On the trail of rare genetic disease, scientists uncover key immune regulator

November 27, 2018

LA JOLLA, CA - Scientists at Scripps Research have found an important immune system-regulating protein that in principle could be targeted to treat cancers and chronic viral infections.

The scientists, in a study published November 12 in Nature Chemical Biology, set out to determine the function of a protein, ABHD12, whose absence causes a rare genetic disease featuring a host of brain and nerve problems.

The researchers found that ABHD12 normally acts as a powerful "brake" on the immune system to keep it from becoming harmfully overactive. Mice engineered without the protein have signs of elevated inflammation, and their immune systems are more likely to overreact to a viral infection.

The discovery suggests that the absence of ABHD12 in people with mutant versions of its gene may cause neurological disease at least in part via excessive immune activity. It also indicates that ABHD12 may be a useful target for drugs that boost the immune system--for example against cancers and viruses that normally persist by shutting down people's immune defenses.

"This is a good example of how the study of a rare genetic disease can reveal a pathway that plays a key role in human biology," says study co-senior author Benjamin Cravatt, professor and chair of the Department of Chemical Physiology at Scripps Research.

The rare disease in this case is a mix of progressive brain, peripheral nerve, and eye problems that scientists have given the acronym PHARC (polyneuropathy, hearing loss, ataxia, retinitis pigmentosa and cataract). Since 2010, researchers have known that PHARC is caused by gene mutations that prevent ABHD12 from being made. But the normal function--or functions--of ABHD12, and the precise reasons its absence causes disease, have been unclear.

The Cravatt laboratory, in a 2013 study, engineered "knockout" mice that lack the ABHD12 gene, and determined that the ABHD12 protein is an enzyme that normally breaks down lysophospholipids--fat-related molecules that include lyso-PS, an important stimulator of immune activity. In the new study, Cravatt's team collaborated with researchers at Abide Therapeutics to extend their work on ABHD12 by developing a compound that selectively inhibits the enzyme's function.

"The idea was to use this inhibitor to disrupt ABHD12 in otherwise normal adult mice, and compare the effects to what we see in the ABHD12-knockout mice that never have a working copy of the enzyme," Cravatt says.

The team found that in adult mice, reducing ABHD12 activity with the inhibitor led to a rise in lyso-PS in immune cells called macrophages, as well as in brain tissue. The rise wasn't as great as that seen in the ABHD12-knockout mice, and even four weeks of treatment with the inhibitor appeared to cause only slight hearing defects--nothing like the profound defects experienced by PHARC patients. However, in further experiments conducted by the laboratory of study co-senior author John Teijaro, an assistant professor in the Department of Immunology and Microbiology at Scripps Research, it was clear that the reduction in ABHD12 activity had a big effect on the mouse immune system.

Teijaro's team infected the inhibitor-treated mice with a virus called lymphocytic choriomeningitis virus (LCMV) clone 13, which can deactivate elements of the immune system to establish a persistent infection in its hosts. Ordinary mice infected with LCMV clone 13 typically have minor symptoms but take a long time to clear the infection.

Teijaro and colleagues found that the ABHD12-knockout mice, as well as the mice treated with the ABHD12 inhibitor, had immune responses that were much more vigorous and effective in clearing the virus, often excessively so.

"The enhanced mortality and lung pathology were striking in clone-13 infected mice following ABHD12 inhibition or deletion," Teijaro says.

The findings suggest several possibilities to investigate with future research. For example, the enhanced immune activity in the knockout and inhibitor-treated mice hints that the signs and symptoms of PHARC may have an immunological basis.

"It is now known that the immune system plays a big role in many brain diseases, including neurodegenerative diseases such as Alzheimer's and Parkinson's," Cravatt notes. "There have also been hints of immune involvement in developmental brain disorders such as autism and schizophrenia."

He adds that if PHARC turns out to be caused in part by chronic brain and nerve inflammation, it might be treatable, if caught early enough, with anti-inflammatory or immune-suppressing drugs.

At the same time, treatments that target ABHD12, reducing its activity and stimulating the immune system, might have even broader use.

"The enhanced killer-T-cell activity we saw following ABHD12 deletion in the LCMV-infected mice suggests that blocking ABHD12 may enhance T-cell responses in immune suppressive environments such as chronic viral infections and cancers," Teijaro says.

"We're certainly eager to explore those possibilities," Cravatt says.
The co-first authors of the study, "Selective blockade of the lyso-PS lipase ABHD12 stimulates immune responses in vivo," were Daisuke Ogasawara?, Taka Aki-Ichu, and Vincent Vartabedian, of Scripps Research. Other co-authors, besides Cravatt and Teijaro, were Jacqueline Benthuysen, Hui Jing, Jonathan J. Hulce, Amanda Roberts, Steven Brown and Hugh Rosen, of Scripps Research, and Alex Reed and Olesya Ulanovskaya, of Abide Therapeutics.

Support for the research was provided by the National Institutes of Health (grants DA033760, NS092980, AI123210) and the Skaggs Institute for Chemical Biology at Scripps Research.

Scripps Research Institute

Related Immune System Articles from Brightsurf:

How the immune system remembers viruses
For a person to acquire immunity to a disease, T cells must develop into memory cells after contact with the pathogen.

How does the immune system develop in the first days of life?
Researchers highlight the anti-inflammatory response taking place after birth and designed to shield the newborn from infection.

Memory training for the immune system
The immune system will memorize the pathogen after an infection and can therefore react promptly after reinfection with the same pathogen.

Immune system may have another job -- combatting depression
An inflammatory autoimmune response within the central nervous system similar to one linked to neurodegenerative diseases such as multiple sclerosis (MS) has also been found in the spinal fluid of healthy people, according to a new Yale-led study comparing immune system cells in the spinal fluid of MS patients and healthy subjects.

COVID-19: Immune system derails
Contrary to what has been generally assumed so far, a severe course of COVID-19 does not solely result in a strong immune reaction - rather, the immune response is caught in a continuous loop of activation and inhibition.

Immune cell steroids help tumours suppress the immune system, offering new drug targets
Tumours found to evade the immune system by telling immune cells to produce immunosuppressive steroids.

Immune system -- Knocked off balance
Instead of protecting us, the immune system can sometimes go awry, as in the case of autoimmune diseases and allergies.

Too much salt weakens the immune system
A high-salt diet is not only bad for one's blood pressure, but also for the immune system.

Parkinson's and the immune system
Mutations in the Parkin gene are a common cause of hereditary forms of Parkinson's disease.

How an immune system regulator shifts the balance of immune cells
Researchers have provided new insight on the role of cyclic AMP (cAMP) in regulating the immune response.

Read More: Immune System News and Immune System Current Events
Brightsurf.com is a participant in the Amazon Services LLC Associates Program, an affiliate advertising program designed to provide a means for sites to earn advertising fees by advertising and linking to Amazon.com.