The non-human living inside of you | Cold Spring Harbor Laboratory (2024)

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The non-human living inside of you | Cold Spring Harbor Laboratory (1)

Half of your genome started out as an infection; if left unchecked, some parts of it can turn deadly all over again.

The human genome contains billions of pieces of information and around 22,000 genes, but not all of it is, strictly speaking, human. Eight percent of our DNA consists of remnants of ancient viruses, and another 40 percent is made up of repetitive strings of genetic letters that is also thought to have a viral origin. Those extensive viral regions are much more than evolutionary relics: They may be deeply involved with a wide range of diseases including multiple sclerosis, hemophilia, and amyotrophic lateral sclerosis (ALS), along with certain types of dementia and cancer.

For many years, biologists had little understanding of how that connection worked—so little that they came to refer to the viral part of our DNA as dark matter within the genome. “They just meant they didn’t know what it was or what it did,” explains Molly Gale Hammell, an associate professor at Cold Spring Harbor Laboratory. It became evident that the virus-related sections of the genetic code do not participate in the normal construction and regulation of the body. But in that case, how do they contribute to disease?

Eight percent of our DNA consists of remnants of ancient viruses, and another 40 percent is made up of repetitive strings of genetic letters that is also thought to have a viral origin.”

An early clue came from the pioneering geneticist Barbara McClintock, who spent much of her career at CSHL. In the 1940s, long before the decoding of the human genome, she realized that some stretches of our DNA behave like infectious invaders. These DNA chunks can move around through the genome, copying and pasting themselves wherever they see fit, which inspired McClintock to call them “jumping genes.” Her once-controversial idea earned her a Nobel Prize in 1983.

Geneticists have since determined that jumping genes originate in the viral portion of the genome. Many of these genes turn out to be benign or even helpful. “But some of the things are full-on parasites,” Hammell says, like infections embedded within our own DNA. All it takes to set these bad actors loose, she is finding, is a slip-up in the body’s mechanisms that normally prevent the genes from jumping around and causing harm.

Much of the research on the connection between jumping genes and disease has focused on natural molecules in the body that immobilize the genes by blocking their sequences from being read or copied. In recent years, Hammell and a number of scientists have focused specifically on a once-obscure protein known as TDP-43, which is highly adept at latching onto and hiding stretches of DNA.

Avi Nath, the clinical director of the National Institute for Neurological Disease and Stroke, helped draw attention to the importance of TDP-43 starting a decade ago. While studying a group of HIV-positive patients with ALS-like symptoms, Nath found that the anti-HIV drugs they were taking were also improving their ALS symptoms. He suspected that the drugs designed to fight the HIV virus were also suppressing the virus-like activity from jumping genes.

Subsequent work by Nath and others bolstered that idea, identifying a specific group of viral relics that seemed to be associated with dead neurons in the brains of ALS patients. A study led by biochemist Wenxue Li, now at Yale University, further showed that the ancient viruses in question interacts strongly with TDP-43.

At this point, the puzzle pieces began to fall into place. Medical researchers already knew that nearly all ALS patients experience a severe TDP-43 malfunction that causes large amounts of that protein to build up in their neurons, where it forms toxic clumps. Now it appears that TDP-43 could contribute to ALS in another way: The faulty form of the protein might no longer be able to hold back critical nerve-killing jumping genes.

Over the past two years, Hammell has confirmed that the normal form of TDP-43 suppresses harmful activity (pdf) from jumping genes in mice and humans. Other researchers have found that TDP-43 malfunction is also associated with certain types of Alzheimer’s and dementia.

The case is still not completely solved. Hammell and Nath cannot yet say for certain whether jumping genes cause ALS in some patients, or whether their activity is a byproduct of the way that ALS progresses. But either way, researchers have an important new goal in treating neurodegenerative disease: taming the non-human portion of our genome.

For more about the science underway at Cold Spring Harbor Laboratory and the rest of the world, please visit the new Biology+Beyond channel on Nautilus.

Written by: Carrie Arnold, Nautilus Writer

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ALS Alzheimer's Barbara McClintock DNA genome Molly Gale Hammell Quantitative Biology

DISCOVER: Related stories

Dark matter of the genome, part 1This episode of Base Pairs digs into "dark matter" a type of genetic information that could help scientists better understand diseases like Read more » March 15, 2017 Riding out of the shadows of ALS, toward better treatmentsGraduate student Lisa Krug discusses her research and personal connection to ALS, and Ride for Life, a not-for-profit organization for ALS research. Read more » August 1, 2016 Seeking better treatment for ALS, Lou Gehrig’s diseaseResearchers found that ‘jumping genes’ were de-silenced in post-mortem tissue samples of ALS patients. Read more » October 29, 2019
The non-human living inside of you | Cold Spring Harbor Laboratory (2024)

FAQs

What is the non human living inside of you? ›

The human genome contains billions of pieces of information and around 22,000 genes, but not all of it is, strictly speaking, human. Eight percent of our DNA consists of remnants of ancient viruses, and another 40 percent is made up of repetitive strings of genetic letters that is also thought to have a viral origin.

What is the ancient virus in DNA? ›

HERVs, or human endogenous retroviruses, make up around 8% of the human genome, left behind as a result of infections that humanity's primate ancestors suffered millions of years ago. They became part of the human genome due to how they replicate.

Are transposons good or bad? ›

Many transposons are harmful, but sometimes they give an organism new characteristics that are vital to survival.

What was the conclusion of the human genome project? ›

It was concluded that the human genome is as complex and as special as any other organisms. These findings demystified the special expectations created around the human DNA.

What are non-human beings? ›

1. a creature, animal, or being that is not human. adjective. 2. not related to human beings.

What does non-human entity mean? ›

Non-human entities are defined as fictitious characters, mythological figures, deities, legendary characters, and animals with proper names. RDA allows these entities to be established as personal names, since they can be presented as creators of resources.

What are the 3 DNA viruses? ›

DNA viruses comprise important pathogens such as herpesviruses, poxviruses, adenoviruses, and papillomaviruses, among others.

What was the first virus on Earth? ›

Two scientists contributed to the discovery of the first virus, Tobacco mosaic virus. Ivanoski reported in 1892 that extracts from infected leaves were still infectious after filtration through a Chamberland filter-candle. Bacteria are retained by such filters, a new world was discovered: filterable pathogens.

What is the largest DNA virus? ›

With a diameter of approximately 650 nm, Mimivirus is the largest virus known to date. Morphologically, Mimivirus resembles nucleocytoplasmic large DNA viruses (NCLDVs) such as the Iridovirus, Asfarvirus, and Phycodnavirus. However, evolutionary dissimilarities define a new family, the Mimiviridae.

What is DNA jumping? ›

Transposable elements (TEs), also known as "jumping genes" or transposons, are sequences of DNA that move (or jump) from one location in the genome to another.

Why do jumping genes exist? ›

They jump around the genome in developing sperm and egg cells and are important to evolution. But their mobilization can also cause new mutations that lead to diseases, such as hemophilia and cancer.

What diseases can transposons cause? ›

Apart from cancer, transposons also play a role in neurodegenerative diseases. In Drosophila models of Alzheimer's disease and progressive supranuclear palsy, transcripts of transposons are found. This suggests that transposon dysregulation is associated with the onset of neurodegenerative diseases.

What genetic diseases have already been identified by HGP? ›

Gene therapy began with the Human Genome Project. The Human Genome Project has found gene locations for many diseases. Among the diseases that have been found Huntington's disease, cystic fibrosis, ADA deficiency, and two genes for breast cancer are just a few examples.

What kind of disease can be cured with the help of gene therapy? ›

In the future, genetic therapies may be used to prevent, treat, or cure certain inherited disorders, such as cystic fibrosis, alpha-1 antitrypsin deficiency, hemophilia, beta thalassemia, and sickle cell disease. They also may be used to treat cancers or infections, including HIV.

How similar are all human genomes? ›

Most of our DNA determines that we are human, rather than determining how we are different from any other person. So it is not so surprising that the DNA of any two human beings is 99.9 percent identical.

What is living inside your body? ›

Microbes inhabit just about every part of the human body, living on the skin, in the gut, and up the nose.

What are examples of non-human persons? ›

Often, she says, these other-than-human persons can include animals, ancestors and other dead, elements of the natural world, and things that people make.

Are there non-human persons and human non-persons? ›

First, whereas human is a biological category, in law and ethics, the category of person entails certain duties or rights, such as the right not to be harmed or killed without a very good reason. On this understanding, humans and persons are not necessarily synonymous, and there can be non-human persons.

What is the humans closet living relative? ›

Two African apes are the closest living relatives of humans: the chimpanzee (Pan troglodytes) and the bonobo (Pan paniscus).

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