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Interim FDG-PET analysis to identify patients with aggressive non-Hodgkin lymphoma who benefit from treatment intensification: a post-hoc analysis of…

The interim FDG-PET scans of the treatment intensification PETAL trial were re-analyzed in a comprehensive PET analysis to segment all lymphoma manifestations. The following principal findings arise from this analysis: (1) A fully automated analysis of interim FDG-PET/CTs from lymphoma patients is feasible. (2) The biomarkers derived from the comprehensive PET analysis are statistically significant prognosticators of TTP. (3) The mean-SUVAI parameter identified patients that benefitted from additional application of rituximab as treatment intensification, which could not be achieved using conventional PET metrics.

(R-)CHOP is the standard first-line treatment for patients with aggressive lymphoma, with cure rates of 6070%. In patients with (multiply) relapsed disease, several treatment options exist, such as high-dose chemotherapy with autologous hematopoietic stem cell transplantation, allogeneic transplantation, CAR-T cell therapy, immunomodulation, and others [15,16,17]. Current methods for early prediction of treatment failure, including Deauville-based iPET assessment, appear insufficient.

FDG-PET has a long track record of monitoring initial treatment response to systemic anti-cancer therapy [2, 3, 18]. In principle, early detection of treatment failure could trigger a change in therapy, aiming at improved outcome. However, often only a single target lesion is used to assess treatment failure and guide subsequent therapies. A single lesion, however, cannot accurately capture disease extent and severity. To overcome this limitation, a recent approach tries to employ ctDNA levels as comprehensive biomarker to assess the total lymphoma burden [19]. However, in FDG-PET is comprehensively analyzed, it can also quantify the total lymphoma burden and assess the metabolic heterogeneity of all manifestations. As the delineation of all disease manifestations is too time-consuming for clinical routine, AI-based PET analysis software, like the PARS prototype and others, have been proposed [12, 20].

For the conventional metric max-SUVmanual, which takes account of a single lymphoma manifestation, no statistically significant interaction of treatment intensification by additional rituximab was found in the present analysis. In contrast, for the mean-SUVAI metric, which averages the FDG uptake of all lymphoma manifestations, a statistically significant interaction with treatment intensification was observed. This indicates that the benefit of treatment intensification through additional rituximab is growing with increasing mean-SUVAI. This was corroborated by looking at patients with high mean-SUVAI who had statistically significantly longer survival when treated with two additional rituximab doses than with 6xR-CHOP alone. Interestingly, patients with high mean-SUVAI had higher baseline SUVmax compared to patients with low mean-SUVAI (Supplementary Table5). This indicates that patients with high mean-SUVAI might erroneously be read as iPET-negative due to their high baseline SUVmax, which could lead to a more pronounced relative reduction, despite metabolically active residual lymphoma at the interim timepoint. The finding is in line with recent studies indicating that a more complex PET analysis of lymphoma patients is superior to the IPI index [21].

In patients randomized to 8x(R-)CHOP versus 2x(R-)CHOP followed by the Burkitt protocol, no statistically significant interaction of a PET parameter and treatment intensification was found. However, patients with high mean-SUVAI had statistically significantly longer TTP when they were not treated with the Burkitt protocol. This seems paradoxical as especially patients with very high residual tumor activity seemed to have a disadvantage from therapy intensification. Also, conventional PET metrics such as highest uptake or change in highest uptake between baseline and interim could identify patients who were disadvantaged by the Burkitt protocol; highlighting the need for comprehensive PET analysis. The data, however, need to be interpreted with caution because of imbalances in baseline characteristics (Supplementary Table1).

Our study has several limitations. First, it was a retrospective re-analysis of the prospective PETAL trial. The present analysis was not pre-planned, which might cause an observational bias. Additionally, all patients receiving 6xR-CHOP and 6xR-CHOP+2R were included, but only a subfraction was truly randomized (178 of 397 patients). However, non-randomized patients receiving 6xR-CHOP or 6xR-CHOP+2R were recruited using the same inclusion criteria in the beginning and at the end of the study period, respectively, which should minimize potential biases. Finally, our primary endpoint was TTP which best reflects the impact of therapy on outcome [7,8,9]. In contrast, the PETAL trial employed event-free survival (EFS), which also included death unrelated to lymphoma and events such as treatment-related toxicity.

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Interim FDG-PET analysis to identify patients with aggressive non-Hodgkin lymphoma who benefit from treatment intensification: a post-hoc analysis of...

Five Simple Tips To Keep Your Pets Safe This Halloween – Minnesota’s New Country

Halloween is so much fun for us..but honestly, it's probably pretty horrifying for our pets who don't understand a thing about our scary celebrations. I spoke with Dr. Nancy at Companions Animal Hospital and Vicki Davis from the Tri-County Humane Society, and they gave me some great tips I've kept in mind over the years. I hope these are helpful to you as well.

If you are going to have pumpkins with candles inside, or other lit decorations that cats could knock off a countertop, be watchful. We want you and your pets to have a safe and happy Halloween.

BE CAREFUL WITH COSTUMES

Don't put your dog or cat in a costume if they really hate it. Make sure it's not pinching them, and that they can see, walk and move comfortably. Your pet may look super cute in it, but if they are dancing around and trying to get out of it, don't torcher them.

Photo by Meyer Zinn on Unsplash

You know pets. If there is something they aren't supposed to get into, they'll find a way to get into it. Those treats for example. Unfortunately, many Halloween treats are toxic for your pets. Chocolate can be very dangerous for your cats and dogs, and sugar-free candies and fake sugar sweeteners are also very dangerous.

Does your dog bark, jump, and run every time the doorbell rings? Just think about the number of times it might happen on Halloween. If your pet gets stressed or is super protective, it might be a good night to give them a great chew toy, their favorite blanket, and a room with the tv or radio on, and the door shut.

Photo by Justin Jason on Unsplash

Glow sticks are important when your kids are trick or treating in the dark. Just make sure that if kids come to your home drop them in your yard, and that you pick them up before your pets find them. If your kids are using glow sticks, make sure to collect them once they get home.

To prepare yourself for a potential incident, always keep your vet's phone number handy, along with an after-hours clinic you can call in an emergency. The ASPCA Animal Poison Control Center also has a hotline you can call at (888) 426-4435 for advice.

Even with all of these resources, however, the best cure for food poisoning is preventing it in the first place. To give you an idea of what human foods can be dangerous, Stacker has put together a slideshow of 30 common foods to avoid. Take a look to see if there are any that surprise you.

KEEP READING: Here are 6 foods from your cookout that could harm your dog

Why do they meow? Why do they nap so much? Why do they have whiskers? Cats, and their undeniably adorable babies known as kittens, are mysterious creatures. Their larger relatives, after all, are some of the most mystical and lethal animals on the planet. Many questions related to domestic felines, however, have perfectly logical answers. Heres a look at some of the most common questions related to kittens and cats, and the answers cat lovers are looking for.

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Five Simple Tips To Keep Your Pets Safe This Halloween - Minnesota's New Country

Owner Saying Goodbye to Labrador Leaves Internet in Tears: ‘Have To Go Now’ – Newsweek

A tear-jerking video of a cancer-stricken Labrador's final moments has left the internet in tears.

More than two million people have watched the viral video posted by owner @tailsofjoyco, who has owned Lily for seven years before she was diagnosed with lymphoma, one of the most common types of cancer diagnosed in dogs.

The final stages of Lily's life were filmed, involving snacks, cuddles, and lots of love before she was put to sleep.

The owner added the following text to the video, it said: "Mom: sorry baby girl but you have to go now. Thank you for everything, we're so grateful we had seven years with you. I love you forever and ever."

Canine lymphoma is similar to non-Hodgkin's lymphoma in people. It is so similar, in fact, that veterinarians and human doctors use almost the same chemotherapy protocols to treat lymphoma in their patients.

Scientifically speaking, lymphoma is a blanket term used by doctors to describe a group of cancers that stem from lymphocytes, a type of white blood cell that helps the immune system fight off infection.

They are highly concentrated in organs that play a role in the immune system, like the lymph nodes, the spleen, and bone marrow. While lymphoma can affect any organ in the body, these organs tend to be where most lymphoma cancers are found.

Dealing with the loss of a pet can be devastating as they essentially become a part of the family. Whether they pass away naturally or are put to sleep at the vets, it is always an upsetting time.

Purina, the pet food brand, has shared a few tips on how to cope with the loss of a pet.

Over 4,000 people have commented on the video to send their condolences.

One user wrote: "I'm so sorry!! I feel ur pain!! Don't worry!! She's resting in peace and watching you! Swindling loves and hugs!"

"I'm crying so hard thinking of the day my sweet girl will have to go. I'm so sorry," wrote another.

Another TikToker said: "So sorry for your loss, labradors are the best friends you could ever ask for. Never cried over a dog I didn't know before. Fly high beautiful pup."

Newsweek reached out to @tailsofjoyco for comment. We could not verify the details of the case.

Do you have adorable videos or pictures of your pet you want to share? Send them to life@newsweek.com with some details about your best friend and they could appear in our Pet of the Week lineup.

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Owner Saying Goodbye to Labrador Leaves Internet in Tears: 'Have To Go Now' - Newsweek

Nikon Small World microscopy contest 2022: Meet this years top 10 winners – Ars Technica

Enlarge / This arresting image of the hand of an embryonic Madagascar giant day gecko took first place in the annual competition.

The Madagascar giant day gecko (Phelsuma grandis) is a popular exotic pet, perhaps because it looks a bit like Geico's beloved animated gecko mascot. Adults measure about 10 inches in length and are known for their bright green body color, augmented by a red stripe running from the nostril to the eye. They can lick their eyeballs (a way to keep them clean since the creatures lack eyelids). And, of course, they sport those well-known adhesive pads on their feet and handsideal for clinging to smooth vertical surfacesthat physicists find so fascinating.

Now we have a unique perspective on the gecko's most famous appendage: a striking photomicroscopy image of an embryonic hand ofPhelsuma grandis, courtesy of a Swiss graduate student, Grigorii Timin, at the University of Geneva and his adviser, Michael Milinkovitch. It's the winning image in the 2022 Nikon Small World Photomicrography Competition, designed to highlight "stunning imagery from scientists, artists, and photomicrographers of all experiences and backgrounds from across the globe," according to Nikon's communications manager, Eric Flem.

The first step in creating the winning image was to prepare the sample using whole-mount fluorescent staining of the tissue. And an embryonic gecko hand is actually quite a large sample (about 3 mm or 0.12 inches long) when it comes to high-resolution microscopy. So Timin painstakingly merged hundreds of images300 tiles, each containing some 250 optical sectionstogether using image-stitching to create the final result. Those cyan sections highlight the nerves in the embryonic hand, while other colors highlight bones, tendons, ligaments, skin, and blood cells.

Here are the remaining top 10 winners of this year's contest. You can check out the full list of winners, as well as several honorable mentions, here89 in all, selected from thousands of submissions around the world.

Caleb Dawson

Satu Paavonsalo & Sinem Karaman

Andrew Posselt

Alison Pollack

Ole Bielfeldt

Jianqun Gao & Glenda Halliday

Nathanal Prunet

Marek Sutkowski

Murat ztrk

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Nikon Small World microscopy contest 2022: Meet this years top 10 winners - Ars Technica

The Association Between Alzheimer’s Disease and Epilepsy: A Narrative Review – Cureus

Alzheimers disease (AD) is a progressive neurodegenerative disease typified by loss of memory, language, behavior, and personality [1]. Globally, around 55 million people have dementia, with AD contributing to about 60-70% of the total. As the percentage of older people in the population is on the rise in nearly every nation, this number is expected to grow to 78 million in 2030 and 139 million in 2050 [2]. It is important to note that dementia is now the seventh leading cause of mortality worldwide and the one with the highest economic burden [3].It is now increasingly apparent that undiagnosed and unprovoked seizures exist in a fair number of patients with AD and are eight to 10 times greater in patients with AD compared to the general population [4-7]. Reciprocally, those diagnosed with epilepsy have a 1.6 times higher risk than those without epilepsy of incident AD [8]. A study on the rat hippocampus has shown that epilepsy can increase the production of A-beta 40 amyloid protein [9]. Some studies suggest seizures can cause a decline in cognition in patients with AD [5]. This is supported by the Presentation of Epileptic Seizuresin Dementia (PrESIDe) study, in which initially, patients with and without a suspicion of epilepsy performed similarly on cognitive tests. Still, at a 12-month follow-up, the patients suspected of epilepsy performed much worse on cognitive tests. The rates of unprovoked seizures were significantly elevated in younger individuals with the autosomal dominant form, in African Americans, in severe forms of the disease, and individuals with focal epileptiform findings on electroencephalogram (EEG) [10]. Moreover, subclinical epileptiform activity (epileptiform activity without seizures) predominantly localized to the temporal lobe was found in about 42% of the patients with AD that received extended neurophysiological monitoring [5]. It is worth noting that these subsets of patients also had an accelerated decline in cognition and executive function [5]. Therefore, screening patients for epileptiform activity is recommended to improve diagnosis and outcomes as only 10-22% of patients with AD have clinically detectable seizures [11]. This is in accordance with another study that showed most seizures in AD to be non-motor and, therefore, easily missed [12]. The true prevalence of it is difficult to estimate as fluctuation in cognition could be the only presentation of seizures which is more difficult to decipher in the AD setting, which independently causes cognitive dysfunction. The importance of identifying seizures in patients with AD is of therapeutic significance as anti-epileptic medication has shown to improve memory functions in patients with mild cognitive impairment (MCI) [13]. The focus of this review is to understand the association between AD and epilepsy, briefly explore the pathophysiological and molecular mechanisms underlying it as these are vital in developing treatment strategies, discuss various diagnosing modalities and summarise the current treatment strategies for epilepsy in patients with AD.

The Global Deterioration Scale developed by Dr Barry Reisberg has seven stages and is depicted in Figure 1. The criteria for epilepsy as per the International league against epilepsyis seen summarized in Table 1.

The pathophysiology linking AD and epilepsy is complex and not fully understood. The following factors have been described in the literature:

Beta-Amyloid

Twenty-five percent of people who develop epilepsy in late adulthood have no known cause and are diagnosed with late-onset epilepsy of unknown etiology (LOEU) [14]. People with LOEU have been shown to have amyloid pathology in the brain, with amyloid- (A) deposition increasing their risk of developing cognitive decline over the decades [14]. Histopathological hallmarks of AD are intracellular neurofibrillary tangles (NFTs) and extracellular formation of senile plaques composed of the A peptide. Radioactive metal ions, for example copper, can catalyze the production of reactive oxygen species (ROS) when bound to A[15]. The ROS thus produced, in particular the hydroxyl radical, is the most reactive and may contribute to oxidative damage on both the A peptide and the surrounding molecules (proteins, lipids, neurons) [15]. A is pro-epileptogenic at the oligomer stage, well before plaque deposition, and its accumulation fosters network hyperexcitability [14]. While low concentrations of A facilitate the synaptic transmission, higher concentrations reduce synaptic activity. It is likely that in AD, a steady and small increase of A prompts neuronal hyperexcitability. At higher levels of A, synaptic dysfunction and inhibition occur, which becomes clinically apparent as cognitive impairment [16].Epileptic discharges and seizures during prodromal stages of AD can be set off by A oligomers and increase dynamically with A deposition, supporting the speculation that A-related epileptogenesis sets the stage for resulting neurodegeneration [14]. These discoveries appear to convert into clinical experience, with seizures happening now and again in patients with prodromal AD [14,16]. Thus A is at the interface of epileptogenesis and neuronal loss. A also has epileptogenic potential in the early stages of the amyloid cascade. Preclinical studies have demonstrated that A oligomers can induce spontaneous epileptiform discharges and clinically overt seizures. The epileptogenic potential of oligomers can depend on oligomerization status, threshold concentrations, and interaction with other proteins [17,18]. Production of A species is activity-dependent and consistently increases with neuronal firing [18]. Epileptiform activity favors plaque deposition and A plaque deposition, in turn, alters neuronal signaling, maintains a dynamic environment in equilibrium with oligomers, and promotes epileptiform activity, creating a vicious cycle. The contribution of every single item to the vicious cycle is yet to be fully understood, given that experimental models do not satisfactorily replicate mild Alzheimer's disease stages. Dissection of each mechanism might aid the development of multitarget strategies [14]. Glycogen synthase kinase-3 (GSK-3) is a proline-rich serine/threonine kinase and is essential in the pathogenesis of AD as it acts as a bridge between amyloid and tau; amyloid activates GSK 3, which in turn phosphorylates tau [19]. Many studies have already suggested that Tau and Amyloid play a role in epileptogenesis, and it can be deduced that GSK 3 has a role in developing unprovoked seizures in AD [19]. mTOR A serine/threonine kinase, expressed in multiple cell types, generates A42, and its hyperactivation is reported in both temporal lobe epilepsy (TLE) and AD [20].

Tau Protein

Tau protein is located in axons, a microtubule-associated protein type II; the MAPT gene encodes it on chromosome 17q21 [16]. Physiologically Tau protein is involved in anterograde and retrograde transport in axons via dynein and kinesin respectively. Pathologically paired helical filaments are formed, which are insoluble, self-assembled tau protein structures. Tau protein undergoes two post-translational modifications: hyperphosphorylation and truncation [16]. The hyperphosphorylation and abnormal tau aggregation, combined with its decreased clearance form NFTs and exert neurotoxicity in AD [21]. Hyperphosphorylation further halts microtubule binding, causing altered cytoskeleton stability and eventually loss of axon transport. Tau protein has been implicated in the disturbance of neuronal synchronization and hyperexcitability; along these lines, it could be connected to epilepsy [22]. Tau protein has also been embroiled in abnormal fiber growth and neuronal migration with hippocampal granule layer cell scatterings. These components are linked with epilepsy advancement [16].

Ion Channels

Beta-secretase 1 (BACE1) acts on Ion channels and primarily works on the 2 and 4 subunits of voltage-gated sodium channels [16]. BACE1 cleaves the 2 subunit regulating its transcription and expression on the cell surface; BACE1 also cleaves the channel 4 subunit, which mediates the closure of the voltage-gated sodium channel and, when cleaved, leads to aberrant firing and seizure-like activity. BACE1 levels are elevated in AD [16]. BACE1 also acts on voltage-gated potassium channels, which are linked to benign familial neonatal convulsions when mutated [16].

Gamma Amino Butyric Acid (GABA)

A few trials in AD patients and mice have shown that the collection of misfolded A obstructs GABAergic interneuron action, causing impeded synaptic communication and loss of neural network activity, which ultimately leads to cognitive impairment [17]. A new report showed transcriptional downregulation of 1, 2, 3, 5, 1, 2, 3, , 2, 3and subunits of GABA A receptors andglutamate decarboxylase (GAD) chemical in the middle temporal gyrus (MTG) of post mortem brain samples from AD patients. These changes weaken the harmony among excitatory and inhibitory pathways that might cause cognitive impairment in AD [17]. Similarly, in biochemical examinations, the levels of GABA in the synapses were significantly lower in the CSF and the transient cortex of Alzheimer's patients, suggesting weakened synaptic action and neuronal transmission [17]. Soluble A-actuated hyperexcitability has been related in vitro with a diminished GABAergic inhibition. This fortifies the hypothesis that GABA is one of the intermediaries associated with the organization and cell changes that lead to neuronal hyperexcitability in AD [16].

Glutamate

The capacity of L-glutamate (L-Glu) and various essential amino acids to excite CNS neurons was first exhibited in 1959. Since then, L-Glu has been distinguished as the core transmitter mediating fast excitatory synaptic reactions in the vertebrate central nervous system (CNS). L-Glu distribution inside the CNS is broad [18]. The neuronal cell loss in AD is mainly limited to cell bodies and dendrites of glutamatergic neurons in layers III and IV of the neocortex; loss of glutamatergically innervated cortical and hippocampal neurons are additionally noticed [18]. Disturbance of glutamatergic signaling towards a proepileptic state in AD has been connected to A and Tau protein [16].

Role of Sleep

Interictal epileptiform discharges (IED) are significant intermittent electrophysiological events observed between seizures in patients with epilepsy. Based on a study by Vossel et al., the prevalence of IED detected with the help of routine scalp EEG in AD patients with seizures was about 30% [4]. Another study conducted by Diaz et al. has established that in epileptics and patients with IED, non-rapid eye movement (NREM) sleep is associated with a rise in focal and generalized epileptic discharges as opposed to awake state and rapid eye movement (REM) sleep [23]. This is further supported by other studies that have shown an increase in the epileptiform activity in AD patients with seizures during sleep EEG recordings [5,24]. But, it should also be noted that a normal EEG can be expected in 85% of epileptic patients with AD [25]. Therefore it can be concluded that the prevalence of epileptiform discharges is probably more than observed and also highlights the need for better biomarkers to detect seizures in AD. Further evidence suggests that most sleep-related subclinical epileptiform activity is present in many probable AD patients and recognition of the same would help improve diagnostics and patient outcomes [5,24].

Mutations

Fifty percent of patients with EOFAD have mutations either in presenilin 1 (PSEN1), presenilin 2 (PSEN 2), or amyloid precursor protein (APP) [26]. These mutations can cause increased amyloidogenic processing of APP and increased A aggregates [27]. Mutations in PSEN1 are a significant cause of familial AD, as substantiated by 50% of the cases studied in nearly 480 families [27]. Figure 2 depicts the pathogenesis of AD and epilepsy in a concise way.

The prevalence of AD is inconsistent between several studies and ranges from 0.5% to 64%[28,29]. A meta-analysis published in 2021 found a combined seizure prevalence among patients with pathologically verified AD at 16% and in autosomal dominant AD (ADAD) at 2.8% to 41.7% [30]. It also established an incidence of 4.2 to 31.5 per 1000 person-years among those clinically diagnosed with AD [30]. Eleven percent of patients with adult-onset seizures had AD (95%CI, 7-14), with younger patients having an increased risk of seizures [30]. These differences in prevalence could be due to differences in diagnosing criteria, different databases used for studies, and variable disease severity [24]. It would also be challenging to obtain reliable history in more advanced stages of the disease. Conversely, symptoms such as syncope and behavioral changes can be falsely labeled as seizures. Hayashida et al. have described a case report of a 71-year-oldAD patient who presented with symptoms ofabdominal pain, nausea, vomiting, diarrhea, and bloating and was diagnosed to have abdominal epilepsy [31]. This further highlights the various ways epilepsy can manifest itself in AD, making the diagnosis challenging.

There are common risk factors between AD and epilepsy as seen in Figure 3.

Identifying individuals with AD who are at an increased risk of developing seizures is pivotal in implementing strategies to slow down disease progression and improve outcomes. Filippov et al. proposed genotyping of the apolipoprotein E (APOE) allele in combination with EEG to identify early-onset AD [32]. This is further supported by a meta-analysis that showed that 15-45% of APOE4 carriers had developed AD [33]. The incidences of AD are higher inAPOE4/4 patients (25-45%) whofall into the age group of 75-80 years compared with APOE3/4 carriers (15-25%) when matched for age [34].Recent studies in AD patients and animal models have established the role of blood-brain barrier (BBB) dysfunction in AD pathogenesis. Despite many studies, much remains to be found in our understanding of the BBB. These studies will be of immense value in detecting a potential risk factor for AD and as an important therapeutic modality. A study by Sweeney et al. suggests using in vitro human BBB models using pluripotent stem cells with neurodegenerative conditions to study this in greater detail [35]. Montagne et al. studied the permeability of the BBB using advanced dynamic contrast-enhanced magnetic resonance imaging (DCE-MI) showed age-dependent damage to the BBB in the hippocampus, the part responsible for memory, cognition, and learning [36]. Sleep disorders are also a risk factor for epilepsy as shown by a study conducted by Diaz et al. in which epilepsy was more prevalent in patients with insomnia or hypersomnia [23].

A 10-year cohort study by Lyou et al. showed that male sex, hypertension, hyperlipidemia, diabetes, and chronic kidney disease contributed to an increased risk of epilepsy [37]. It is crucial to note that this study was limited since it did not consider the influence of the environment, EEG findings, and the role of drugs. Literature shows that patients with Down syndrome (DS) have early onset of AD and seizures as the location of APP is on chromosome 21, and DS occurs due to a trisomy in chromosome 21 [38]. Antipsychotic drugs have been found to increase the risk of epileptic seizures. Second-generation antipsychotics, especially clozapine carry a higher risk than the first-generation antipsychotics [39]. Seizures occur in one to five of every 10 people who have had a traumatic brain injury (TBI), depending on the location of injury in the brain [40]. As noted before, age is a significant risk factor for AD [41]. Young age at the onset of AD, in both the sporadic and familial forms, was a risk factor and predictor for seizures and is perhaps one of the most consistent risk factors for AD [10]. A retrospective cohort study found that the black race, TBI, stroke, and pre-existing co-morbid depression were all critical risk factors for epilepsy in patients with AD [42]. This furthers the idea that the depression associated with AD could be due to degeneration of neurons and could point to a much more widespread insult to the brain, thus indicating a grimmer prognosis [43]. Smoking is said to be independently associated with both AD and epilepsy. In this case, epilepsy is believed to account for impaired neuron functioning and atherosclerotic changes in the brain's vasculature. However, a retrospective study found that these ischemic changes did not vary significantly among epileptic and non-epileptic subgroups [44]. Higher education is also believed to be a risk factor for seizures in AD, according to a study conducted by Horvath et al. [44].

AD can be classified as sporadic or familial and the semiology varies depending on the form of AD. The most common type of seizure in sporadic AD, accounting for about 55-70%, is the focal epileptic seizure that presents with an altered state of consciousness but with no motor component [4,10,41]. Other symptoms like dj vu or jamais vu and staring episodes are also common and are wrongly interpreted as cognitive fluctuations [4]. In familial ADAD, motor symptoms are more frequently seen asfocal or tonic-clonic, or myoclonic seizures [30,42,43].

Diagnostic challenges include identifying the best biomarkers for measuring sub-clinical epileptiform discharges and finding modalities for early detection.

Myelin Sheath Imaging

In their study, Drenthen et al. stated that reduced myelin content is commonly associated with epilepsy and other neurodegenerative conditions such as AD. Myelin sheath studies include imaging methods such as magnetic resonance imaging (MRI) and positron emission tomography (PET) scans and histopathological methods such as immunohistochemistry and Western blot. Thus, making it a potential candidate for a proper diagnostic procedure [45].

Scalp EEG

Many studies show that epileptiform activity is often undiagnosed in AD, and here EEGs are of great value especially when taken overnight during sleep. In astudy, Horvath et al. aimed to identify subclinical epileptiform activity (SEA) in patients with AD and its effect on the progression of the disease. They examined 52 Alzheimer patients and 20 healthy individuals. They found that SEA changes are associated more significantly and frequently in patients with AD and are accompanied by decreased cognitive ability and memory impairment. Thus, SEA may not present clinically and is present in only 50% of patients with AD, but its association with rapid deterioration of the disease indicates the importance of its early detection by EEG [46].When monitored for a minimum duration of eight hours or by including sleep, the sensitivity was improved to 60-80% [12,24]. Serial EEGs are also helpful in diagnosis as opposed to standard 30 minutes EEG [12]. A study by Lam et al. included 24-hour ambulatory EEG monitoring of patients with AD and healthy elderly individuals. This study aimed to find how some EEG findings correlate to the clinical presentations of seizures in AD and concluded that left temporal hyperexcitability on EEG was seen in the early stages of AD, with clinical seizures more commonly associated with bitemporal lobe excitability [47].

CSF Biomarkers

A study conducted by Cretin et al. evaluated CSF findings of epileptic and nonepileptic Alzheimer patients and found no significant differences in the levels of neurodegenerative biomarkers and albumin. They also found a significant correlation between the presence of CSF amyloid proteins and epileptic patterns on EEG. However, the authors concluded that CSF analysis could not serve as a substitute biomarker since there can be other causative factors apart from an amyloid-centric pathology, thus making this diagnostic modality inferior to others [25].

Functional Magnetic Resonance Imaging (fMRI)

According to Dickerson et al., fMRIcan identify pathologies of AD and epilepsy in frontal, temporal, and parietal cortices and can also identify areas in the brain showing hypoactivation due to atrophy and compensatory hyperactivation. It helps identify large-scale functional abnormalities and minute neuronal dysfunction in the early stages of AD [48].

Magnetoencephalogram (MEG)

Kitchigina et al., in their study, stated that MEG could be very useful in the early detection of temporal lobe epilepsy and AD since it has the potential to detect changes occurring in the early stages of the disease. MEG can also see alterations in theta and gamma rhythms familiar to AD and epilepsy [49].

Foramen Ovale Electrodes

Lam et al., in their study, used foramen ovale electrodes to study electrical changes in two patients with AD and found hippocampal seizure activity and epileptiform spikes, which did not have any clinical presentation. Thus, this is a helpful modality in detecting occult hippocampal activity in the early stage of the disease [50].

Genetic Studies

Juzwik et al. stated that microRNAs are common genetic markers that are dysregulated in various neurodegenerative disorders, including AD and epilepsy, and thus can be used as a potential biomarker for their diagnosis [51].

PET Scan

A review by Cai et al. talks about the role of PET imaging in the detection of synaptic vesicle glycoprotein 2A (SV2A) to study many neuropsychiatric conditions, one of which is AD. It could potentially be a reliable biomarker due to synaptic abnormalities in all neuropsychiatric disorders [52]. 18F-labeled fluoro-2-deoxyglucose positron emission tomography (FDG-PET) is also believed to help localize epileptogenic foci, especially in patients with underlying AD or other neurodegenerative diseases, especially if surgical treatment is warranted [53]. Altered adenosine receptor expression, a feature of many neurological conditions, including AD, can also be detected using a PET scan [54].

Cognitive Testing

Cretin et al., in their study, stated that epilepsy occurring in sporadic AD could be associated withother symptoms such as amnesia and behavioral changes. This can be a factor that can lead to a misdiagnosis ifclinical cognitive assessment is used as the only diagnostic modality. Moreover, epilepsy is seen in various stages of sporadic AD, mild, moderate, and severe, thus rendering it nonspecific and necessitating other modalities such as brain imaging [55]. The diagnostic modalities are summarized in Table 2.

Managing epilepsy in patients with AD can be especially challenging as the disease itself is a risk factor for epilepsy [56] and the concerned population is more proneto drug interactions due to different pharmacokinetics and effects on the CNS [57,58]. Therefore, the objective of antiepileptic drugs (AEDs) treatment in this group takes into account several factors beyond adequate seizure control [58]. Patients without witnessed seizures but positive epileptiform activity should be treated based on clinician judgment for example if there is concern that it is causing impairment of cognition [4]. Slow titration and monotherapy with vigilant monitoring of side effects are general recommendations [56].

Consideration of AD Drugs in Seizures

It is important to consider that some of the medications for Alzheimers can lower the seizure threshold. While one study reports that memantine can lower seizure threshold [59], another study reports statistically significant benefits of using memantine to improve cognition in epileptic patients with a good safety profile and no noted adverse effects [60]. Out of all the adverse drug reactions noted on donepezil and rivastigmine, 8.4% and 6.4% respectively were accounted for by convulsions [61]. On the other hand, no increased frequency of seizures was noted in the randomized, double-blind, placebo-controlled study of donepezil [62]. Galantamine was deemed to be safe in epilepsy and aducanumab was approved in 2021 for AD but needs further research on this topic [63,64]. Typical antipsychotics and bupropion commonly used for depression and mood stabilization can also lower the seizure threshold in these patients [65]. AEDs remain the intervention of choice with an excellent response rate of 79%, defined as a 95% reduction in seizures or fewer than three seizures annually [56,66]. Clinical judgment should be exercised for individual patients. No Empirical treatment with AED is indicated in patients without clinical or electrographic signs of network hyperexcitability but can be started if concerned that it is causing cognitive impairment [59]. In symptomatic AD patients, the risk of recurrence after the first unprovoked seizure stands at 70% and it is recommended to treat them indefinitely [67].

Pharmacological Interventions

Levetiracetam: A comparatively well-studied AED with proven efficacy and a good safety profile in AD. It can be used for both generalized and focal seizures and has fewer drug interactions [56]. One parallel randomised controlled trial (RCT) comparing lamotrigine (LTG), levetirecetam (LEV), and phenobarbital (PB) reported that around 71% (27 out of 38 people) of patients were responders on LEV monotherapy, with doses ranging from 500 mg to 2000 mg followed for a year after a month of dose adjustment [68]. Another prospective open-label study investigated 25 patients with advanced AD and noted a similar response rate of 72% with doses of 1000-1500mg and followed the patient for a year after giving a four week period for adjustment, while 16% discontinued due to issues with tolerability [69]. LEV was also noted to have an improvement in cognition, spatial memory, and executive function in AD with epileptiform activity. It also showed improved scores on mini-mental state examination (MMSE) and Alzheimer's Disease Assessment Scale-Cognitive Subscale (ADAS-cog) [59,69,70]. The medication was also well tolerated with no participant discontinuing treatment due to adverse effect [13]. Low doses of 125 mg twice a day was shown to improve hippocampal-basedmemory performance [13]. Levetiracetam also does not affect cytochrome p450 function and is exclusively renally excreted, hence accounting for fewer drug interactions [71] though, it is well established that LEV is noted for behavioral side effects, including irritation, agitation and even depression [72].

Lamotrigine: Another excellent option with a good safety profile and efficacy similar to LEV is lamotrigine with a response rate of 59% in a parallel RCT by Cumbo et al. [12,57]. It was also shown to improve cognition, mood, and performance on recognition and naming tasks as seen in a study by Tekin et al. after eight weeks of a trial of 300 mg of lamotrigine [73].

Gabapentin (GBP): Rowan et al. noted that 1500 mg per day of gabapentin had comparable efficacy with LTG 150 mg per day in older adults with a mean age of 72 years with mild cognitive impairment in a double-blinded RCT with 593 participants. While this is not specific to AD, it is a potential option [74]. Participants were followed for 12 months and remained seizure-free. GBP use in advanced AD remains questionable. Notable side effects include drowsiness and weight gain [75]. Hommet et al. reported similar findings though tolerance was better than LTG [75].

Carbamazepine (CBZ): Double-blinded RCT showed comparable efficacy of LTG, GBP, and carbamazepine at 600 mg per day but the tolerability was lowest [75]. CBZ, also being an enzyme inducer, was noted to be associated with osteomalacia, hence vitamin D, calcium, and physical therapy should be co-administered. Other side effects include cardiac dysfunction and low sodium [59].

Phenobarbital: It was seen to have an effective response of around 64 % similar to lamotrigine and levetiracetam in a randomized case-control study with a dose of 50-100 mg per day followed for a 12-month period. The major side effect was somnolence in nearly one-third of the patients. Cognitive outcome was poorer when compared to levetiracetam and lamotrigine. Studies suggest against its use for the abovementioned side effects but also due to increased risk of osteomalacia, ataxia leading to greater risk of fractures [59].

Valproate: It was associated with significant side effects including increased cortical volume loss, worsened MMSE and cognition, tremor, and gait disturbance compared to placebo in patients with AD which provide cases for not using it as your drug of choice [76,77].

Phenytoin: The efficacy of phenytoin remains controversial and variable with a lack of RCTs, and significant side effects including cognitive decline, ataxia, and sedation which are severe concerns in existing Alzheimer's [67,72]. Phenytoin was seen to increase seizure risk in mouse models [78].

Benzodiazepines: While highly efficacious in terminating seizures, they are well known to cause cognitive decline, delirium, and withdrawal seizures [79,80]. They also have significant addictive potential and hence should be only used as a last resort. Interestingly, long-term use has also been linked to the development of AD with one study reporting an odds ratio of 1.51 [81]. Other AEDs including oxcarbazepine and lacosamide have been used to treat seizures, but insufficient data is available for their efficacy in Alzheimers.

Levetiracetam (LEV) and lamotrigine have currently been shown to be the most effective treatment for seizures in patients with AD with levetiracetam also showing positive effects on cognition and lamotrigine helps stabilize mood [57,61,72,73]. Phenytoin and phenobarbital are not recommended for epilepsy in AD due to negative cognitive effects. The response to treatment is, however, good as can be seen summarized in Table 3.

Non-pharmacological Interventions

Non-pharmacological interventions, such as transcranial magnetic stimulation (TMS), deep brain stimulation, chiropractic care, Reiki, and acupuncture, have been shown to improve outcomes in people with AD or epilepsy [54-56].Stem cell therapyhas shown independent benefit in cases of both epilepsy and AD in rodent model studies and thus could potentially be explored as a future modality [82].

AD and epilepsy have a complex association and although a lot of studies have established an association, the mechanisms underlying the same are still not fully understood. In this review, we have discussed the existing literature with respect to epidemiology, risk factors, possible mechanisms, diagnosis, and treatment. We have only briefly discussed the latest clinical trials without going into the details of the mechanisms of individual AEDs. We have also not discussed upcoming treatment options such as anti-amyloid treatment, GSK3 inhibitors, and Tau inhibitors due to insufficient evidence on their efficacies. At present, it is difficult to give recommendations on treatment strategies in AD patients with epilepsy as there are insufficient trials and data is still evolving.

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The Association Between Alzheimer's Disease and Epilepsy: A Narrative Review - Cureus

Animal Control Says Dog Dumping On The Rise Here In South Jersey – catcountry1073.com

My heart can't help but break for all the animals here in South Jersey that don't have a warm and cozy home to call their own.

That's why it's so sad to hear about all the abandoned pets we have in this part of the Garden State. Most recently, the folks at Shore Animal Control based in Seaville, Cape May County, have shared that dog dumping has become more and more common in this region over the last few years. How can anyone's ears, or heart for that matter, bear that?

As unfortunate as that is to hear, that's what they shared in a recent Facebook post. We know it to be true, though. For example, we shared the news just last week about a whole litter of kittens abandoned at the Funny Farm Rescue in Mays Landing. They're over capacity at the moment, by the way, so if you're here because you're unsure of where to surrender your animal(s), don't do it there.

With that being said, if you or anyone you know does need to surrender a pet, don't just leave it out in the wild to fend for itself. Once an animal is domesticated, it's cruel to expect them to just pick up and fend for themselves as if they've always done so. If worst comes to worst, reach out to rescues and shelters in your area, preferably no-kill shelters, that have room and are willing to take in your pet. If you choose to re-home them yourself, make sure you're properly vetting all candidates. You don't want your pet going to an unfit home.

As a mama to two amazing rescue dogs myself, it's heartbreaking to hear that pups are being dumped outside without a care in the world. If you see someone attempting to dump their pet, the folks from Shore Animal control suggest that you contact the police immediately.

Source: Facebook

To prepare yourself for a potential incident, always keep your vet's phone number handy, along with an after-hours clinic you can call in an emergency. The ASPCA Animal Poison Control Center also has a hotline you can call at (888) 426-4435 for advice.

Even with all of these resources, however, the best cure for food poisoning is preventing it in the first place. To give you an idea of what human foods can be dangerous, Stacker has put together a slideshow of 30 common foods to avoid. Take a look to see if there are any that surprise you.

Spooky season is upon us! And whether you like to keep your celebrations low-key with a hayride or having the living daylights scared out of you, we've put together your ultimate guide for spooky and haunted attractions in South Jersey this Halloween.

Howl-oween? Meow-een? Even pets are getting in on the costume action this Halloween in South Jersey!

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Animal Control Says Dog Dumping On The Rise Here In South Jersey - catcountry1073.com

Unlocking the Mysteries of Brain Regeneration Groundbreaking Study Offers New Insight – SciTechDaily

Neuron generation trajectories. Credit: BGI Genomics

Because of its distinctive and adorable look, the axolotl Ambystoma mexicanum is a popular pet. Unlike other metamorphosing salamanders, axolotls (pronounced ACK-suh-LAH-tuhl) never outgrow their larval, juvenile stage, a trait known as neoteny. Its also recognized for its ability to regenerate missing limbs and other tissues including the brain, spinal cord, tail, skin, limbs, liver, skeletal muscle, heart, upper and lower jaw, and ocular tissues like the retina, cornea, and lens.

Mammals, including humans, are almost incapable of rebuilding damaged tissue after a brain injury. Some species, such as fish and axolotls, on the other hand, may replenish wounded brain regions with new neurons.

Tissue types the axolotl can regenerate as shown in red. Credit: Debuque and Godwin, 2016

Brain regeneration necessitates the coordination of complex responses in a time and region-specific way. In a paper published on the cover of Science, BGI and its research partners used Stereo-seq technology to recreate the axolotl brain architecture throughout developing and regenerative processes at single-cell resolution. Examining the genes and cell types that enable axolotls to renew their brains might lead to better treatments for severe injuries and unlock human regeneration potential.

Cell regeneration images at seven different time points following an injury; the control image is on the left. Credit: BGI Genomics

The research team collected axolotl samples from six development stages and seven regeneration phases with corresponding spatiotemporal Stereo-seq data. The six developmental stages include:

Through the systematic study of cell types in various developmental stages, researchers found that during the early development stage neural stem cells located in the VZ region are difficult to distinguish between subtypes, and with specialized neural stem cell subtypes with spatial regional characteristics from adolescence, thus suggesting that various subtypes may have different functions during regeneration.

In the third part of the study, the researchers generated a group of spatial transcriptomic data of telencephalon sections that covered seven injury-induced regenerative stages. After 15 days, a new subtype of neural stem cells, reaEGC (reactive ependymoglial cells), appeared in the wound area.

Axolotl brain developmental and regeneration processes. Credit: BGI Genomics

Partial tissue connection appeared at the wound, and after 20 to 30 days, new tissue had been regenerated, but the cell type composition was significantly different from the non-injured tissue. The cell types and distribution in the damaged area did not return to the state of the non-injured tissue until 60 days post-injury.

The key neural stem cell subtype (reaEGC) involved in this process was derived from the activation and transformation of quiescent neural stem cell subtypes (wntEGC and sfrpEGC) near the wound after being stimulated by injury.

What are the similarities and differences between neuron formation during development and regeneration? Researchers discovered a similar pattern between development and regeneration, which is from neural stem cells to progenitor cells, subsequently into immature neurons and finally to mature neurons.

Spatial and temporal distribution of axolotl brain development. Credit: BGI Genomics

By comparing the molecular characteristics of the two processes, the researchers found that the neuron formation process is highly similar during regeneration and development, indicating that injury induces neural stem cells to transform themselves into a rejuvenated state of development to initiate the regeneration process.

Our team analyzed the important cell types in the process of axolotl brain regeneration, and tracked the changes in its spatial cell lineage, said Dr. Xiaoyu Wei, the first author of this paper and BGI-Research senior researcher. The spatiotemporal dynamics of key cell types revealed by Stereo-seq provide us a powerful tool to pave new research directions in life sciences.

Corresponding author Xun Xu, Director of Life Sciences at BGI-Research, noted that In nature, there are many self-regenerating species, and the mechanisms of regeneration are pretty diverse. With multi-omics methods, scientists around the world may work together more systematically.

Reference: Single-cell Stereo-seq reveals induced progenitor cells involved in axolotl brain regeneration by Xiaoyu Wei, Sulei Fu, Hanbo Li, Yang Liu, Shuai Wang, Weimin Feng, Yunzhi Yang, Xiawei Liu, Yan-Yun Zeng, Mengnan Cheng, Yiwei Lai, Xiaojie Qiu, Liang Wu, Nannan Zhang, Yujia Jiang, Jiangshan Xu, Xiaoshan Su, Cheng Peng, Lei Han, Wilson Pak-Kin Lou, Chuanyu Liu, Yue Yuan, Kailong Ma, Tao Yang, Xiangyu Pan, Shang Gao, Ao Chen, Miguel A. Esteban, Huanming Yang, Jian Wang, Guangyi Fan, Longqi Liu, Liang Chen, Xun Xu, Ji-Feng Fei and Ying Gu, 2 September 2022, Science.DOI: 10.1126/science.abp9444

This study has passed ethical reviews and follows the corresponding regulations and ethical guidelines.

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Unlocking the Mysteries of Brain Regeneration Groundbreaking Study Offers New Insight - SciTechDaily

The power of a strong doctor-patient partnership and positivity when fighting lymphoma – Curetoday.com

After hearing the words you have cancer, a persons life instantly changes. Once the initial shock wears off, patients and their caregivers are often met with significant fear and uncertainty for the future. For Louise, a mother of five and grandmother to many more, after learning she had cancer, her oncologist, Dr. Ruemu Birhiray, MD, Hematology Oncology of Indiana, quickly assured her that they were going to fight her disease together. They adopted the motto for every problem, there is a solution, which would become an important mantra for Louise throughout her cancer journey.

Louises cancer story began in November 2019 when she went for a routine check-up. The doctors took her vitals and quickly noticed her pulse was high. Urgently, they recommended Louise go to the emergency room. Once there, Louise was given a computed tomography (CT or CAT) scan and informed that she needed to see an oncologist.

That oncologist turned out to be Dr. Birhiray, who diagnosed Louise with diffuse large B-cell lymphoma (DLBCL), the most common type of non-Hodgkin lymphoma (NHL), which affects approximately 28,000 people per year in the United States. DLBCL is a fast-growing but treatable cancer affecting B-lymphocytes, also known as B cells, a type of white blood cell that helps the body fight infections. As they develop, cancerous B cells become larger than normal and multiply uncontrollably.

Meeting Dr. Birhiray, I realized pretty quickly that he was going to take good care of me, said Louise. One of the first things you notice with Dr. Birhiray is how warm of a person he is. It felt like he was talking to me, not at me, and he was very attentive to my needs and questions.

After going through an intensive chemotherapy regimen, Louise was thrilled to hear that her DLBCL had gone into remission, only to learn six months later that the cancer had returned. That unfortunately made Louise one of up to 50% of patients whose DLBCL relapses (returns) or does not respond to treatment (becomes refractory).

While initially devasted to hear the cancer had returned, Louise and Dr. Birhiray swiftly worked together to determine next steps.

When Louises cancer relapsed after initial treatment, I wanted to take a different approach, said Dr. Birhiray. For her next treatment, I initially thought about doing a bone marrow transplant, but together we decided it wasnt appropriate. So I considered a different treatment regimen that had proven results in certain patients and did not require a hospital stay.

Dr. Birhiray again assured Louise that for every challenge, there are options. For Louise, that option was ultimately Monjuvi (tafasitamab-cxix) a targeted immunotherapy treatment given with another medicine called lenalidomide to treat adults with certain types of DLBCL that has come back or that did not respond to previous treatment and who cannot receive a stem cell transplant.

Shortly after beginning treatment with Monjuvi and lenalidomide, Louise had to go to another unrelated check-up that involved a CAT scan, where she received extremely encouraging news: her cancer was showing rapid improvement. A couple of months later, a positron emission tomography (PET) scan revealed there were no detectable signs of cancer in her body.

It was such a relief to no longer see any cancer on the CAT scan and to have confirmation that treatment with Monjuvi had worked for me, said Louise. Im very grateful to Dr. Birhiray and my healthcare team for helping me through my journey with DLBCL so far. They are always so positive and honest with me, and I feel like they listened to my needs and included me in important decisions, which made getting through treatment so much easier.

Louise is representative of a patient responding to Monjuvi. Every patient is different and individual results may vary. Louise continues to be under the care of Dr. Birhiray who routinely checks to make sure her cancer has not returned. Please read the Important Safety Information below to learn more about the side effects of Monjuvi.

Dr. Birhiray was also pleased by Louises results with Monjuvi. From their very first meeting, he had worked closely with Louise to develop a treatment plan that took into account her individual needs and circumstances.

According to Dr. Birhiray, it is also critical to involve patients in treatment-related decisions by having open and honest conversations about their options and what will happen in their body with certain treatments, including possible side effects. Beyond the effects of treatments, Dr. Birhiray believes it is important to account for a patients treatment goals, which includes factors such as the experience they are seeking while undergoing treatment and their life goals while on and following treatment.

As an oncologist, you really need to get to know your patient and establish trust from the beginning said Dr. Birhiray. More than just knowing their names, you need to know their bodies and understand their disease and how it affects them in order to develop a treatment plan that meets their needs. This requires in-depth conversations that can take upwards of an hour, in which I ensure my patients are knowledgeable about the treatment they are about to undergo and how it will affect them, and to understand how they are feeling.

Louises DLBCL continues to be in remission and she has a positive outlook for her future. She hopes her story can inspire others to build relationships with their doctors like the one she has with Dr. Birhiray.

I feel extremely fortunate to have found Dr. Birhiray and received a treatment for my DLBCL that led to remission, said Louise. I feel strongly that my outcome is a result of the partnership with my oncologist, working together to come up with a treatment plan that was right for me.

If you, like Louise, have DLBCL that came back or didnt respond to the first treatment (relapsed or refractory DLBCL), start a conversation with your healthcare team about your options. To learn more about Monjuvi, DLBCL and for support and resources, visit http://www.Monjuvi.com.

What is MONJUVI?

MONJUVI (tafasitamab-cxix) is a prescription medicine given with lenalidomide to treat adults with certain types of diffuse large B-cell lymphoma (DLBCL) that has come back (relapsed) or that did not respond to previous treatment (refractory) and who cannot receive a stem cell transplant.

It is not known if MONJUVI is safe and effective in children.

The approval of MONJUVI is based on a type of response rate. There is an ongoing study to confirm the clinical benefit of MONJUVI.

IMPORTANT SAFETY INFORMATION

What are the possible side effects of MONJUVI?

MONJUVI may cause serious side effects, including

The most common side effects of MONJUVI include

These are not all the possible side effects of MONJUVI. Your healthcare provider will give you medicines before each infusion to decrease your chance of infusion reactions. If you do not have any reactions, your healthcare provider may decide that you do not need these medicines with later infusions. Your healthcare provider may need to delay or completely stop treatment with MONJUVI if you have severe side effects.

Before you receive MONJUVI, tell your healthcare provider about all your medical conditions, including if you

You should also read the lenalidomide Medication Guide for important information about pregnancy, contraception, and blood and sperm donation.

Tell your healthcare provider about all the medications you take, including prescription and over- the-counter medicines, vitamins, and herbal supplements.

Call your doctor for medical advice about side effects. You may report side effects to the FDA at (800) FDA-1088 or http://www.fda.gov/medwatch. You may also report side effects to MORPHOSYS US INC. at (844) 667-1992.

DIRECTIONALS TO THE PI:

Please see the full Prescribing Information, including Patient Information, for additional Important Safety Information.

These participants were compensated for their time.

RC-US-TAF-01576 August 2022

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The power of a strong doctor-patient partnership and positivity when fighting lymphoma - Curetoday.com

Cell culture market is projected to grow at a CAGR of 11.11% during the forecast period – openPR

Cell Culture Market

Key players covered in the Cell Culture Market report are Thermo Fisher Scientific, BD, General Electric, Merck KGaA, Lonza, HiMedia Laboratories, FUJIFILM Irvine Scientific, Miltenyi Biotec, InvivoGen, Danaher, Eppendorf AG, Bio-Rad Laboratories , Inc., Corning Incorporated, Sartorius AG, PromoCell GmbH, VWR International LLC, Illumina Inc., Novogene Co., Ltd., Geneious, and Advanced BioMatrix, Inc., among other domestic and global players. Market share data is available separately for Global, North America, Europe, Asia-Pacific (APAC), Middle East and Africa (MEA) and South America . DBMR analysts understand competitive strengths and provide competitive analysis for each competitor separately.

This Cell Culture Market report provides details about recent new developments, trade regulations, import and export analysis, production analysis, value chain optimization, share of market, the impact of domestic and localized market players, analyzes opportunities in terms of emerging revenue pockets, market changes regulations, strategic market growth analysis, market size, category market growth, applications of niche and domain, product approvals, product launches, geographic expansions, technological innovations in the market. For more insights on Cell Culture Market, please contact Data Bridge Market Research for a analysis note. Our team will help you make an informed market decision to achieve market growth.

For more information on Market Analysis, view the Research Report Summary at:- https://www.databridgemarketresearch.com/reports/global-cell-culture-market

Cell Culture Market Scope and Market SizeThe cell culture market is segmented on the basis of product, application, and end user. The growth between these segments will help you analyze low growth segments within industries and provide users with valuable market insights and insights to help them make strategic decisions to identify major applications of the market.

Based on product, the cell culture market is segmented into consumables and equipment.Based on application, the cell culture market is segmented into biopharmaceutical production, diagnostics, drug detection and development, stem cell research, tissue engineering, and regenerative medicine, among other applications.On the basis of end user, the cell culture market is segmented into pharmaceutical and biotechnology companies, hospitals and diagnostic laboratories, research institutes and cell banks.

Country Level Analysis of the Cell Culture MarketCell Culture Market is analyzed and market size insights and trends are provided by country, product, application and end-user as above. The countries covered in the Cell Culture market report are USA, Canada & Mexico, North America, Germany, France, UK, Netherlands, Switzerland , Belgium, Russia, Italy, Spain, Turkey, the rest of Europe in Europe, China and Japan. , India, South Korea, Singapore, Malaysia, Australia, Thailand, Indonesia, Philippines, Rest of Asia-Pacific (APAC) in Asia-Pacific (APAC), Saudi Arabia, United Arab Emirates, South Africa, Egypt, Israel, Rest of Middle East and Africa (MEA) within Middle East and Africa (MEA), Brazil,

North America dominates the cell culture market due to rising healthcare costs. Furthermore, increasing elderly population will further drive the cell culture market growth in the region during the forecast period. The Asia-Pacific region is expected to see significant growth in lower stem cell transplant spending. Furthermore, increasing large-scale research and development is expected to drive the cell culture market growth in the region in the coming years.

Explore Complete TOC At:- https://www.databridgemarketresearch.com/toc/?dbmr=global-cell-culture-market

The country section of the Cell Culture market report also provides individual market impact factors and regulatory changes in the national market that affect current and future market trends. Data points such as consumption volumes, production sites and volumes, import and export analysis, price trend analysis, raw material cost, value chain analysis Downstream and Upstream are some of the major indicators used to forecast the market scenario for each country. Additionally, the presence and availability of global brands and the challenges they face due to significant or rare competition from local and national brands.

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Cell culture market is projected to grow at a CAGR of 11.11% during the forecast period - openPR

Outstanding Midwestern News! We Might Have An Excuse To Not Rake Leaves This Fall – 1440wrok.com

We're still a few weeks away from the leaves changing color and eventually fall to the ground causing everyone with deciduous trees to pick up a rake and gather the leaves into an appropriate receptacle.

But what if the ecologically sound decision was to just leave them wherever they fell?

That's what the Minnesota Bee Lab would like you to do.

According to the Bee Lab, (and where else would you get your bee news from?) the U.S. Fish and Wildlife Service is considering putting the American bumblebee on the endangered species list.

The significant drop in bee population isn't a new story. It's been known for a while that the bee population is in trouble and the fallout in the near future could be disastrous.

No bees isn't a left or right issue. That's an everyone issue. No bees = a very bad time for humanity.

So what does this have to do with raking leaves? Great question.

The University of Minnesota Bee Lab suggests to "leave some messy piles of leaves in the corner of your yard. This will give queen bees somewhere to nest for the winter. If the queen doesn't make it, no one makes it.

While they suggest that you only need to leave a couple piles of leaves in your yard, I think for the good of humanity, we should just leave all the leaves on the ground this year. If it's good enough for Yellowstone, it's good enough for your Illinois home.

Some other bee friendly tips from a Master Gardener:

Be sure to have this article handy when a nosy neighbor asks you to clean up your yard this fall. Just tell them you're doing it for the planet. I'm sure they'll understand.

Eight Wisconsin Hikes That Will Immerse You In the Beauty of Fall

To prepare yourself for a potential incident, always keep your vet's phone number handy, along with an after-hours clinic you can call in an emergency. The ASPCA Animal Poison Control Center also has a hotline you can call at (888) 426-4435 for advice.

Even with all of these resources, however, the best cure for food poisoning is preventing it in the first place. To give you an idea of what human foods can be dangerous, Stacker has put together a slideshow of 30 common foods to avoid. Take a look to see if there are any that surprise you.

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Outstanding Midwestern News! We Might Have An Excuse To Not Rake Leaves This Fall - 1440wrok.com

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