes essential for life can't be studied with this knockout approach. Eight years ago, scientists stumbled on a phenomenon called RNA interference RNA interference n. A process in which the introduction of double-stranded RNA into a cell inhibits the expression of genes. (RNAi). They've now developed it into a technique that many researchers suspect might be more useful than the other tools available for inactivating genes. RNAi precisely targets a specific bit of RNA, effectively stifling its message before it makes a protein. The tool, also known as gene silencing, doesn't actually turn the volume all the way down. Genes are muted at 90 to 95 percent efficiency, a state that scientists refer to as a knockdown. For the past several years, the technique has been picking up steam. Scientists in thousands of labs are using RNAi to determine the roles of particular genes in a variety of organisms. Other teams are using RNAi to develop potential treatments for diseases including macular degeneration macular degeneration, eye disorder causing loss of central vision. The affected area, the macula, lies at the back of the retina and is the part that produces the sharpest vision. , AIDS, and Huntington's disease Huntington's disease, hereditary, acute disturbance of the central nervous system usually beginning in middle age and characterized by involuntary muscular movements and progressive intellectual deterioration; formerly called Huntington's chorea. . "There's almost no field not affected by the discovery of RNAi," says Phillip Zamore of the University of Massachusetts Medical School UMMS is ranked fourth in primary care education among the nation’s 125 medical schools in the 2006 U.S.News & World Report annual guide, “America’s Best Graduate Schools”. UMMS is also a major center for research. in Worcester, who studies the mechanisms by which RNAi works. MOLECULAR MUTE RNAi got its humble start in the mid-1990s after researchers had witnessed some strange genetic behavior. Adding bits of DNA to some organisms, including fungi, plants, and worms, seemed to snuff out to extinguish by snuffing. See also: Snuff the activity of selected genes. A second set of odd observations came from researchers trying to block certain genes with the antisense antisense, DNA or RNA manipulated in a laboratory so that its components (nucleotides) form a complementary copy of normal, or "sense," messenger RNA (mRNA; see nucleic acid). method. In this technique, a complementary strand of RNA, the antisense strand antisense strand one of the two strands in a DNA molecule that is not transcribed. , binds to part of a cell's normal, single-stranded RNA. When ribosomes encounter the resulting doublestranded bumps on a strip of singlestranded RNA, they don't translate those regions into proteins. This technique was applied to the roundworm roundworm, another name for a nematode. See phylum Nematoda. Caenorhabditis elegans by several researchers, including Andrew Fire, then of the Carnegie Institution in Baltimore, Md., and now of the Stanford School of Medicine, and Craig Mello of the University of Massachusetts Medical School. The scientists soon had a mystery on their hands. Working together, Fire and Mello performed tests with copies of a cell's single-stranded RNA, which shouldn't bind to the cell's RNA because this so-called sense RNA isn't complementary to it. But sense RNA seemed to work just as well as antisense RNA does at muzzling genes. "We couldn't see a reason why sense and antisense would both work," Fire says. After puzzling over the phenomenon for months, Fire and Mello hit on an explanation. Both the sense and antisense samples that they had been injecting into C. elegans were contaminated contaminated, v 1. made radioactive by the addition of small quantities of radioactive material. 2. made contaminated by adding infective or radiographic materials. 3. an infective surface or object. by tiny amounts of double-stranded RNA (dsRNA). The researchers next tailored bits of dsRNA to match particular gene sequences. When the scientists deliberately injected the worms with that RNA, they effectively shut down those genes. The RNAi technique was born. Over the next 7 years, Fire, Mello, and other scientists began deciphering RNAi'S basic mechanism. Interference starts when a piece of double-stranded RNA, either present naturally in a cell or injected by researchers, bumps into an enzyme called dicer dic·er n. A device used for dicing food. Noun 1. dicer - a mechanical device used for dicing food mechanical device - mechanism consisting of a device that works on mechanical principles , which circulates inside a cell's fluid contents. As its name suggests, dicer acts like a samurai-wielding ninja. It chops the dsRNA into bite-size pieces of about 22 base pairs, the individual chemical blocks that make up RNA. Each of these smaller pieces, called short interfering RNAs (siRNAs), then unzips into two RNA strands. One of these strands joins with a clump of several different proteins, the combination being dubbed an RNA-induced silencing complex RNA-induced silencing complex, or RISC, is a multi-protein siRNA complex which cleaves (incoming viral) dsRNA and binds short antisense RNA strands which are then able to bind complementary strands. (RISC RISC in full Reduced Instruction Set Computing Computer architecture that uses a limited number of instructions. RISC became popular in microprocessors in the 1980s. ). This complex then hunts down strands of RNA inside a cell that bind to, or complement, its siRNA strand. Once a complementary piece of RNA binds to RISC, several enzymes, including one named slicer, hack through and degrade it. Since the viruses known as retroviruses often produce dsRNA while they're replicating, some researchers have proposed that dicer, slicer, and other components associated with RNAi acted in early animals as a defense mechanism. This primitive type of protection, the theory goes, is no longer necessary in mammals and other organisms with complex immune systems. However, modern cells seem to use RNAi to control a wide variety of genes. Studies over the past few years have turned up dozens of RNAi-like mechanisms that affect, for example, embryonic development, stem cell stem cell In living organisms, an undifferentiated cell that can produce other cells that eventually make up specialized tissues and organs. There are two major types of stem cells, embryonic and adult. activity, or virus assembly inside cells. "We've discovered a way that nature turns genes off," says Zamore. CAN OF WORMS Scientists are still figuring out the details of how RNAi works. Zamore notes that a cadre of yet-unknown proteins, for example, seems to participate in each step of the process. But what's important, he says, is that RNAi does work. During the past few years, thousands of researchers have used RNAi to determine the functions of genes that were previously inaccessible to laboratory study. For example, one group is elucidating which genes are important for regeneration in planarian planarian, common name for several genera of the free-living (turbellarian) flatworms belonging to the order Tricladida, a name that derives from their characteristic three-branched digestive cavities. Most species range from 1-8 in. to about 1 in. in length (. worms. These flatworms can fully regrow Re`grow´ v. i. & t. 1. To grow again. The snail had power to regrow them all [horns, tongue, etc.] - A. B. Buckley. Verb 1. any amputated part of their bodies in just a few days, and an entire worm can regenerate from a tiny fragment of its body. A team led by Alejandro Sanchez Alvarado of the University of Utah The University of Utah (also The U or the U of U or the UU), located in Salt Lake City, is the flagship public research university in the state of Utah, and one of 10 institutions that make up the Utah System of Higher Education. Health Sciences Center in Salt Lake City recently used RNAi to examine this process. By discovering how these worms regenerate, researchers may eventually find tools to improve wound healing wound healing Physiology The repair of a wound Steps Inflammation, repair and closure, remodeling, final healing; repair of incisions may be either simple–'clean' wounds with little loss of tissue heal by 'primary intention', or 'dirty' wounds heal by in people. "Planarians have been around [in biological research] for about 200 years, and we've sliced and diced them in every conceivable fashion," says Sanchez Alvarado. However, the worms, which are frequently sterile, aren't suitable for traditional genetics studies, in which scientists breed organisms. Sanchez Alvarado happened to be working at the Carnegie Institute when Fire and Mello made their pivotal RNAi discovery. "[Fire] surmised that I should be able to use these methods to make this genetically intractable organism tractable tractable easy to manage; tolerable. ," Sanchez Alvarado notes. "It's worked extremely well." The May Developmental Cell describes his team's most recent efforts using RNAi to find regeneration genes in planarians. Most of the worms' genome had already been sequenced. The researchers produced bacteria containing bits of dsRNA engineered to match an individual planarian gene and then fed that interfering RNA to a batch of worms. The RNA made its way into the worms' cells. The researchers repeated the process using each of 1,065 different bits of RNA and observed each bit's effect in silencing individual worm genes. About 145 of the silenced genes affected regeneration. Sanchez Alvarado and his colleagues now plan to determine how each of these genes operates. Sanchez Alvarado notes that 38 of the other genes tested are related to human genes associated with diseases, including cancer. Only 8 of those 38 genes are currently under study in knockout mice. So, researchers using planarians may learn about gene functions that can't currently be studied in knockout animals. Muting genes with RNAi holds advantages over creating knockout animals. While attempts to engineer animals free of certain genes sometimes simply kill them, animals that have a gene that's knocked down usually survive long enough to provide information about the gene's function, says Bryan Cullen of Duke University in Durham, N.C. Greg Hannon of Cold Spring Harbor (N.Y.) Laboratory says, "RNAi will never replace knockouts, but what it does is it hugely expands the questions you can ask and the speed with which you can ask them." Hannon explains that creating a knockout mouse knock·out mouse n. A transgenic mouse that has been genetically engineered to exhibit mutations in specific genes. can take well over a year, while knocking down a gene with RNAi takes only a few days. Furthermore, Hannon notes that scientists don't plan on tinkering with people's genomes by knocking out genes. Instead, RNAi can silence a human gene in cells growing in lab dishes, enabling scientists to get a sense of the gene's role in the body. To that end, Hannon and his colleagues have set up a library of RNAi sequences at Cold Spring Harbor (N.Y.) Laboratory that researchers can use to study gene function in mice and people. The library already has enough siRNA sequences to silence about two-thirds of the human genome and around half of the mouse genome. DICING DISEASE Applying the new, reliable way to reduce activity of genes in human cells, researchers are now developing RNAi-based drugs to quiet genes that cause diseases. The main prerequisite to developing an RNAi-based solution is to learn which gene is problematic, says Fire. Another limiting factor, notes Howard Robin of San Francisco-based Sirna Therapeutics, is getting the bits of interfering RNA inside cells and making sure the bits don't degrade before they do their jobs. "That is the huge challenge of developing these drugs," he says. Many researchers predict that macular degeneration will be the first disease successfully treated with RNAi. This currently incurable disease is a leading cause of blindness in older Americans. It obscures a person's straight-ahead vision when extra blood vessels Blood vessels Tubular channels for blood transport, of which there are three principal types: arteries, capillaries, and veins. Only the larger arteries and veins in the body bear distinct names. grow, and then leak, in a central portion of the retina. According to Robin, the retina is an ideal place for administering RNAi. The retina is self-contained, so a drug injected there would remain where it needs to work. Moreover, retina cells easily take up bits of siRNA on their own. Several companies, including Sirna Therapeutics and Cambridge, Mass.-based Alnylam Pharmaceuticals, are currently developing RNAi-based drugs for macular degeneration. Sirna recently wrapped up its first phase of experiments of its top drug candidate. Each of 10 people with the disease received an RNAi-containing solution injected into the eye. This treatment halted progression of the disease with no notable side effects Side effects Effects of a proposed project on other parts of the firm. . Five of these patients also improved their ability to read letters, a significant advance in treating macular degeneration. Clinical trials will also be under way next year for an RNAi-based drug to treat HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. , the virus that causes AIDS. John Rossi of City of Hope, a medical-research center in Duarte, Calif., is now testing the drug in mice. The treatment prompts immune cells to produce siRNA that shuts down critical viral genes. Without the activity of these genes, the virus can't replicate and spread through the body. In experiments with human blood cells blood cells, n.pl the formed elements of the blood, including red cells (erythrocytes), white cells (leukocytes), and platelets (thrombocytes). blood cells See erythrocyte and leukocyte. Platelets are classed separately. growing in the laboratory, the intervention "works like a charm," says Rossi. "It basically blasts away at the virus." Researchers are making steady advances in work on several other diseases, including neurological disorders, although RNAi-based therapies there probably have a long way to go before they reach the clinic. For example, Beverly Davidson of the University of Iowa Not to be confused with Iowa State University. The first faculty offered instruction at the University in March 1855 to students in the Old Mechanics Building, situated where Seashore Hall is now. In September 1855, the student body numbered 124, of which, 41 were women. in Iowa City has developed a strategy to use RNAi to treat Huntingtoffs disease, which chips away at a person's ability to walk, talk, and reason. The fatal disease results from production of a mutated protein that's toxic to some types of brain cells. Davidson and her colleagues created genes that produce a type of RNAi that blocks production of the toxic protein. The researchers shuttled those genes into the brain cells of mice that develop a version of Huntington's. The mice have since shown a dramatic improvement in symptoms. Davidson notes that these results are somewhat surprising because this intervention knocks down the mutant proteins by only about 60 percent, making the payoff remarkable. "We got a lot for a little," she says. Even with these promising successes, many researchers don't expect RNAi to provide a quick fix for many health problems. Fire predicts years of ups and downs ups and downs pl.n. Alternating periods of good and bad fortune or spirits. ups and downs Noun, pl alternating periods of good and bad luck or high and low spirits as scientists learn the potential of RNAi. "I think there will be failures and successes in trying to get these therapeutics to work," says Fire. Nevertheless, says Robin, "I think we're making excellent progress." With so many researchers turning to RNAi, this field is now moving swiftly--and not so silently--ahead. |
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