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Novel Opioid Offers Potent Pain Relief Without Classic Side Effects

Researchers have discovered a novel synthetic opioid that provided potent pain relief in preclinical models without many of the dangerous side effects that limit current opioid therapies.

The compound, N-desethyl-fluornitrazene (DFNZ), produced strong analgesia in rodents without causing respiratory depression, tolerance, or other indicators of potential addiction, reported the researchers, led by Michael Michaelides, PhD, with the National Institute on Drug Abuse (NIDA).

“Opioid pain medications are essential for medical purposes, but can lead to addiction and overdose. Developing a highly effective pain medication without these drawbacks would have enormous public health benefits,” NIDA Director Nora D. Volkow, MD, said in a news release.


A novel mu-opioid receptor agonist showed strong analgesia without respiratory depression, tolerance, or significant addiction signals in animal models.

Waves of gene control reveal how a key gene times limb development

In a new study published in Genes & Development, research led by Dr. Lila Allou at the MRC Laboratory of Medical Sciences (LMS) in London and Professor Stefan Mundlos at the Max Planck Institute for Molecular Genetics and Charité in Berlin demonstrates how different regulatory genetic elements coordinate the temporal activity of a key developmental gene. Their findings likely explain subtle differences seen in patients with congenital limb malformations, for which the underlying disease mechanisms often remain unknown.

Although every cell contains the same genes, not all genes are active at any given time. Gene regulation is a fundamental process that ensures only the necessary genes are expressed in each cell type. This is why, for example, neurons differ in structure and function from muscle cells. Precise fine-tuning of gene regulation is especially critical during development. Timed waves of transcriptional activity ensure that an embryo develops into a healthy organism with properly positioned and formed limbs, organs, and tissues. This process is driven by specialized genes and controlled by regulatory elements in the genome.

Attenuated Single Neuron and Network Hyperexcitability Following MicroRNA-134 Inhibition in Mice with Drug-Resistant Temporal Lobe Epilepsy

JNeurosci: Findings from Quintana-Sarti et al. help explain how targeting microRNA-134 in mice can reduce seizure activity and support the continued development of this novel RNA-based approach for the treatment of epilepsy.

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The multifactorial pathophysiology of acquired epilepsies lends itself to a multitargeting therapeutic approach. MicroRNAs (miRNA) are short noncoding RNAs that individually can negatively regulate dozens of protein-coding transcripts. Previously, we reported that central injection of antisense oligonucleotides targeting microRNA-134 (Ant-134) shortly after status epilepticus potently suppressed the development of recurrent spontaneous seizures in rodent models of temporal lobe epilepsy. The mechanism(s) of these antiseizure effects remain, however, incompletely understood. Here we show that intracerebroventricular microinjection of Ant-134 in male mice with preexisting epilepsy caused by intra-amygdala kainic acid-induced status epilepticus potently reduces the occurrence of spontaneous seizures.

Oxidative Stress and Neuroinflammation in Parkinson’s Disease: The Role of Dopamine Oxidation Products

Parkinson’s disease (PD) is a chronic neurodegenerative condition affecting more than 1% of people over 65 years old. It is characterized by the preferential degeneration of nigrostriatal dopaminergic neurons, which is responsible for the motor symptoms of PD patients. The pathogenesis of this multifactorial disorder is still elusive, hampering the discovery of therapeutic strategies able to suppress the disease’s progression. While redox alterations, mitochondrial dysfunctions, and neuroinflammation are clearly involved in PD pathology, how these processes lead to the preferential degeneration of dopaminergic neurons is still an unanswered question. In this context, the presence of dopamine itself within this neuronal population could represent a crucial determinant.

Scientists find evidence some Alzheimer’s symptoms may begin outside the brain

Researchers used a microscopic model of human nerves and muscles to show that Alzheimer’s disease directly damages peripheral nerves. This physical damage happens independently of cognitive decline and does not improve with standard medications for the illness.

Why discarded brain ‘noise’ matters: Overlooked networks may reshape mental health treatment

Scientists who use imaging to understand the brain’s complexity often focus on the strongest signals and ignore the rest. But this strategy, researchers warn, may reveal only the tip of the iceberg. A study published in Nature Human Behavior reveals that connections routinely overlooked as “noise” during neuroimaging data analysis can predict behavior with remarkable accuracy—and implicate entirely different brain networks. The finding could open many new targets for treating psychiatric illness, the researchers say.

“Many studies that rely on techniques like feature selection—which simplifies the brain down to a narrow slice—might only uncover a small part of the true neurobiology that underlies a given behavior,” says lead author Brendan Adkinson, Ph.D., an MD-Ph. D. student at Yale School of Medicine.

“Our study suggests that there may be multiple, non-overlapping networks capable of predicting a given behavior just as well.”

What does it Feel Like to be God? | John Polkinghorne

God is said to be all-powerful, all-knowing, all-good. But what is God’s private mental life like? Can we reach in to appreciate God as a supreme being? It may seem absurd, or arrogant, for finite human beings to strive to imagine what an infinite God is like and even what God may feel like privately and inside. But that is what we do.

John Charlton Polkinghorne KBE FRS was an English theoretical physicist, theologian, and Anglican priest.

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