The man who stole over 50,000 bitcoins from the Silk Road marketplace has pleaded guilty. According to the U.S. Department of Justice, “the seizure was then the largest cryptocurrency seizure” in the history of the DOJ and “remains the department’s second-largest financial seizure ever.”
Silk Road Exploiter Pleads Guilty
The U.S. Department of Justice (DOJ) announced Monday that James Zhong pleaded guilty on Friday “to committing wire fraud in September 2012 when he unlawfully obtained over 50,000 bitcoin from the Silk Road dark web internet marketplace.” The Justice Department also announced a “historic $3.36 billion cryptocurrency seizure” in connection to the case.
The DOJ explained that law enforcement conducted a search at Zhong’s house in Gainesville, Georgia, on Nov. 9, 2021, and “seized approximately 50,676.17851897 bitcoin, then valued at over $3.36 billion,” elaborating:
This seizure was then the largest cryptocurrency seizure in the history of the U.S. Department of Justice and today remains the department’s second-largest financial seizure ever.
Zhong also had about 3,500 more bitcoins from exchanging into BTC over 50,000 bitcoin cash (BCH) which he received following the bitcoin blockchain hard fork in August 2017. He used an overseas cryptocurrency exchange for the conversion.
Besides the BTC seized at his house, Zhong began “voluntarily surrendering to the government additional bitcoin” beginning in March this year, the DOJ revealed, adding that “In total, Zhong voluntarily surrendered 1,004.14621836 additional bitcoin.”
The government is seeking the forfeiture of “approximately 51,680.32473733 bitcoin,” the DOJ noted. At the time of writing, BTC is trading at $20,641.28, so the amount sought by the government is about $1.07 billion.
Zhong’s Scheme to Defraud Silk Road Marketplace
Zhong executed a scheme to defraud the Silk Road marketplace of its money and property in September 2012, the DOJ said, adding that he “was able to withdraw many times more bitcoin out of Silk Road than he had deposited in the first instance.” For example, the Justice Department detailed that on Sept. 19, 2012:
Zhong deposited 500 bitcoin into a Silk Road wallet. Less than five seconds after making the initial deposit, Zhong executed five withdrawals of 500 bitcoin in rapid succession — i.e., within the same second — resulting in a net gain of 2,000 bitcoin.
On Monday, the U.S. government filed an Amended Preliminary Order of Forfeiture in the United States v. Ross Ulbricht case “seeking to forfeit approximately 51,351.89785803 bitcoin traceable to Silk Road, valued at approximately $3,388,817,011.90 at the time of seizure.” Silk Road’s founder, Ross Ulbricht, was convicted in 2015 and is currently serving a double life sentence, plus 40 years without parole.
U.S. District Judge Paul Gardephe also entered a Consent Preliminary Order of Forfeiture on Friday for 154.4268793000044 BTC, $661,900 in cash, 25 Casascius coins (physical bitcoin) worth about 174 BTC, various metals, and Zhong’s 80% interest in Memphis-based RE&D Investments LLC. The metals seized consisted of “four one-ounce silver-colored bars, three one-ounce gold-colored bars, four 10-ounce silver-colored bars, and one gold-colored coin,” the Justice Department highlighted.
Following the DOJ’s announcement, some people on social media began noticing that one of Zhong’s BTC addresses revealed in a court document matches one posted by Bitcointalk user “Loaded.” Bitmex Research tweeted: “In March 2017, Bitcointalk user ‘Loaded’ signed a message from an address with 40,000 bitcoin, asking to do a 1 to 1 swap for ‘Bitcoin Unlimited’ with Roger Ver. It now appears these funds have been seized by the U.S. authorities.”
Commenting on Loaded’s Bitcointalk post, Bitcoin.com founder Ver, stated: “As I recall, he never replied to my DMs about making the bet.”
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Kevin Helms
A student of Austrian Economics, Kevin found Bitcoin in 2011 and has been an evangelist ever since. His interests lie in Bitcoin security, open-source systems, network effects and the intersection between economics and cryptography.
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Scientists in Australia believe that they’ve discovered the centuries-old origins of a rare form of childhood epilepsy caused by a genetic mutation: a single common ancestor who lived in Britain roughly 800 years ago. The find is especially notable because hereditary conditions of this kind typically don’t survive for so long in the population.
Epilepsy is a broad term for recurring bursts of abnormal brain activity that trigger neurological symptoms, most prominently seizures. It can have many different causes, including variations in our genes passed down between families. When these seizures are accompanied by fever, they’re also known as febrile seizures.
This new study, led by researchers at the University of Melbourne’s Epilepsy Research Center, looked at cases of childhood febrile seizures strongly tied to the SCN1Bc.363C>G variant. This variant has been found among multiple unrelated families in Australia, the UK, and the U.S. Many of the families had a long history of early epilepsy, and the disorder appears to be a dominant genetic condition, meaning a disease that can be caused by only having one copy of the bad gene. But the researchers were curious whether this mutation had been passed down by a lone common ancestor to these affected families or if it had independently arisen multiple times in human history.
The group tried to trace back the lineage of the SCN1Bc.363C>G variant in 14 families with these seizures. They also analyzed genome data from the UK Biobank, a large-scale and long running study of people’s health that also collects their genetic information.
Within the biobank, the researchers identified another 74 individuals with the same variant. And all of these people had similar patterns of other genetic variations surrounding the variant—a grouping of genes that’s known as a haplotype. It’s very unlikely that all of these people would have the same common haplotype without having some shared ancestry, the researchers say, meaning that the existence of this genetic disease today is probably due to just one ancestor, also known as a founder event. And as near as they can tell, this ancestor lived about 800 years ago.
“Here, we report evidence of a single founder event giving rise to the SCN1Bc.363C>GQ11variant in 14 independent families with epilepsy,” the authors wrote in their paper, published Tuesday in The American Journal of Human Genetics.
There are other genetic disorders or traits that can be cleanly traced back to a single founder event. But these disorders tend to appear later in life (after a person has already reproduced) or to be recessive, meaning that they only cause disease when someone inherits both copies of the bad variant. So it’s very unusual to see the same with a damaging dominant mutation that shows up in childhood. Often, these mutations are weeded out in a short time, since affected people would be less likely to survive into adulthood and pass on the mutation to the next generation—an example of natural selection.
This mutation, the authors speculate, might have endured because most people with it experience relatively mild seizures. Only about 70% of people with the mutation seem to become sick at all, something known as incomplete penetrance. In other words, this mutation might cause trouble, but not enough to have kept people who had it from living their lives and passing on their genes.
Aside from learning more about this disease, the authors say their findings could have broader implications. There may very well be other genetic mutations out there that similarly linger in the population at low levels but which might actually turn out to be more harmful than currently assumed.
“These findings suggest variants present in the population at low frequencies should be considered potentially pathogenic in mild phenotypes with incomplete penetrance and may be more important than previously thought,” they wrote.
Days after federal officials announced the largest fentanyl seizure in New York City history, an even greater quantity of the highly addictive substance has been found, authorities say.
Two people have been arrested and charged with multiple drug and firearm charges in connection to the seizure on October 7 at a Bronx apartment building, prosecutors said in a news release.
Authorities found roughly 300,000 rainbow-colored fentanyl pills inside two closets in the apartment, and more than 22 pounds of the drug in powdered form were wrapped in clear plastic packaging in multiple rooms, according to the Office of the Special Narcotics Prosecutor for the City of New York. The total sum of the drugs is worth about $9 million in street value, officials said.
The historic seizure saved lives, according to DEA Special Agent in Charge Frank Tarentino.
“Hundreds of thousands of lethal pills were lying in wait in a Bronx apartment to be unleashed onto our streets. In today’s world, the potential to overdose is dangerously high,” Tarentino said. “There is no quality control in these fake pills and it only takes two milligrams of fentanyl to be lethal.”
The seizure comes after federal officials announced last week that a woman has been charged with concealing about 15,000 rainbow-colored fentanyl pills in a Lego box as part of a drug trafficking scheme in September. That seizure at the time was also deemed the largest of fentanyl in New York City’s history.
Fentanyl is a synthetic opioid that’s highly addictive. It can be up to 50 times stronger than heroin and 100 times stronger than morphine, the US Centers for Disease Prevention and Control said.
Rainbow fentanyl comes in bright colors and can be used in pill form or powder.
“Rainbow fentanyl is the latest threat we face in our fight against the opioid epidemic that sadly continues to ravage our communities – a multi-colored poison specifically designed to attract younger users,” Nassau County District Attorney Anne T. Donnelly said.
And as Halloween nears, officials have been warning families to be especially vigilant regarding their children’s candy before they consume it.
The dangerous drug has been a major driver of fatal and nonfatal overdoses in the US as well as the opioid epidemic.
Although there has been a slight decrease in recent months in drug overdose deaths, the numbers remain high. About 108,000 people died of a drug overdose in the 12-month period ending May 2022 – which is down from the record high of more than 110,000 deaths reported in the 12-month period that ended March 2022, CDC provisional data published Wednesday shows.
The latest overdose death figure remains 32% than it was two years earlier and higher than any other period before November 2021, according to the CDC data. Synthetic opioids, including fentanyl, were involved in more than two-thirds of deaths in the 12-month period ending May 2022, and psychostimulants were involved in nearly a third.
Brandy is at an LA area hospital recovering from what is believed to be a possible seizure.
The singer and actress was at home when the medical emergency occurred, with an ambulance being called in at noon local time on Tuesday, October 11, according to TMZ.
She appears to be in recovery, per the outlet, with her parents with her at the hospital.
The latest: Brandy is at an LA area hospital recovering from what is believed to be a seizure; pictured on September 20, 2018 in Atlanta
The outlet noted that it is unknown if there were any other health issues that led to the medical emergency.
Brandy is currently still in the hospital, per TMZ.
Their insider believes the star suffered a seizure but it has not been confirmed.
Get well: She appears to be in recovery, per the outlet, with her parents with her at the hospital; seen on July 15, 2022 in LA
The health emergency occurred just days after her younger brother Ray J, 41, raised alarm over distressing content shared on his Instagram last week.
In the since-deleted posts, one video showed the star’s legs hanging over a ledge, while he asked if he should ‘just jump off.’ Despite the posts, a source informed TMZ Ray J had been drinking at the time and that he is now doing well.
The star uploaded a throwback of her and Ray J to her Instagram soon after from their childhood, ‘Need you bro.’
The two siblings have been known for their close bond and have supported each other throughout the years.
Earlier in July, Ray J shared a post that showed off a tattoo he got on his leg which depicted his sister.
When talking to TMZ about the decision to get the tattoo and responding to some of the initial backlash he received, the One Wish singer explained, ‘It’s my leg, it’s my sister.’
Support: Brandy uploaded a post on her Instagram sending her love and support to her younger brother Ray J, 41, earlier on Friday after he shared a post expressing suicidal thoughts
Close siblings: Throughout the years, the siblings have remained close and supported each other; pictured together earlier in June in Los Angeles
Although Brandy herself was, ‘a little uneasy about it,’ at first, he expressed that, ‘I love my sister and that was just a symbol of me saying thank you for putting me in. If it wasn’t for her, I wouldn’t be here. I’m humbled just to have her helping me.’
Due to their close relationship, Brandy quickly expressed her love to her younger brother following his concerning posts on Thursday.
‘If it wasn’t 4 my Kidz I would jump off and die tonight,’ he wrote over one video that showed his view from a high point.
A source told TMZ that he had been drinking when he posted the messages and his wife Princess Love eventually persuaded him to delete them.
Concerning: The rapper shared a series of posts and videos on his Instagram last week where he appeared to be contemplating his life
The TMZ insider further stated that Ray J — real name William Ray Norwood Jr. — was only ‘messing around’ on social media and did not require a trip to the hospital.
His original disquieting posts included a picture of his feet dangling over a drop, captioned: ‘SHOULD I JUST JUMP off and end it rit. Now!!! ????’
On his Instagram Stories, he wrote: ‘trying to figure it out – maybe this life was a illusion – – maybe the next life was my real reality.’
A source claimed he put up the posts while on a trip in Mexico with his wife and their children Melody, four, and Epik, two.
Message: On his Instagram Stories, he wrote: ‘trying to figure it out – maybe this life was a illusion – – maybe the next life was my real reality’
Potential cause: An insider informed TMZ that Ray J had been drinking at the time he had posted on Instagram and ‘did not require’ hospitalization
MOSCOW/HOUSTON, Oct 7 (Reuters) – Russian President Vladimir Putin signed a decree on Friday that establishes a new operator for the Exxon Mobil Corp-led (XOM.N) Sakhalin-1 oil and gas project in Russia’s Far East.
Putin’s move affecting Exxon’s largest investment in Russia mimics a strategy he used to seize control of other energy properties in the country.
The decree gives the Russian government authority to decide whether foreign shareholders can retain stakes in the project.
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Exxon holds a 30% operator stake in Sakhalin-1, with Russian company Rosneft (ROSN.MM), India’s ONGC Videsh (ONVI.NS) and Japan’s SODECO as partners.
Oil production at the Sakhalin-1 project fell to just 10,000 barrels per day (bpd) in July from 220,000 bpd before Russia invaded Ukraine.
NAVIGATING AN EXIT
Exxon has been trying to exit its Russia operations and transfer its role in Sakhalin-1 to a partner since March, after international sanctions imposed on Moscow.
Russia’s government and Exxon have clashed, with the oil producer threatening to take the case to international arbitration.
Exxon declined to comment on Friday’s decree.
Japan’s SODECO was not immediately available to comment, but an official of the industry ministry, which owns a 50% stake in the firm, said it was gathering information and talking with partners. Japan has stopped buying crude from Russia since June. read more
Exxon took an impairment charge of $4.6 billion in April for its Russian activities and said it was working with partners to transfer Sakhalin-1’s operation. It also reduced energy production and moved staff out of the country.
In August, Putin issued a decree that Exxon said made a secure and environmentally safe exit from Sakhalin-1 difficult. The U.S. producer then issued a “note of difference,” a legal step prior to arbitration.
Friday’s decree said the Russian government was establishing a Russian company, managed by Rosneft subsidiary Sakhalinmorneftegaz-shelf, that will own investors’ rights in Sakhalin-1.
Foreign partners will have one month after the new company is created to ask the Russian government for shares in the new entity, the decree said.
Putin used a similar strategy in a July decree to seize full control of Sakhalin-2, another gas and oil project in the Russian Far East, with Shell (SHEL.L) and Japanese companies Mitsui & Co (8031.T) and Mitsubishi Corp as partners.
Russia has approved applications by the two Japanese trading houses seeking to transfer their stakes to a new operator. read more
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Reporting by Reuters; Additional reporting by Yoshifumi Takemoto, Yuka Obayashi in Tokyo, Editing by Cynthia Osterman and Clarence Fernandez
Our Standards: The Thomson Reuters Trust Principles.
Summary: A1R-CT, a novel peptide that binds to neurabin, can be administered via a nasal spray and holds the potential to interrupt uncontrollable brain activity associated with TBI, stroke, epilepsy, and Alzheimer’s disease.
Source: Medical College of Georgia at Augusta University
A novel peptide augments the brain’s natural mechanism to help prevent seizures and protect neurons in research models of both Alzheimer’s and epilepsy, scientists report.
The A1R-CT peptide the scientists developed, which can be administered through a nasal spray, holds promise for tamping down the uncontrolled electrical activity that is common after traumatic brain injury, stroke and which affects more than half of individuals with Alzheimer’s, says Dr. Qin Wang, neuropharmacologist and founding director of the Program for Alzheimer’s Therapeutics Discovery at the Medical College of Georgia at Augusta University.
The fact that it can be delivered through the nose indicates the peptide’s potential as a new seizure rescue medication as well, to help interrupt, for example, a seizure cluster, where disabling seizures are occurring back-to- back, says Wang, corresponding author of the study in the journal JCI Insight.
A1R-CT works by inhibiting neurabin, a protein that helps ensure that the protective mechanism itself, which tamps down the hyperexcitability of neurons that disrupts normal communication and produces seizures, doesn’t overdo, she says.
The peptide was named after the protective adenosine 1 receptor on the surface of neurons, which gets activated by adenosine, a chemical made mostly in the brain by neuron-supporting glial cells in response to hyperexcitability.
“This is a powerful receptor to then silence the neurons,” Wang says. This natural, calming relationship also is known to block electrical activity that can result in an irregular heartbeat. In fact, an injectable form of adenosine is used to treat a very high heart rate.
“But the A1 receptor itself has to be regulated because if it’s activated too much, you will fall asleep,” says Wang. “The neurons try to make sure everything stays in control and in most of us, it works pretty well. We don’t fall asleep at our desk. We don’t have seizures,” she says, noting that caffeine blocks the A1 receptor.
Alzheimer’s often is accompanied by seizures because the characteristic buildup of the proteins amyloid and tau in the brain disrupts communication between neurons, creates increased oxidative stress and resulting inflammation, and in response to the altered dynamic, neurons can become hyperexcited, she says.
“In Alzheimer’s there are so many things that go wrong,” she says. Seizures can precede the cognitive decline in Alzheimer’s, and definitely contribute to it, Wang says.
A1 receptor’s activation by adenosine in this type of hyperactive scenario makes it seem like a logical treatment target for seizures. But the fact that it is so pervasive throughout the body, including in the heart, lungs and kidneys, makes potential extensive side effects likely.
Back to neurons’ desire for homeostasis, Wang and her colleagues were the ones who found that the protein neurabin, which appears to be primarily present in the brain, provides that balance to prevent hyperactivity of the A1 receptor.
The fact neurabin is primarily in the brain, means that altering its activity should not have the potential body-wide impact of directly altering A1 receptor activity, Wang says.
“Neurabin is a brake so it doesn’t do too much,” Wang says. “But now we need to remove it to unleash A1’s power.”
So, they set to work developing the peptide that could instead interfere with the A1 receptor and neurabin’s interaction and so enable more of the natural protective, seizure-reducing benefit.
A1 receptor activation tamps down the excited state of the neurons by modulating ion channels — proteins in the cell membrane that allow passage through the cell of other proteins — which help generate electrical signals.
A result is so-called hyperpolarization, which means the neuron is less likely to fire an electrical signal.
“The more polarized the neurons are, the harder it is for them to get excited,” Wang says.
A1 receptor activation also decreases the release of glutamate, a neurotransmitter produced by neurons that excites neurons. It also provides additional benefit to neurons by providing some protection from inadequate oxygen and blood supplies, which may occur in the case of an injury. The scientists have noted a dramatic reduction in death of neurons in their Alzheimer’s model, for example, with the use of their peptide.
Now they’ve shown that inhibiting neurabin — either by reducing it directly or with their peptide — enables increased action by A1C to reduce excessive electrical activity in the brain. They’ve shown the peptide is effective in both a mouse model of severe seizures and seizures in an Alzheimer’s mouse model. And It’s effective when directly injected into the brain or via nasal spray.
The scientists opted to look at nasal spray delivery to fully explore the peptide’s potential clinical benefit. They found a similar robust response in both the seizure and Alzheimer’s models.
Looking further at the impact of targeting neurabin, they found that mice with a neurabin deficiency had significantly shorter, less severe seizures and they all survived. Those with the normal neurabin levels intact experienced seizures lasting for up to 30 minutes and about 10% of the mice died shortly afterward.
A1R-CT works by inhibiting neurabin, a protein that helps ensure that the protective mechanism itself, which tamps down the hyperexcitability of neurons that disrupts normal communication and produces seizures, doesn’t overdo, she says. Image is in the public domain
Blocking A1 receptor resulted in more severe seizures in the neurabin-deficient mice and increased the death rate to more than 50%.
Next steps include additional exploration of ideal doses and delivery times for specific conditions the peptide may be used to treat.
The scientific team also continues to tweak the peptide to ensure it functions optimally, and is pursuing funding needed to pursue clinical trials.
Wang, a Georgia Research Alliance Eminent Scholar, came to MCG in April 2021 from the University of Alabama at Birmingham, where she began the studies of A1 receptor and peptide development. She continues extensive collaboration with her colleagues at UAB on the studies who are coauthors on the new paper. First author Dr. Shalini Saggu is now also a faculty member in the MCG Department of Neuroscience and Regenerative Medicine.
Epileptic seizures are common after a traumatic brain injury; a stroke, which is considered an acquired brain injury; and with chronic neurodegenerative diseases including Alzheimer’s.
See also
As much as 64% of the some 50 million individuals with Alzheimer’s experience seizures, the scientists write. Patients can experience generalized tonic-clonic seizures, in which they fall down, shake and become unresponsive. Also, focal onset seizure, which tend to be shorter and may include repetitive movement of the arms or legs, lip smacking and chewing.
Seizures are uncontrolled in about 40% of people, which indicates an urgent need for novel therapies, the scientists write, and current therapies tend to be less effective in individuals with Alzheimer’s. Left uncontrolled, seizures can produce brain damage and cognitive impairment.
Adenosine also is a building block of our DNA and a component of the cell fuel ATP.
Funding: The research was supported by the National Institutes of Health.
About this neuropharmacology research news
Author: Toni Baker Source: Medical College of Georgia at Augusta University Contact: Toni Baker – Medical College of Georgia at Augusta University Image: The image is in the public domain
Original Research: Open access. “A peptide blocking the ADORA1-neurabin interaction is anticonvulsant and inhibits epilepsy in an Alzheimer’s model” by Qin Wang et al. JCI Insights
Abstract
A peptide blocking the ADORA1-neurabin interaction is anticonvulsant and inhibits epilepsy in an Alzheimer’s model
Epileptic seizures are common sequelae of stroke, acute brain injury, and chronic neurodegenerative diseases, including Alzheimer’s disease (AD), and cannot be effectively controlled in approximately 40% of patients, necessitating the development of novel therapeutic agents.
Activation of the A1 receptor (A1R) by endogenous adenosine is an intrinsic mechanism to self-terminate seizures and protect neurons from excitotoxicity. However, targeting A1R for neurological disorders has been hindered by side effects associated with its broad expression outside the nervous system.
Here we aim to target the neural-specific A1R/neurabin/regulator of G protein signaling 4 (A1R/neurabin/RGS4) complex that dictates A1R signaling strength and response outcome in the brain. We developed a peptide that blocks the A1R-neurabin interaction to enhance A1R activity. Intracerebroventricular or i.n. administration of this peptide shows marked protection against kainate-induced seizures and neuronal death.
Furthermore, in an AD mouse model with spontaneous seizures, nasal delivery of this blocking peptide reduces epileptic spike frequency. Significantly, the anticonvulsant and neuroprotective effects of this peptide are achieved through enhanced A1R function in response to endogenous adenosine in the brain, thus, avoiding side effects associated with A1R activation in peripheral tissues and organs.
Our study informs potentially new anti-seizure therapy applicable to epilepsy and other neurological illness with comorbid seizures.
ENGLEWOOD, Colo. — Former Denver Broncos wide receiver Demaryius Thomas died from “complications of a seizure disorder,” according to an autopsy report from the Fulton County (Ga.) Medical Examiner’s office.
Portions of the report were shared with ESPN on Friday. Thomas was found dead in his Roswell, Georgia, home on Dec. 9 at age 33, and an autopsy was performed the following day.
In December, the medical examiner’s office released a statement that “the cause and manner of death are pending the completion of laboratory studies and microscopic tissue samples.” In the final report, the medical examiner said the manner of Thomas’ death remains undetermined and it was unknown if the seizure disorder was the result of natural causes or due to impacts to Thomas’ head during his NFL career.
Last month, researchers at Boston University told ABC News that Thomas had suffered from chronic traumatic encephalopathy (CTE), a degenerative brain disease, but said that CTE had not caused his death. The autopsy report said those same researchers said they did not believe Thomas’ CTE caused the seizure disorder.
The autopsy report revealed that Thomas, who was found dead in the shower, had traces of nicotine and marijuana in his system, but neither was listed as a contributing factor in his death.
At the time of his death, some of Thomas’ family members said publicly he had suffered seizures for about a year before he died. Several former teammates also said at the time that Thomas had told them he had suffered seizures in recent months.
Thomas’ trademark smile and ever-present desire to help those in need made him one of the franchise’s most popular players in the community. His death sent shock waves through the NFL and Denver.
Thomas, who would have turned 34 on Christmas, had announced his retirement from the NFL in June 2021 with a short video in which he flashed a peace sign and a smile.
Thomas was the first of two first-round picks for the Broncos in the 2010 NFL draft — Tim Tebow was the other — and spent nine seasons with the team. He finished his career as the Broncos’ second-leading receiver (9,055 yards), behind Rod Smith. He is third in franchise history in catches (655) behind Smith and Hall of Famer Shannon Sharpe.
Thomas played in 10 seasons overall with the Broncos, Houston Texans and New York Jets and finished with 724 catches for 9,763 yards and 63 touchdowns.
A ‘Geodesic Sensor Net,’ used to obtain a highly detailed EEG reading. Photo: Oli Scarff (Getty Images)
Seemingly for the first time ever, doctors have gotten a detailed look at the brain of a person during their final moments of life. The findings were obtained from a hospital patient who suddenly died while having his brain monitored for seizures, and they may offer some support for the idea that people see their lives flashing before their eyes when near death.
The research was published Tuesday in the journal Frontiers in Aging Neuroscience. According to the report, the patient was an 87-year-old man who had been admitted to the hospital after a serious fall that left him with bleeding in his brain. Following an operation to treat the injury, the man briefly stabilized for two days before appearing to develop seizures. He was then given an electroencephalography (EEG), which measures the brain’s electrical activity. The EEG did confirm his ongoing seizures, but midway through, the man’s heart stopped beating and he went into cardiac arrest. In accordance with his family’s wishes and the patient’s Do-Not-Resuscitate status, the doctors did not attempt any further treatment and the man soon passed away. Because the EEG machine kept running through the man’s last minutes of life, though, the doctors had a unique set of data on their hands.
There have been numerous attempts to study what happens to our bodies and minds as we’re dying. But much of this research, for understandable reasons, has involved extrapolating what we see in controlled animal studies over to humans. Some studies have been able to track the vital signs or simple brain activity of people as they’re taken off life support or dying, which have provided some interesting insights. But this appears to be the first time that a person’s dying brain has been studied in this much detail using EEG.
The most tantalizing result, the authors say, is evidence that there may be something real to the stereotypical portrayal of a near-death experience. Right before and after the man’s heart stopped beating, for instance, there was an increase in gamma brain waves, which are associated with learning and memory. And the patterns of brain activity, including gamma, that the team documented in the man as he died resembled the patterns seen in people who are dreaming or recalling memories. “Such activity,” they wrote, “could support a last ‘recall of life’ that may take place in the near-death state.”
Of course, these findings are based on a single person’s brain readings. The man also suffered a traumatic brain injury and swelling, developed seizures, and was on anticonvulsants prior to his death, all of which could have made his brain activity different from the average person experiencing death. But the authors also note that much of what they found lines up with what’s been seen in lab studies of dying rats, lending some support that their research could be generalizable.
The authors do plan to look for similar cases, and they hope that further work can better shine a light on how we die, and whether we’re likely to see our lives play back for us before the end.
“Something we may learn from this research is that, although our loved ones have their eyes closed and are ready to leave us to rest, their brains may be replaying some of the nicest moments they experienced in their lives,” study author Ajmal Zemmar, a neurosurgeon at the University of Louisville, told Frontier Science News.
MIAMI (AP) — A cruise ship that was supposed to dock in Miami sailed to the Bahamas instead after a U.S. judge granted an order to seize the vessel as part of a lawsuit over unpaid fuel.
Cruise trackers show Crystal Symphony currently docked in the Bahamian island of Bimini.
Passengers told news outlets that they’ll be taken by ferry to a South Florida port Sunday. It was unclear how many passengers were aboard, with one news outlet reporting 300 and another, 700. According to the company website, the vessel can carry up to 848 passengers.
The ship was scheduled to land in Miami on Saturday. But a federal judge in Miami issued an arrest warrant for the ship on Thursday, a maritime practice where a U.S. Marshal goes aboard the vessel and takes charge of it once it enters U.S. waters.
The lawsuit was filed in a Miami federal court by Peninsula Petroleum Far East against the ship under a maritime procedure that allows actions against vessels for unpaid debts. The complaint says Crystal Symphony was chartered or managed by Crystal Cruises and Star Cruises, which are both sued for breach of contract for owing $4.6 million in fuel.
Crystal Cruises announced earlier this week that it was suspending operations through late April. Besides Crystal Symphony, it has two other ships currently cruising, which end their voyages on Jan. 30 in Aruba and on Feb. 4 in Argentina.
“Suspending operations will provide Crystal’s management team with an opportunity to evaluate the current state of business and examine various options moving forward,” said the company in a statement earlier this week.
In a statement on its website, Gilead said “in coordination with the US Marshals and local law enforcement, Gilead has executed seizures at 17 locations in nine states, seizing thousands of bottles of Gilead-labeled medication with counterfeit supply chain documentation.”
Over the course of a two-year investigation, “evidence showed that the distributor defendants sold 85,247 bottles” of the counterfeit drugs, according to the statement.
The bottles were labeled Biktarvy and Descovy, two popular medicines to help treat HIV-1.
An ongoing investigation “revealed that pharmaceutical distributors not authorized by the company to sell Gilead medicine were selling drugs to pharmacies that they sourced from various fly-by-night entities as part of the illegal counterfeiting scheme.”
In August of 2021, Gilead warned of the counterfeits, issuing a consumer alert at the time.
In court documents, which were filed in U.S. District Court for the Eastern District of New York in July of 2021, Gilead asked that the court bar certain distributors from “selling any Gilead medication, whether genuine or counterfeit.” Additionally, it is asking that the defendants cease “falsely representing themselves as being connected with Gilead or sponsored by or associated with Gilead.”
The complaint, which was unsealed by a judge on Tuesday, alleged in one glaring example that “the tablets inside those bottles were not Gilead’s HIV medication. They were completely different drugs.”
An outside laboratory tested the medicines and allegedly found “the most common contents of the tested counterfeits was quetiapine furmarate, a non-Gilead… prescription anti-psychotic medication with a number of known serious side effects,” the complaint says.
Attempts by CNN to reach attorneys for the defendants were unsuccessful.
Gilead warned about the dangers of using counterfeit medicine. “Counterfeit and tampered medicines can result in serious and or life-threatening health risks,” it said, adding that “They are not equivalent in quality, safety, and/or efficacy to genuine medicines.”
“Patient safety is our first priority, and our actions were instrumental in removing counterfeit HIV medications from the U.S. supply chain and protecting individuals who rely on our medications,” Lori Mayall, head of anti-counterfeiting and brand protection at Gilead Sciences, said in a statement. “Based on our actions, we believe that we have successfully stopped these defendants from distributing additional counterfeit versions of Gilead medication to patients.”
