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Thursday, October 27, 2022

Mobius Says China May Ease Covid Zero by End-2022 to Aid Economy

  • No choice but to open as government needs money, Mobius says
  • Veteran investor says he’s turned “more negative” on China

 

China will probably ease its disruptive Covid Zero policy by the end of this year as its economy is in trouble and the government needs money “badly,” according to veteran emerging-markets investor Mark Mobius.

“I don’t think Covid is an issue going forward,” Mobius said in response to queries from Bloomberg News. “China has no choice but to open up to ensure the economy can function."

https://www.bloomberg.com/news/articles/2022-10-28/mobius-says-china-may-ease-covid-zero-by-end-2022-to-aid-economy

'Developmental-behavioral pediatricians can diagnose most autism cases in young children without ADOS testing'

 Trained developmental-behavioral pediatricians can generally diagnose autism spectrum disorder (ASD) in young children without the need for additional Autism Diagnostic Observation Schedule (ADOS) testing, finds a prospective multicenter study. The study, conducted through the Developmental Behavioral Pediatrics Research Network (DBPNet) and led by Boston Children's Hospital, was published in JAMA Pediatrics.

The ADOS was originally developed as a research tool. Through semi-structured observations, specially trained evaluators assess children's communication skills, , and imaginative use of materials.

"The ADOS was never designed to be used in the clinic," says William Barbaresi, MD, the study's principal investigator and chief of the Division of Developmental Medicine at Boston Children's. "But currently, ADOS testing is often required for  to receive an ASD diagnosis that is accepted by early intervention agencies, schools, and insurers. This study shows that in the majority of cases, young children may be able to have a  for ASD by a developmental-behavioral pediatrician without using the ADOS."

ADOS administration is time consuming, adds additional cost to the diagnostic process, and there are not enough people trained to administer it. "The requirement for ADOS testing has become a barrier to timely diagnosis and initiation of treatment," Barbaresi says. "Young children can wait months or even years for an assessment, making it difficult for them to access intensive early intervention services when they are most effective—ideally starting at around 24 months of age."

The study involved 349 children aged 18 months to 5 years who were evaluated at nine academic pediatric centers. Developmental-behavioral pediatricians (DBPs) first made a diagnosis based on their clinical assessment. A specially trained clinician then administered the ADOS, the results of which were shared with the DBP, who then could revise their diagnosis.

In 90 percent of cases, the diagnosis including the ADOS was consistent with the original clinical diagnoses. Consistency was most likely when the clinician felt highly certain of their original diagnosis.

"Overall, this study is good news," says Barbaresi. "We believe it has the potential to change  by reducing wait times for diagnostic evaluations so that children can receive early, intensive treatment for ASD."


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Clinical diagnoses of autism spectrum disorder mostly consistent with, without Autism Diagnostic Observation Schedule

More information: William Barbaresi et al, Clinician Diagnostic Certainty and the Role of the Autism Diagnostic Observation Schedule in Autism Spectrum Disorder Diagnosis in Young Children, JAMA Pediatrics (2022). DOI: 10.1001/jamapediatrics.2022.3605
https://medicalxpress.com/news/2022-10-developmental-behavioral-pediatricians-autism-cases-young.html

Why immunotherapy works well for some cancer patients, but not others

 Immunotherapy, a biotherapy that boosts the ability of the immune system to recognize and attack mutant tumor cells, has transformed the treatment landscape for patients battling cancer, which emerges from the progressive accumulation of DNA mutations. However, many patients do not respond to immunotherapy. For instance, among highly-mutated colorectal and endometrial cancers, research has shown that only half will show a response to immunotherapy.

A new study by Yale School of Medicine researchers published Oct. 27 in the journal Cancer Discovery has identified a possible explanation for why this happens. In an analysis of a phase 2 trial investigating the immunotherapy drug pembrolizumab in 24 patients with , the Yale team identifies a specific mechanism of faulty DNA repair in tumors as a key factor in determining patient outcomes.

"We wanted to understand why some patients respond better than others to immunotherapy," said co-corresponding author Ryan Chow, an M.D./Ph.D. candidate working in Yale's Department of Genetics and the Systems Biology Institute.

For the study, the Yale team focused on the failure of a process known as "mismatch repair." When cells divide, errors often arise in their DNA. Through mismatch repair, a special group of proteins recognizes and corrects errors in the DNA. A breakdown in this editing process occurs in many different types of , however, leading to high mutation levels.

The research team—led by Chow, Dr. Eric Song, an ophthalmology resident and former M.D./Ph.D. student at Yale, and Dr. Alessandro Santin, a professor of obstetrics, gynecology, and reproductive sciences—zeroed in on the fact that mismatch repair deficiency can result from two distinct mechanisms.

In one, mutations occur in the DNA repair machinery itself, leading to the production of defective repair proteins; in the second, production of the DNA repair machinery is halted entirely. In both cases, the tumors accumulate very high levels of mutations that would be expected to make them good candidates for immunotherapy.

"An analogy would be a dysfunctional toy factory," Chow said. "Maybe the factory makes broken toys that don't work, or the factory has no personnel and stops producing toys altogether. Either way, kids won't be happy."

However, the researchers found that tumors with defective DNA repair proteins had significantly better responses to immunotherapy than those in which the production of DNA repair proteins had been silenced. These differences could ultimately be traced to changes in the  that was mounted against each of the two classes of tumors, they said.

"When it comes to immunotherapy, it seems that the journey—in this case, the underlying cause of  deficiency—may be just as important as the destination," Chow said.

Song added that "the innovative use of clinical trial data can guide our understanding of how  manipulates the  and ultimately improve how we treat patients."


Explore further

FDA approves cancer drug for personalized immunotherapy approach

More information: Ryan Chow et al, Distinct mechanisms of mismatch repair deficiency delineate two modes of response to PD-1 immunotherapy in endometrial carcinoma, Cancer Discovery (2022). DOI: 10.1158/2159-8290.CD-22-0686
https://medicalxpress.com/news/2022-10-explanation-immunotherapy-cancer-patients.html

After rehab for opioids, nearly half of Medicaid beneficiaries do not receive follow-up care

 Despite strong evidence for the importance of outpatient care after inpatient residential treatment for opioid use disorder, nearly half of Medicaid beneficiaries are not receiving follow-up care or medication-assisted treatment within a month of discharge, according to a new analysis led by University of Pittsburgh School of Public Health scientists.

Discharge from residential treatment is a sensitive time when people with  are at higher risk to relapse. Outpatient treatment with counseling, medication or both can reduce this risk. The findings, published this week in Drug and Alcohol Dependence, are the first to study patient and episode-level factors related to the likelihood of receiving post-discharge follow-up among recipients of Medicaid, which is the largest payer of opioid use disorder-related inpatient stays and emergency department visits.

"Over the past few years, Medicaid programs have really expanded the scope of substance use disorder treatments they will cover, including residential treatment," said lead author Evan Cole, Ph.D., research associate professor in the Department of Health Policy and Management at Pitt Public Health. "But outpatient follow-up is key to predicting long-term recovery, and there is very little research—particularly in the past decade when the opioid epidemic has gripped the U.S.—into whether that critical follow-up care is actually happening."

An estimated 10 million Americans have misused opioids in the past year, and more than 100,000 people died of drug overdoses in the U.S. last year, the majority after taking opioids, according to the U.S. Centers for Disease Control and Prevention. Residential treatment for substance use disorder—commonly known as "rehab"—includes 24-hour living support with on-site clinical services, which can include counseling and addiction treatment. Most residential treatment stays are less than 30 days.

Medicaid provides  for low-income or disabled people, and, with more than 88 million enrollees, it is the largest health insurer in the U.S. It covers 38% of people with opioid use disorder.

Cole and his colleagues looked at data from more than 90,000 residential treatment stays in 2018 and 2019 for Medicaid beneficiaries across 10 states—Delaware, Kentucky, Maryland, Michigan, North Carolina, Ohio, Pennsylvania, Tennessee, Virginia and West Virginia—using the Medicaid Outcomes Distributed Research Network.

Previous research has shown that after leaving residential treatment, timely follow-up for outpatient addiction treatment, which can include medications such as buprenorphine, methadone or naltrexone, reduces relapse and lowers risk of death.

Cole's team found that 47% of the time, Medicaid beneficiaries discharged from residential treatment did not receive follow-up care or a medication for opioid use disorder within 30 days. Medicaid enrollees who were male, lived in rural areas or were members of racial and ethnic minority groups were the least likely to receive follow-up care.

"This was not what we'd hoped to see," said Cole, who is also research director of the Medicaid Research Center at Pitt. "I'm sure Medicaid programs want people to be engaged in outpatient care to continue their treatment and successfully manage opioid use disorder after residential treatment."

On a positive note, patients who had been prescribed medications to treat opioid use disorder before they'd been admitted to residential treatment were 24% more likely to get follow-up care and medication after discharge than their counterparts who hadn't had such a prescription before entering residential treatment.

Cole hypothesized that previous engagement in addiction treatment made it easier for patients to navigate to treatment after discharge. He said future research could test this by exploring whether patients were seeing the same outpatient provider before and after residential treatment, and, if so, more effort could be made to connect patients to outpatient providers before they enter residential treatment.

Since Medicaid enrollment soared by 25% during the COVID-19 pandemic, it will be interesting to see if that impacted connection with care after residential treatment, Cole said. He also noted that some states, including Pennsylvania, have become more committed to "warm handoffs," creating protocols intended to facilitate a seamless transition to addiction treatment after an emergency.

"While our study wasn't designed to see the impact of warm hand-off protocols, it certainly indicates that exploring whether or not these programs are working could be worthwhile for future research," Cole said.


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Outpatient visits are critical to success of treating opioid-use disorder, researchers find

More information: Evan S. Cole et al, Outpatient Follow-Up and Use of Medications for Opioid Use Disorder after Residential Treatment among Medicaid Enrollees in 10 States, Drug and Alcohol Dependence (2022). DOI: 10.1016/j.drugalcdep.2022.109670
https://medicalxpress.com/news/2022-10-rehab-opioids-medicaid-beneficiaries-follow-up.html

Cancer therapy shows potential to treat severe COVID-19 in pre-clinical trials

 An article published in Science Advances suggests that a type of cancer treatment known as immune checkpoint blockade may be beneficial in certain cases of severe COVID-19. The creators of this therapy, which can successfully activate the immune system to fight cancer, won the 2018 Nobel Prize in Physiology or Medicine.

The findings reported by the authors were based on experiments involving cells from patients treated in  units (ICUs) after being infected by SARS-CoV-2, and mice infected by MHV-A59 (murine hepatitis virus A59), another betacoronavirus.

"PD-1 blockade is one of the known immune checkpoint therapies and one of the therapies we analyzed in the study. It tells T lymphocytes [a type of white blood cell] to stop responding to infection after a time so that the response is not excessive. In cases of cancer, sepsis and severe COVID-19, however, PD-1 makes T cells stop functioning even before the disease has been resolved and must therefore be blocked," said Pedro Moraes-Vieira, one of the leaders of the study. Moraes-Vieira is a professor at the State University of Campinas's Institute of Biology (IB-UNICAMP).

"These are very expensive treatments, but we believe it could be a viable option because there aren't as many critical patients as there were at the start of the pandemic, provided further research confirms that it's safe for COVID-19 patients," Moraes-Vieira said.

Murine coronavirus

The hypothesis tested in the study arose when Uruguayan researchers (co-authors of the article) observed that mice that did not express the protein TMEM176D responded more acutely to infection by MHV-A59. This protein regulates inflammasomes, protein complexes deployed by the innate  to trigger inflammation as a weapon against tumors, viruses and bacteria.

Inflammasome activation is more intense without TMEM176D. More  are released, including interleukin-1 beta (IL-1β), which is known to play a role in severe COVID-19.

"Excessive release of IL-1β leads to T lymphocyte dysfunction, which we call T cell exhaustion," Moraes-Vieira said. "These cells are so strongly activated that they can no longer respond adequately. This is common in chronic viral diseases like severe COVID-19, as we found in a study conducted early in the pandemic."

An article on the study in question, published in 2020 in the Journal of Experimental Medicine, is one of the most cited articles published in this journal in the last three years and motivated the Uruguayan team to propose a partnership.

In the trials involving mice, treatment with a PD-1 inhibitor restored T cell functionality. In addition, the researchers had access to blood from healthy donors and COVID-19 patients hospitalized at two institutions in Montevideo, Uruguay's capital.

Experiments involving healthy cells infected with SARS-CoV-2 were conducted at UNICAMP's Laboratory of Emerging Virus Studies (LEVE) headed by Professor José Luiz Proença Módena, a co-author of the article

In trials involving human blood samples, only cells that came from patients in intensive care benefited from the administration of atezolizumab, a PD-1 inhibitor used in the study. This was because of inflammasome overactivation leading to exhaustion and dysfunction of adaptive immunity in these patients.

The findings should be considered with caution, the researchers warn. Studies involving cancer patients who were treated in this manner before contracting COVID-19 showed no benefits or pointed to negative results.

In one study, administration of the therapy before viral infection did not lead to an improvement in COVID-19. In another study, involving 423 patients, there were more cases of hospitalization and severe disease among those who had been given the inhibitor. On the other hand, a clinical trial of PD-1 inhibitors in sepsis patients showed the therapy to be safe. More research will therefore be needed to glean a deeper understanding of the effects of the treatment in the context of COVID-19.


Explore further

In pre-clinical trials, drug shows potential to combat exaggerated inflammation associated with COVID-19

More information: PD-1/PD-L1 blockade abrogates a dysfunctional innate-adaptive immune axis in critical β-coronavirus disease, Science Advances (2022). DOI: 10.1126/sciadv.abn654

Tamara S. Rodrigues et al, Inflammasomes are activated in response to SARS-CoV-2 infection and are associated with COVID-19 severity in patients, Journal of Experimental Medicine (2020). DOI: 10.1084/jem.20201707


https://medicalxpress.com/news/2022-10-cancer-therapy-potential-severe-covid-.html

Biology of frontotemporal dementia

 Dementia encompasses a range of neurodegenerative conditions that lead to memory loss and cognitive deficiencies and affect some 55 million people worldwide. Yet despite its prevalence, there are few effective treatments, in part because scientists still don't understand how exactly dementia arises on a cellular and molecular level.

Now, a team led by scientists at Harvard Medical School and Harvard T. H. Chan School of Public Health has made progress in unraveling the mechanism underlying a type of dementia that strikes early in life.

In a study published Oct. 7 in Nature Communications, researchers discovered that a genetic form of  (FTD) is associated with accumulation of specific lipids in the brain—and this accumulation results from a protein deficiency that interferes with cell metabolism.

The results, based on experiments in human brain cells and in animal models, provide new insights into FTD that could inform the design of new therapies. Additionally, the findings highlight a mechanism of metabolic disruption that may be relevant in other forms of , the researchers said.

A black box

There are several different types of dementia, each with complicated genetics that involve various mutations. FTD, characterized by a loss of cells in the frontal and temporal lobes of the brain, accounts for 5 to 10 percent of dementia cases. Often diagnosed in patients between 45 and 65 years old, the genetic forms tend to cluster in families. Around 15 percent of the time, FTD is linked to a specific mutation in the GRN gene, which causes brain cells to stop making a protein called .

Previous studies have linked progranulin to parts of the cell called lysosomes, which are responsible for cleanup and other metabolic activities in cells. However, "the function of the protein, including its role in the , has remained sort of a black box," said co-senior author Wade Harper, the Bert and Natalie Vallee Professor of Molecular Pathology in the Department of Cell Biology in the Blavatnik Institute at HMS.

Harper collaborated on the study with co-senior authors Tobias Walther and Robert Farese Jr., who were professors of cell biology at HMS and professors of molecular metabolism at Harvard Chan School when they conducted the research, as well as lead authors Sebastian Boland, a former research fellow in the Farese & Walther Lab, and Sharan Swarup, a former research fellow in the Harper lab.

The researchers initially found that progranulin-deficient human cell lines and mouse brains, as well as brain cells from patients with FTD, had an accumulation of gangliosides—lipids commonly found throughout the nervous system.

Next, the team used recently developed technology for purifying lysosomes to analyze the types and amounts of proteins and lipids present inside them. Using this technique, the scientists found that lysosomes in these cells and tissues from brains with FTD had reduced levels of progranulin, as well as lower-than-normal levels of a lipid called BMP, which is required to break down gangliosides, the lipids commonly found in the central nervous system. However, when researchers added BMP to cells, they observed that these cells accumulated far lower levels of gangliosides.

Together, the findings suggest that progranulin in lysosomes helps maintain the BMP levels needed to prevent gangliosides from accumulating in brain cells—buildup that may contribute to FTD.

"We've uncovered a role for progranulin in supporting proper degradation of gangliosides," while also showing that it may be possible to correct the problem, Farese said.

"People are already working on treatments that involve giving patients a source of progranulin, and our results are consistent with that approach potentially being therapeutically beneficial," Walther added. Moreover, it may be possible to develop therapies that focus on replacing BMP rather than progranulin, he said, and thus target a different part of the mechanism.

The researchers also think that a similar lysosome-based mechanism could be relevant for neurodegenerative diseases beyond FTD—an idea that they note is rapidly gaining ground in the field.

"The lysosome may be a key feature of many kinds of neurodegenerative diseases—but these diseases likely all connect with the lysosome in different ways," Harper said. For example, scientists already know that a protein implicated in a genetic form of Parkinson's disease controls aspects of lysosomal function. More research is needed, Farese added, to understand precisely how various lipids and proteins interact with lysosomes within the context of different neurodegenerative diseases.

Now, the researchers are studying several genes linked with lysosomal function, including genes associated with lysosomal storage diseases, to find connections between them. A central remaining question is how progranulin elevates BMP levels in the . Additional studies are needed to further elucidate the steps of the mechanism the team uncovered and to explain how  translates into .

"This study demonstrates the power of collaboration and following the science," Walther said. "By using the right tools and asking the right detailed questions, you can sometimes uncover things that are unexpected."


Explore further

Granulins are brain treasure, not trash

More information: Sebastian Boland et al, Deficiency of the frontotemporal dementia gene GRN results in gangliosidosis, Nature Communications (2022). DOI: 10.1038/s41467-022-33500-9
https://medicalxpress.com/news/2022-10-basic-biology-frontotemporal-dementia.html

College students suffer more than 100 alcohol-related consequences in 4 years: study

 On average, students experience an estimated total of 102 alcohol-related consequences, such as blacking out, being hung over, or missing work or school, due to drinking across their four years in college, according to a new study led by Penn State. The research also revealed that students who think their parents disapprove of the consequences of drinking are likely to experience fewer negative consequences from drinking during college.

"We often think of peers as having an influence on drinking behaviors, but we found that parents can make a difference, even after their child has left home," said Kimberly Mallett, research professor at the Edna Bennett Pierce Prevention Center and a clinical psychologist.

The research team surveyed students at a large, public northeastern U.S. university about how many alcohol-related consequences they experienced and which predictors resulted in higher rates of consequences. Although the work was conducted at a single university, the researchers said the findings likely apply to students at all colleges and universities. The findings are published in the journal Addictive Behaviors.

The team followed 1,700 students for four years, surveying them twice a year. The surveys included questions to determine the amount of alcohol students were drinking, as well as the total number of alcohol-related consequences students experienced across all four years of college, as well as questions about why people experience consequences and how they view them.

Specifically, the surveys assessed the prevalence of 21 possible consequences from drinking and focused on whether they thought their parents would disapprove of 12 of those consequences, including blacking out, being hung over, or missing work or school due to drinking, said Shannon Glenn, Penn State doctoral candidate in biobehavioral health and the paper's lead author.

The team found that the average number of alcohol-related consequences per student over the four-year period was 102. The amount of alcohol students drank impacted the total number of consequences they experienced. As drinking increased, so did consequences, Glenn said.

The most common consequence, with 96.7% of respondents experiencing at least once during the four years, was 'having a hangover the morning after drinking.' This was followed by 'saying or doing embarrassing things,' which affected 96.1% of respondents at least once. Nearly 25% of respondents said they had 'been pressured or forced to have sex with someone because they were too drunk to prevent it.'

"More than 70% of respondents said they 'needed larger amounts of alcohol to feel any effect,' which is concerning because this indicates increased tolerance to alcohol and is an early risk factor for developing an alcohol use disorder," said Mallett, who is a co-author on the paper.

The surveys also assessed students' beliefs about how their parents would react to their drinking, by asking, "How would your mother/father respond if she/he knew you experienced [specific consequence] as a result of your drinking?"

"The research shows that parents have an influence on students' drinking habits and whether they experience problems from drinking," Mallett said.

Students who thought their parents would disapprove of alcohol-related consequences had fewer such consequences overall. A previous Penn State study found that students who think their parents approve of drinking may drink more.

"Kids really look to their parents for guidance in a lot of ways even if they don't outwardly say it," Mallett said. She suggested these practices for parents:

  • Talk about the possible serious consequences of drinking, emphasizing that you are having the conversation out of love and care for them.
  • Discuss approaches to decision-making when confronted with possible drinking scenarios.
  • Brainstorm strategies for not drinking to the point where they are putting themselves at greater risk.
  • Maintain an open dialogue about drinking through their entire college experience.

"It's empowering for parents to know that they can make a difference," Mallett said. "For parents who have been permissive about drinking in the past, it's never too late to switch gears."

Mallett also recommended that colleges develop protocols to identify individuals who are experiencing above average alcohol problems so they can receive intervention or treatment at earlier ages.

The paper's co-authors are Robert Turrisi, Penn State professor of biobehavioral health; Katja Waldron, Penn State doctoral candidate in biobehavioral health; Michael Russell, Penn State assistant professor of biobehavioral health; and Racheal Reavy, technical architect and Tableau specialist with Silverline.

This research was funded by the National Institute on Alcohol Abuse and Alcoholism.


Story Source:

Materials provided by Penn State. Original written by Sara P. Brennen. Note: Content may be edited for style and length.


Journal Reference:

  1. Shannon D. Glenn, Robert Turrisi, Katja A. Waldron, Kimberly A. Mallett, Michael A. Russell, Racheal R. Reavy. Examining the impact of early college experiences on the cumulative number of alcohol-related consequencesAddictive Behaviors, 2022; 132: 107357 DOI: 10.1016/j.addbeh.2022.107357