MINORITY REPORT

Blood testing identifies biomarkers of suicidal thoughts

UC San Diego study suggests new way to personalize mental health care

Peer-Reviewed Publication

UNIVERSITY OF CALIFORNIA - SAN DIEGO

 

IMAGE: 

IN MOST CELLS, MITOCHONDRIA (GREEN) FORM COMPLEX TUBULAR NETWORKS THAT HELP THEM DISTRIBUTE ENERGY THROUGHOUT THE CELL. DISRUPTION OF THESE MITOCHONDRIAL NETWORKS IS A HALLMARK OF MANY HUMAN DISEASES.

view more 

CREDIT: UC SAN DIEGO HEALTH SCIENCES

Major depressive disorder affects 16.1 million adults in the United States and costs $210 billion annually. While the primary symptoms of depression are psychological, scientists and doctors have come to understand that depression is a complex disease with physical effects throughout the body. For example, measuring markers of cellular metabolism has become an important approach to studying mental illnesses and developing new ways to diagnose, treat and prevent them.

Researchers at University of California San Diego School of Medicine have now advanced this line of work in a new study, revealing a connection between cellular metabolism and depression. They found that people with depression and suicidal ideation had detectable compounds in their blood that could help identify individuals at higher risk of becoming suicidal. The researchers also found sex-based differences in how depression impacts cell metabolism.

The findings, published December 15, 2023 in Translational Psychiatry, could help personalize mental health care and potentially identify new targets for future drugs.

“Mental illnesses like depression have impacts and drivers well beyond the brain,” said Robert Naviaux, MD, PhD, a professor in the Department of Medicine, Pediatrics and Pathology at UC San Diego School of Medicine. “Prior to about ten years ago it was difficult to study how the chemistry of the whole body influences our behavior and state of mind, but modern technologies like metabolomics are helping us listen in on cells’ conversations in their native tongue, which is biochemistry.”

While many people with depression experience improvement with psychotherapy and medication, some people’s depression is treatment-refractory, meaning treatment has little to no impact. Suicidal thoughts are experienced by the majority of patients with treatment-refractory depression, and as many as 30% will attempt suicide at least once in their lifetime.

“We’re seeing a significant rise in midlife mortality in the United States, and increased suicide incidence is one of many things driving that trend,” said Naviaux. “Tools that could help us stratify people based on their risk of becoming suicidal could help us save lives."

The researchers analyzed the blood of 99 study participants with treatment-refractory depression and suicidal ideation, as well as an equal number of healthy controls. Among the hundreds of different biochemicals circulating in the blood of these individuals, they found that five could be used as a biomarker to classify patients with treatment-refractory depression and suicidal ideation. However, which five could be used differed between men and women.

“If we have 100 people who either don’t have depression or who have depression and suicidal ideation, we would be able to correctly identify 85-90 of those at greatest risk based on five metabolites in males and another 5 metabolites in females,” said Naviaux. “This could be important in terms of diagnostics, but it also opens up a broader conversation in the field about what’s actually leading to these metabolic changes.”

While there were clear differences in blood metabolism between males and females, some metabolic markers of suicidal ideation were consistent across both sexes. This included biomarkers for mitochondrial dysfunction, which occurs when the energy-producing structures of our cells malfunction.

“Mitochondria are some of the most important structures of our cells and changed mitochondrial functions occur in a host of human diseases,” added Naviaux.

Mitochondria produce ATP, the primary energy currency of all cells. ATP is also an important molecule for cell-to-cell communication, and the researchers hypothesize it is this function that is most dysregulated in people with suicidal ideation.

“When ATP is inside the cell it acts like an energy source, but outside the cell it is a danger signal that activates dozens of protective pathways in response to some environmental stressor,” said Naviaux. “We hypothesize that suicide attempts may actually be part of a larger physiological impulse to stop a stress response that has become unbearable at the cellular level.”

Because some of the metabolic deficiencies identified in the study were in compounds that are available as supplements, such as folate and carnitine, the researchers are interested in exploring the possibility of individualizing depression treatment with these compounds to help fill in the gaps in metabolism that are needed for recovery. Naviaux hastens to add that these supplements are not cures.

“None of these metabolites are a magic bullet that will completely reverse somebody’s depression,” said Naviaux. “However, our results tell us that there may be things we can do to nudge the metabolism in the right direction to help patients respond better to treatment, and in the context of suicide, this could be just enough to prevent people from crossing that threshold.”

In addition to suggesting a new approach to personalize medicine for depression, the research could help scientists discover new drugs that can target mitochondrial dysfunction, which could have wide implications for human health in general.

“Many chronic diseases are comorbid with depression, because it can be extremely stressful to deal with an illness for years at a time,” said Naviaux. “If we can find ways to treat depression and suicidal ideation on a metabolic level, we may also help improve outcomes for the many diseases that lead to depression. Many chronic illnesses, such as post-traumatic stress disorder and chronic fatigue syndrome, are not lethal themselves unless they lead to suicidal thoughts and actions. If metabolomics can be used to identify the people at greatest risk, it could ultimately help us save more lives.”

Co-authors include: Jane C. Naviaux, Lin Wang, Kefeng Li, Jonathan M. Monk and Sai Sachin Lingampelly at UC San Diego, Lisa A. Pan, Anna Maria Segreti, Kaitlyn Bloom, Jerry Vockley, David N. Finegold and David G. Peters at University of Pittsburgh School of Medicine, and Mark A. Tarnopolsky at McMaster University.

This graphic describes the metabolomics workflow the researchers used to analyze the blood of people with depression and suicidal ideation. Their approach generates a unique metabolic signature that could be used to help personalize treatment for depression.

CREDIT

UC San Diego Health Sciences

---

JOURNAL

Translational Psychiatry

DOI

10.1038/s41398-023-02696-9 

En.wikipedia.org

https://en.wikipedia.org/wiki/Minority_Report_(film)

Minority Report (film) - Wikipedia

Minority Report is a futuristic film which portrays elements of a both dystopian and utopian future. ... The film renders a much more detailed view of its future ...

En.wikipedia.org

https://en.wikipedia.org/wiki/The_Minority_Report

The Minority Report - Wikipedia

In the story, Precrime Police Commissioner John A. Anderton believes that the prediction that he will commit a murder has been generated as a majority report.

 

Menu labeling and calories purchased in restaurants in a national fast food chain

JAMA Network Open

Peer-Reviewed Publication

JAMA NETWORK

About The Study: Fewer calories were purchased in restaurants with calorie labels compared with those with no labels, suggesting that consumers are sensitive to calorie information on menu boards, according to the results of this study of 2,329 Mexican-inspired fast food restaurants in six U.S. locations. Associations differed by location. 

Authors: Brian Elbel, Ph.D., M.P.H., of the New York University School of Medicine in New York, is the corresponding author. 

To access the embargoed study: Visit our For The Media website at this link https://media.jamanetwork.com/ 

(doi:10.1001/jamanetworkopen.2023.46851)

Editor’s Note: Please see the article for additional information, including other authors, author contributions and affiliations, conflict of interest and financial disclosures, and funding and support.

#  #  #

Embed this link to provide your readers free access to the full-text article 

 http://jamanetwork.com/journals/jamanetworkopen/fullarticle/10.1001/jamanetworkopen.2023.46851?utm_source=For_The_Media&utm_medium=referral&utm_campaign=ftm_links&utm_term=121523

About JAMA Network Open: JAMA Network Open is an online-only open access general medical journal from the JAMA Network. On weekdays, the journal publishes peer-reviewed clinical research and commentary in more than 40 medical and health subject areas. Every article is free online from the day of publication. 

---

JOURNAL

JAMA Network Open

 

Immune cells shape lung before birth and provide new avenues for treating respiratory diseases

Healthy lung development hinges on immune-epithelial crosstalk, revealing a new role for immune cells outside of immunity, with implications for treating respiratory diseases

Peer-Reviewed Publication

WELLCOME TRUST SANGER INSTITUTE

Immune cells play an active and intimate role in directing the growth of human lung tissue during development, researchers find, revolutionising our understanding of early lung development and the role of immune cells outside of immunity.

The research offers new insights for understanding and treating respiratory conditions, such as chronic obstructive pulmonary disease (COPD). Respiratory conditions account for almost 20 per cent of all deaths in children under five years worldwide1.

The work reveals a surprising coordination between the immune and respiratory systems, much earlier in development than previously thought. This discovery raises questions about the potential role of immune cells in other developing organs across the body.

Researchers from the Wellcome Sanger Institute, University College London (UCL) and their collaborators at EMBL’s European Bioinformatics Institute used advanced single-cell technologies to map the development of early human lung immune cells over time.

This study has created a first-of-its-kind immune cell atlas of the developing lung2. It is part of the international Human Cell Atlas3 initiative, which is mapping every cell type in the human body, to transform our understanding of health, infection and disease.

The findings, published today (15 December) in Science Immunology, will help shed light on the mechanisms behind childhood lung diseases.

Immune cells make up a substantial portion of the airways and mature lungs, which have critical gas exchange and barrier functions, providing protection against infection of the respiratory tract. However, the roles of immune cells in the developing organ have remained unexplored compared to structural or lining cell types. Recent discoveries confirm the presence of immune cells in human lungs as early as five weeks into development4.

To explore whether the immune system might influence how lungs grow, the team studied immune cells in early human lungs from 5 to 22 weeks of development. They used various techniques, including single-cell sequencing and experiments with lung cell cultures, to see if immune cells could affect lung cell development.

They identified key regulators of lung development, including signalling molecule IL-1β and IL-13 that facilitate the coordination of lung stem cells differentiating into specialised mature cell types5.

The researchers detected an infiltration of innate, followed by adaptive immune cells. Innate cells included innate lymphoid cells (ILCs), natural killer (NK) cells, myeloid cells and progenitor cells. With respect to adaptive immune cells, as well as T cells, both developing and mature B lineage cells were detected, indicating that the lung environment supports B cell development.

The findings fundamentally change the understanding of the immune and epithelial interactions that are crucial for foetal lung maturation. They also suggest that early immune disturbances could manifest as paediatric lung disease.

These new insights into mechanisms in early lung formation will also contribute to the development of new therapeutic approaches for regenerating damaged lung tissue and restoring lung function.

Dr Peng He and Dr Jo Barnes, co-first authors of the study at the Wellcome Sanger Institute and EMBL’s European Bioinformatics Institute, and UCL Division of Medicine respectively, said: “By adopting a focused strategy in mapping the immune system, we reveal a symbiotic relationship between immune cells and developing lungs. These detailed insights open the door to potential regenerative therapies in not only the lung, but in other vital human organs.”

Dr Marko Nikolić, senior author of the study at UCL Division of Medicine and honorary consultant in respiratory medicine, said: "We now know immune-epithelial crosstalk is a feature of early lung development. This vital baseline of healthy lung development will help us understand what happens when lung developmental processes get disrupted, for example in preterm births, which can lead to respiratory deficiencies.”

Dr Kerstin Meyer, senior author of the study at the Wellcome Sanger Institute, said: “The active participation of immune cells expands the possibilities for understanding and addressing impaired lung formation. What is super exciting about this mechanism is that it may well apply in other organ systems too.”

Dr Sarah Teichmann, senior author of the study at the Wellcome Sanger Institute and Co-founder of the Human Cell Atlas, said: “If we are to fully understand the root causes of disease, we require a complete view of cells at all stages in the human body. This important contribution towards a comprehensive Human Cell Atlas will be a valuable reference for studying lung diseases.”

ENDS

Contact details:
Jelena Pupavac
Press Office
Wellcome Sanger Institute
Cambridge, CB10 1SA
Email: press.office@sanger.ac.uk

Notes to Editors:

1. https://www.who.int/data/gho/indicator-metadata-registry/imr-details/3147
2. The researchers analysed human embryonic and foetal lung tissue between 5 and 22 weeks post-conception. Human embryonic tissue was provided by the Joint MRC/Wellcome Trust Human Developmental Biology Resource (www.hdbr.org)
3. The Human Cell Atlas (HCA) is an international collaborative consortium which is creating comprehensive reference maps of all human cells—the fundamental units of life—as a basis for understanding human health and for diagnosing, monitoring, and treating disease. The HCA is likely to impact every aspect of biology and medicine, propelling translational discoveries and applications and ultimately leading to a new era of precision medicine.
   The HCA was co-founded in 2016 by Dr Sarah Teichmann at the Wellcome Sanger Institute (UK) and Dr Aviv Regev, then at the Broad Institute of MIT and Harvard (USA). A truly global initiative, there are now more than 3,100 HCA members, from 98 countries around the world. https://www.humancellatlas.org
4. https://www.cell.com/cell/fulltext/S0092-8674(22)01415-5?_returnURL=https%3A%2F%2Flinkinghub.elsevier.com%2Fretrieve%2Fpii%2FS0092867422014155%3Fshowall%3Dtrue
5. Experimentation showed that IL-1β, a cytokine produced by immune cells, directly induced airway epithelial progenitor cells to differentiate into mature lung lining cells. They do this by decreasing SOX9 expression and proliferation, driving lung epithelial progenitor cells to stop self-renewal.

Publication:
J.L. Barnes et al. (2023) ‘Early human lung immune cell development and its role in epithelial cell fate.' Science Immunology. DOI: 10.1126/sciimmunol.adf9988

Funding:
This research was supported by Wellcome. For full funding acknowledgements, please refer to the publication.

Selected websites:

About UCL (University College London)
UCL was founded in 1826. We were the first English university established after Oxford and Cambridge, the first to open up university education to those previously excluded from it, and the first to provide systematic teaching of law, architecture and medicine. We are among the world’s top universities, as reflected by performance in a range of international rankings and tables. UCL currently has over 39,000 students from 150 countries and over 12,500 staff. Our annual income is more than £1 billion. www.ucl.ac.uk | Follow us on Twitter @uclnews | Watch our YouTube channel YouTube.com/UCLTV

The Wellcome Sanger Institute
The Wellcome Sanger Institute is a world leader in genomics research. We apply and explore genomic technologies at scale to advance understanding of biology and improve health. Making discoveries not easily made elsewhere, our research delivers insights across health, disease, evolution and pathogen biology. We are open and collaborative; our data, results, tools, technologies and training are freely shared across the globe to advance science.

Funded by Wellcome, we have the freedom to think long-term and push the boundaries of genomics. We take on the challenges of applying our research to the real world, where we aim to bring benefit to people and society.

Find out more at www.sanger.ac.uk or follow us on Twitter, Instagram, Facebook, LinkedIn and on our Blog.

About Wellcome
Wellcome supports science to solve the urgent health challenges facing everyone. We support discovery research into life, health and wellbeing, and we’re taking on three worldwide health challenges: mental health, infectious disease and climate and health. https://wellcome.org/

---

JOURNAL

Science Immunology

DOI

10.1126/sciimmunol.adf9988 

METHOD OF RESEARCH

Observational study

SUBJECT OF RESEARCH

Human tissue samples

ARTICLE TITLE

Early human lung immune cell development and its role in epithelial cell fate

ARTICLE PUBLICATION DATE

15-Dec-2023

 

Mothers and children have their birthday in the same month more often than you’d think – and here’s why

Study of more than ten million births finds shared birth months are statistically common

Peer-Reviewed Publication

TAYLOR & FRANCIS GROUP

Do you celebrate your birthday in the same month as your mum?  If so, you are not alone. The phenomenon occurs more commonly than expected – a new study of millions of families has revealed. 

 

Siblings also tend to share month of birth with each other, as do children and fathers, the analysis of 12 years’ worth of data shows, whilst parents are also born in the same month as one another more often than would be predicted. 

 

Previous research has found that women’s season of birth somehow influences that of their children. But this research, published today in the peer-reviewed journal Population Studies, is the first to show that women are more likely to have children in the same month as their own birth. 

 

The researchers from Spain and the US analyzed official data on more than 10 million births.  They looked all births in Spain from 1980 to 1983 and from 2016 to 2019 and all births in France from 2000 to 2003 and from 2010 to 2013. 

 

The records provided the child’s month of birth, as well as those of their parents and the sibling that was closest to them in age. 

 

Births in a particular country tend to follow a pattern, with more babies being born at certain times of the year than at others. This is known in academic literature as birth seasonality. 

 

But when the researchers divided the birth data into groups based on the month of birth of the mothers, the births didn’t follow the expected pattern.  

 

Instead, there was a spike in January births among the mothers who were born in January, a spike in February babies in the mothers who were born in February and so on.  

 

Overall, there were 4.6% more births in which mother and child shared the same birth month than would be expected.  

 

This was true for both countries and all four time periods studied.  

 

It was also the case for siblings (there were 12.1% more births than expected in which adjacent siblings had the same month of birth), parents with the same month of birth (4.4% more births) and when a child had the same birth month as their father (2% more births). 

 

A second, less detailed, analysis of all the births in Spain from 1980 to 2019 and all births in France from 2000 to 2019, confirmed the result. 

 

The phenomenon likely has its roots in relatives sharing socio-demographic characteristics: people of similar backgrounds are known to pair up and to be more likely to give birth at certain times of the year, say researchers Dr. Adela Recio Alcaide, of the University of Alcalá in Spain, and Professor Luisa N. Borrell, of the City University of New York in the United States. 

 

In Spain, for example, a woman with a higher education is more likely to give birth in the spring than woman without a higher education. If she has a daughter, in addition to being more likely to be born in the spring, this daughter may be more likely to have higher education, since her mother has it. And thus, when this daughter has children, she will be more likely to have them in the spring too.  

 

That is, this daughter will be more likely to have children in the same season in which she was born because she has kept her family sociodemographic characteristics – specifically the higher education– which make her more likely to give birth at a given time – spring – and, as a result, the season – and even month – of birth is passed between the generations. 

 

Factors that can affect the biology of fertility, such as availability of food and exposure to sunlight, can also vary according to a person’s background. 

 

“What could cause the higher probabilities of family members being born in the same season? The potential explanations seem to be both social and biological,” states Dr. Adela Recio Alcaide, an epidemiologist at the University of Alcala. 

 

“The excess of children with a father and mother born in the same month seems to be due to social or behavioral causes prior to conception that relate to the choice of a partner born in the same month, as we have observed this excess with marriage statistics, with spouses being more likely to mate with someone from the same month.” 

“This,” adds co-author Professor Luisa Borrell, from The City University of New York, “may not be surprising considering things such as partnerships tend to be formed by people with similar socio-demographic characteristics”. 

 

“Moreover, biological factors that are known to affect birth seasonality—such as photoperiod exposure, temperature, humidity, and availability of food—also depend on socio-demographic characteristics, since different social groups are exposed to these biological factors to varying degrees,” Professor Borrell, a social epidemiologist at the City University’s Department of Epidemiology & Biostatistics, Graduate School of Public Health & Health Policy, says. 

 

The study’s strengths include the large number of births included in the analysis and the inclusion of data from different decades and different countries.  However, one limitation is that the analysis assumes an “independence of outcomes but that might not be the case and, therefore, dependence of the outcomes within families may have affected findings”. To adjust for this, the team repeated their analyses to account for dependency of outcomes within families and the results were very similar to those presented. 

 

While this is a novel finding, further research is needed to confirm and deepen the results and their implications. 

 

Concluding, the authors outline the importance that the link between family characteristics and birth month is considered in any future research into how a child’s month of birth affects their health, educational and other outcomes. 

---

JOURNAL

Population Studies

DOI

10.1080/00324728.2023.2272983 

METHOD OF RESEARCH

Data/statistical analysis

SUBJECT OF RESEARCH

People

ARTICLE TITLE

Is there an association between family members? season of birth that could influence birth seasonality? Evidence from Spain and France

ARTICLE PUBLICATION DATE

14-Dec-2023

WAIT, WHAT?!

Mice with humanized immune systems to test cancer immunotherapies

Peer-Reviewed Publication

KOBE UNIVERSITY

 

IMAGE: 

CURRENTLY DEVELOPED CANCER IMMUNOTHERAPIES MODIFY THE INTERACTION OF CANCER CELLS AND THE IMMUNE SYSTEM, MAKING DRUG TESTING TARGETING HUMAN CANCER OUTSIDE OF CLINICAL TRIALS DIFFICULT. KOBE UNIVERSITY IMMUNO-ONCOLOGIST SAITO YASUYUKI AND HIS TEAM DEVELOPED A MOUSE MODEL WITH A HUMANIZED IMMUNE SYSTEM. WITH THIS THEY SUCCESSFULLY TESTED A NEW THERAPEUTIC APPROACH IN WHICH IMMUNE CELLS THAT PROTECT CANCER CELLS GET ACTIVATED TO ATTACK THEM, BY DISABLING THE IMMUNE CELLS’ RECOGNITION SYSTEM FOR CELLS BELONGING TO THE OWN BODY.

view more 

CREDIT: SAITO YASUYUKI (ILLUSTRATION CREATED WITH BIORENDER.COM)

Mice with human immune cells are a new way of testing anti-cancer drugs targeting the immune system in pre-clinical studies. Using their new model, the Kobe University research team successfully tested a new therapeutic approach that blindfolds immune cells to the body’s self-recognition system and so makes them attack tumor cells.

Cancer cells display structures on their surface that identify them as part of the self and thus prevent them from being ingested by macrophages, a type of immune cell. Cancer immunotherapy aims at disrupting these recognition systems. Previous studies showed that a substance that blinds macrophages to one of these identifiers, called “CD47,” by disabling their CD47-scanning structure, “SIRPα,” can activate the cells to fight the tumor when given in combination with therapeutic cancer-targeting antibodies such as Rituximab. However, because this approach is so specific to the self-identification of human cells, until now it could only be tested in humans or monkeys, making pre-clinical studies in mice impossible.

To overcome this, Kobe University immuno-oncologist SAITO Yasuyuki and his team built on their experience with creating mouse immunological models and transplanted parts of the human immune system into mice. Saito says, "Studies using mouse models with humanized immune systems have focused on lymphocytes, a type of immune cell relevant to infectious diseases.

The special aspect of our approach is that our new mouse model focuses on macrophages because we want to target them for the development of new cancer immunotherapies." This enabled the researchers to both create a more fully functioning mouse model of human cancer and test the effectiveness of the blindfolding approach for the first time in this environment.

Their results, published in the journal Frontiers in Immunology, showed that the macrophage-targeted therapy indeed induced an effective cancer response. However, Saito explains, "The most exciting aspect of this result is that this approach not only promotes the engulfment (ingestion) of tumor cells by macrophages but also reprograms tumor-associated macrophages, one of the current topics of cancer immunotherapy."

The immune system has an ambiguous role in the development of and fight against cancer. On the one hand, it can recognize cancer cells and fight them. On the other hand, macrophages also associate with tumors, both supporting their growth and suppressing other anti-tumor immune responses. To turn these cells against cancer is the novel approach that the Kobe University researchers could now help propel forward with their new humanized mouse model.

But the result has a broader relevance, too. Saito says, "There were no suitable preclinical in vivo models to develop therapeutics targeting human macrophages surrounding tumors, so new approaches had to be tested directly on patients. I believe our model perfectly fills the gap and may help in the selection of the most effective treatment from several candidates for therapeutics targeting human immune cells. The long-term goal of my project is to develop a humanized immune system mouse model that faithfully represents the immune response against the tumor."

The new treatment approach is effective in combating cancer. 14 days after the onset of the treatment, the mice having received the treatment (right) have much smaller tumors (shown through bioluminescence intensities) than those who received only a control (left).

CREDIT

SAITO Yasuyuki

This study was supported by the Ministry of Education, Culture, Sports, Science, and Technology of Japan Grant-in-Aids 20K21547, 21H04807 and 20K16358; by Japan Agency for Medical Research and Development (AMED) grants 21cm0106308h0006 and 22674074; by Japan Science and Technology Agency (JST) grant JPMJPF2018; by the Bristol-Myers Squibb Foundation, the Takeda Science Foundation, and by the Japanese Society of Hematology. It was conducted in collaboration with researchers from the University and University Hospital Zurich and the Comprehensive Cancer Center Zurich.

Kobe University is a national university with roots dating back to the Kobe Commercial School founded in 1902. It is now one of Japan's leading comprehensive research universities with nearly 16,000 students and nearly 1,700 faculty in 10 faculties and schools and 15 graduate schools. Combining the social and natural sciences to cultivate leaders with an interdisciplinary perspective, Kobe University creates knowledge and fosters innovation to address society’s challenges.

---

JOURNAL

Frontiers in Immunology

DOI

10.3389/fimmu.2023.1294814 

METHOD OF RESEARCH

Experimental study

SUBJECT OF RESEARCH

Animals

ARTICLE TITLE

Preclinical evaluation of the efficacy of an antibody to human SIRPα for cancer immunotherapy in humanized mouse models

ARTICLE PUBLICATION DATE

14-Dec-2023

H G WELLS THE ISLAND OF DR. MOREAU

 

Not to go on all-fours; that is the Law. Are we not men? Not to suck up Drink; that is the Law. Are we not men? Not to eat Fish or Flesh; that is the Law. Are we not men? Not to claw the Bark of Trees; that is the Law. Are we not men? Not to chase other Men; that is the Law. Are we not men?

ISLAND OF LOST SOULS, BW, 1921

Facial symmetry doesn’t explain “beer goggles”

A new study has tested the hypothesis that people are more likely to find someone attractive while drunk, because their face appears more symmetrical

Peer-Reviewed Publication

UNIVERSITY OF PORTSMOUTH

If you thought blurry eyes were to blame for the “beer goggles” phenomenon, think again.

Scientists from the University of Portsmouth have tested the popular theory that people are more likely to find someone attractive while drunk, because their faces appear more symmetrical. 

The term “beer goggles” has been used for decades to describe when a person finds themselves sexually attracted to someone while intoxicated, but not sober.

One possible explanation for the effect is that alcohol impairs the drinker’s ability to detect facial asymmetry, thus making potential partners more visually appealing.

Existing research has shown that a part of what makes people attractive to others is how well both sides of their face match. The thinking goes, the more symmetry the better the gene pool. But when alcohol is introduced, it’s thought a person is less likely to notice if the faces around them are non-symmetrical.

However, a new experiment found that while alcohol did impair face symmetry detection, it had no influence on facial attractiveness judgements. 

Dr Alistair Harvey from the University of Portsmouth’s Department of Psychology, said: “Alcohol is a strong predictor of sexual behaviour, often consumed before or during dates.

“There are a range of possible reasons why alcohol drinkers are more inclined to engage in sex, including a lack of inhibition, heightened expectations, personality traits, and the beer goggles effect.

“Due to the limited research on this topic, we ran a field experiment to help determine why people often experience unexpected – and regretted – sexual escapades after having one too many.”

To gather the results, the team visited a local pub in the Portsmouth area. 99 men and women volunteered for the study, ranging in age from 18 to 62 years old. 

They were asked to rate 18 individual faces for attractiveness and symmetry. Each type of rating was given twice, once for faces showing an enhanced asymmetry, and again for the same faces in their natural form. Participants then judged which of two same-face versions (one normal, the other perfectly symmetrised) was more attractive and, in the final task, more symmetrical.

The study used a robust procedure, taking ratings of individual faces in addition to the usual binary approach where participants select the more attractive or symmetrical face in a pair. 

As predicted, heavily intoxicated individuals were less able to distinguish natural from perfectly symmetrised faces than more sober drinkers. But the more drunk viewers did not rate the faces as being any more attractive. 

As expected, both male and female participants rated natural faces as being more attractive than the ones which were doctored to look wonky. But, surprisingly, this bias was stronger among women.

The paper, published in the Journal of Psychopharmacology, says one possible explanation to the findings could be that attractiveness depends on many factors that simply swamp the small effects of face symmetry.

“We don’t deny the existence of a “beer goggles” effect”, added Dr Harvey.

“But we suspect it would be more easily detectable when using live models for an experiment, instead of static photographs. Images conceal a range of important visual criteria for attractiveness, including build, body shape, height, expression, and clothing.

“Therefore, further research is needed to find the missing piece to the puzzle.”

---

JOURNAL

Journal of Psychopharmacology

DOI

10.1177/02698811231215592 

METHOD OF RESEARCH

Experimental study

SUBJECT OF RESEARCH

People

ARTICLE TITLE

Impaired face symmetry detection under alcohol, but no ‘beer goggles’ effect

 

Multiple sclerosis: Possible basis for vaccine researched

Researchers identified immune cells as a potential key factor for protection against MS disease

Peer-Reviewed Publication

MEDICAL UNIVERSITY OF VIENNA

The underlying cause of MS has not yet been fully clarified, but a connection with the Epstein-Barr virus (EBV) has long been suspected. In most patients who develop MS, specific immune responses against EBV are detectable, which are also directed against certain structures of the central nervous system and thus contribute to the development of MS. Until now, however, it was unclear why an EBV infection, one of the most common and lifelong persistent viral infections in humans, only leads to MS in a small number of people. A research group at the Centre for Virology led by Elisabeth Puchhammer-Stöckl, in cooperation with a team from the Department of Neurology at the Medical University of Vienna led by Thomas Berger and Paulus Rommer, has now shown that the risk of MS is particularly high in people with a combination of certain host factors and virus variants.

Natural killer cells as a potential protective factor
To be specific, the investigations revealed a greatly increased risk of MS, if, on the one hand, the EBV-specific and autoreactive immune responses are strong and, on the other hand, the patients are unable to control this autoimmunity efficiently. The study authors identified a subgroup of the natural killer cells of the human immune system as a potential key factor for protection against MS. "These immune responses could therefore play a decisive role in the development of future vaccines," says Hannes Vietzen from the Centre for Virology, first author of the study, describing the new possibilities that arise from the research work with regard to the prevention and early detection of MS. According to the investigations, the development of MS proved to be dependent on certain genetic factors as well as on infection with a specific EBV virus variant, which, according to the laboratory experiments, leads to a significantly weakened immune response against the autoreactive processes and thus contributes to the development of MS. "It may be helpful to analyse the EBV variants detected in these patients in order to identify patients at risk at an early stage," says Hannes Vietzen in the run-up to further studies that are intended to deepen these findings.

 

 

 

---

JOURNAL

Cell

DOI

10.1016/j.cell.2023.11.015 

ARTICLE TITLE

Ineffective Control of Epstein-Barr Virus-Induced Autoimmunity Increases the Risk for Multiple Sclerosis

ARTICLE PUBLICATION DATE

12-Dec-2023