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Joseph P. boosted
Elon Musk's Jet

Thanks for joining us on Mastodon now!

Other platforms Instagram, Facebook, Telegram
grndcntrl.net/links/

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Joseph P. boosted
Skulls in the Stars

I miss the naive old days when Bill Gates was the worst billionaire we could imagine

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Joseph P. boosted
bioRxiv

Sequencing-free Tissue-wide Spatial Profiling of Post-transcriptional Regulations biorxiv.org/content/10.1101/20

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Joseph P. boosted
Gregg Gonsalves

Put that into the context of the racist, antisemitic, homophobic hate unleashed on Twitter over the past few months and you can see that Elon Musk loves this, this monetizing of hate, it arouses him, it gets him going. 5/

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Joseph P. boosted
Gregg Gonsalves

I don't care what you think of the man, but the idea that Elon Musk, thug and right wing oligarch can amp up hate directed towards one man is evil. It just is. 4/

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Joseph P. boosted
Gregg Gonsalves

This is an 81 year old scientist and physician. He and his family have had death threats for close to three years and needed Secret Service protection. 3/

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Joseph P. boosted
Gregg Gonsalves

But we NEVER rained down threats on anyone. Now Elon Musk on the bird site is tweeting out "prosecute/Fauci." 2/

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Joseph P. boosted
Gregg Gonsalves

If you know my history, you know I grew up as part of ACT UP, the AIDS activist group in the 80s and 90s. I've protested every President, multiple drug companies, and federal officials. 1/

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Joseph P.

If you're a full grown professional that's learning an 'umpteenth" language, i dont like you because you're better than me and I'm small minded

qoto.org/@true_mxp/10949178018

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Joseph P. boosted
Hao Yin

Apold1, a -enriched gene, in pathological
⏬Reperfusion (3 dpi🤓)-> An arteriogenic defect?
⏫border zone vascularization at day 21 but not day 7
Tumor ⏫Nonproductive angiogenesis-> more non-perfusable endothelial channels

Apold1 KO⏬EC Proliferation-How😁

@bohaceklab@nerdculture.de & Katrien de Bock bioRxiv 2022
biorxiv.org/content/10.1101/20

Also very interesting, Apold1 KO->⏫KLF2 & KLF4 in EC

Apold1 is recently identified as an ascending aortic EC-enriched gene (vs descending aorta/carotid artery)
Dr. Thomas Quertermous lab bioXRiv 2022
biorxiv.org/content/10.1101/20

Are Apold1 KO mice ready for /#Aneurysm?

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Joseph P. boosted
🎓 Doc Freemo :jpf: 🇳🇱

I am excited to hear that as of today the user member count int he has just hit a record high of ~400,000 user members! That gets us to about 5% fediverse coverage!

@ufoi

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Joseph P. boosted
Philip N Cohen

#ChatGPT is very cagey about #gender. But if you ask it for stories, with, "Tell a story about...", you can see: statistical matches with working class jobs, like dental hygienist ("Sarah"), truck driver ("Jake"), police officer ("John"). With male dominated professional jobs, you get only women: Nuclear physicist, aerospace engineer, corporate executive, store owner. But if you make the story about some "abusive" ("abusive store owner") or #SexualHarassment, they become male.

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Joseph P. boosted
Yogi Jaeger

Scary how much this describes the current situation in Austria as well. We are about to get orbanized. Well, we've been about to get orbanized for a while...
---
RT @TimothyDSnyder
Six years ago, I published a list of political advice following Trump's election, which became the pamphlet "On Tyranny." The history of #fascism was important in that advocacy. I wrote then that "post-truth is pre-fascism," which has proven true. https:…
twitter.com/TimothyDSnyder/sta

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Joseph P.

@explainpaper

Tumoral Immune Cell Exploitation in Colorectal Cancer Metastases Can Be Targeted Effectively by Anti-CCR5 Therapy in Cancer Patients

Niels Halama, Inka Zoernig, Anna Berthel, Christoph Kahlert, Fee Klupp, Meggy Suarez-Carmona,Thomas Suetterlin, Karsten Brand, Juergen Krauss, Felix Lasitschka, Tina Lerchl, Claudia Luckner-Minden, Alexis Ulrich, Moritz Koch, Juergen Weitz, Martin Schneider, Markus W. Buechler, Laurence Zitvogel,
Thomas Herrmann, Axel Benner, Christina Kunz, Stephan Luecke, Christoph Springfeld, Niels Grabe, Christine S. Falk, and Dirk Jaeger

Targeting Tumor-Promoting Microenvironment Through CCR5 Blockade in Metastases

progression is a process in which cancer cells and cells interact with each other in a way that can lead to the growth and spread of cancer. In cancer, when the cancer has spread to other parts of the body, it is called and it is very difficult to treat. Treatments such as PD-1/PD-L1 blockade and modulation have been successful in modifying the interactions between the immune system and cancer, leading to the rejection or suppression of progression. Cancer cells can also alter the immune microenvironment, leading to and evasion. In this research paper, the authors studied the microenvironment in metastases and identified a network of cells and immune cells that exploit the CCL5-CCR5 axis. They then investigated and characterized the effects of blocking the CCL5-CCR5 axis.

the microenvironment of metastases of cancer ().

the environment induces migration of T lymphocytes, which produce a called CCL5. This CCL5 then supports tumor growth and spread by influencing macrophages and cells. The environment is immunosuppressive and the tumor cells are exploiting the host's cells to their advantage. In other words, the tumor cells are using the host's immune cells to help them grow and spread.

the effects of CCR5 blockade on the level.

Tumor death and a specific pattern of and modulation are observed in the and in biopsies from a . Macrophages are the key for these anti-tumoral effects, as they produce IFNs and reactive oxygen species which cause tumor cell death. blockade induces a phenotypic shift in the macrophages, which is referred to as a switch from an M2 to an M1 phenotype. This repolarization also reduces levels of CD163+ cells, reshaping the cell composition in the microenvironment. The influx of new effector cells due to CCR5 inhibition can shift the effects of CCL5 towards beneficial effects, such as reduction of , , and resistance.

The microenvironment of the invasive margin of metastases.

There was no relevant Th1, Th2, or Th17 signature present in any of the samples. However, the authors did find that and -related cytokines were significantly increased at the invasive margin. Chemokines are molecules that help to attract cells to the area, and macrophage-related cytokines are molecules that help to regulate the activity of , which are a type of immune cell. 98% of the CD3+ s in the resection specimens were positive for PD-1, which is a molecule that helps to regulate the activity of the immune system.

is a protein produced by T cells, which are a type of white blood cell. is a receptor found on metastatic tumor cells, which are cancer cells that have spread from the primary to other parts of the body. In this research paper, it was found that CCL5 has tumor-promoting effects on cells and tumor-associated s. This means that CCL5 has multiple effects on both the cancer cells and the macrophages, which are a type of white , that are associated with the . CCL5 was produced mainly by T cells located at the invasive margin and stroma of metastases, and that CCR5 was dominantly expressed by metastatic tumor cells. CCL5 also had effects on tumor , invasive tumor , and increased production of matrix es by tumor-associated macrophages. Finally, they found that CCR5 inhibition had an effect on key molecules of to transition ( ).

The researchers wanted to test the effects of blockade, which is a way of blocking the CCR5 receptor on cells, using a drug called maraviroc. They used human s, which are samples of from advanced patients with metastases. Maraviroc led to morphologically overt tumor in the , which means that the tumor cells died and changed in appearance. The researchers then tested the hypothesis that s, (type of white blood cell), were required for the tumor cell death-inducing effects of CCR5 blockade. They used clodronate s to deplete CD163+ TAMs, ( s associated with tumors) and found that combining clodronate with CCR5 inhibition abrogated the immediate tumor cell death-inducing effects of inhibition. This confirmed the role of macrophages in this process. IFN-g induced stromal CD163+ death and led to a reconfiguration of the cell compartment. Inhibition of macrophage-derived reactive oxygen species could partially block the anti-tumoral effects of CCR5 inhibition. Finally, they tested the effects of CCL5/CCR5 inhibition and found that both a CCL5 neutralizing antibody and a CCR5 blocking had similar functional effects to maraviroc.

A (MARACON) was conducted to test the effects of a drug called maraviroc on patients with advanced-stage colorectal . The involved taking biopsies of the patients before and after treatment with maraviroc, and the results showed that the drug had beneficial effects on the tumor-promoting and led to objective clinical responses. These responses included induction of central , reduction of tumor cell death, and reduction of key s and growth factors that promote tumor growth. The drug was also found to be very well tolerated, with mild elevation of enzymes being the most common side effect. Finally, the trial showed that partial responses were achieved in patients with previously refractory disease.

CCR5 blockade, is a type of used to treat .

The MARACON clinical trial, showed that CCR5 blockade had a positive effect on the tumor microenvironment and led to a higher response rate in subsequent chemotherapies. The authors suggest that this effect is not limited to the metastases, but is a systemic feature. They also suggest that the local presence of multiple layers of subversion in cancers depends on the individual tissue, , tumor type, and the difference between primary and metastatic lesion. The authors also found that the results of the were in line with the results of a fully human organotypic tumor , which is a simple model with a straightforward approach. The authors also note that the survival data from the trial is not conclusive due to the limited number of patients, but that the objective treatment responses are very encouraging. They suggest that CCR5 blockade may be a promising approach and needs to be evaluated further scientifically and clinically.

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Joseph P. boosted
Caroline Lynn Kamerlin

Our latest paper, exploring allosteric rescue of catalysis through a protein-protein interface in the activation of ATP phosphoribosyltransferase. @CorbellaMorato@twitter.com @fisher_gem@twitter.com @GT_CHEM@twitter.com @UUBiochem@twitter.com nature.com/articles/s41467-022

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Joseph P. boosted
Philip N Cohen

I reviewed a paper for International J of Enviro Res and Pub Health, an MDPI journal you may not think highly of. Now that it has been published, you can evaluate it and see: "Fertility Intention and Influencing Factors for Having a Second Child among Floating Women of Childbearing Age." mdpi.com/1660-4601/19/24/16531. They also posted the reviews and author responses. I made substantive suggestions, and they improved it (IMO). It was published #OA 5 weeks after submission.
#demography

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Joseph P.

Using Human Pluripotent Stem Cells to Create Human Skeletal Muscle Organoids for Repair and Regeneration 

Skeletal is a type of tissue that makes up a large part of the human body. It is made up of many different cells that are able to contract and move. Skeletal muscle has the ability to itself when it is damaged due to , exercise, or diseases like . A small group of cells called s help with the repair process. Scientists have been trying to create models to study how develops and regenerates. Recently, they have been using human pluripotent to create 3D models of skeletal muscle tissue. However, these models have not been able to recreate the full process of muscle regeneration. In this research paper, the authors introduce a new method of using human pluripotent stem cells to create 3D models of skeletal muscle tissue that can retain the ability to repair itself.

Over the past decades, scientists have used to study , which is regulated by s. These animal models have been very helpful in understanding the mechanisms of muscle , but they don't always accurately reflect the same range of diseases that humans experience. Therefore, researchers have suggested creating reliable in vitro models using human muscle cells. ( s) could be used to create 3D human skeletal muscle s ( s) that contain sustainable and distinct myofibers with the same proteins and structure as adult muscles. Previous approaches to skeletal muscle differentiation have been developed using 2D systems, but these lack the natural environment and niche that are necessary to model adult and muscle .

s ( s) can be used to repair damaged muscle tissue. They explain that SCs can be activated in response to muscle injuries and that other types can contribute to the process of . The author then goes on to explain that s, such as IL-4, can influence the and promote SCs differentiation, which helps with muscle regeneration. While s generated from s have potential, they do not fully replicate the in vivo native microenvironment. To address this, treat the s with extrinsic s to promote . s might then be used to study aspects of human muscle and to identify novel candidates for muscle-wasting disorders.

To create a 3D structure of muscle tissue. They used activator and inhibitors at the beginning of the differentiation process to induce paraxial s. They then added to the Matrigel to promote the 3D structure. and IGF1 were added later to accelerate the specification and further differentiation. They optimized the timing of the Matrigel embedding to day seven. After this, they observed s and withdrew FGF2 to focus on muscle tissue development. They then prolonged the HGF and IGF1 treatment to propagate s. They found that 62% of the was tissue and that it contained PAX7+ / cells, MYOD+ activated/committed s, and MYOG+ s. They also found that 31% of PAX7+/Ki67− and 29% of MYOD−/PAX7+ non-dividing quiescent SCs were present in the mature s. This indicates that the s were able to effectively recreate nic and have regenerative potential. Future studies using sequencing may be necessary to further characterize the different types of cells in s.

The stepwise process to generate human skeletal muscle organoid s (hSkMOs) from human pluripotent stem cells (hPSCs)

The process begins with dissociating s into s and allowing them to form bodies ( s) in low-attachment V-shaped 96-well plates. Then, paraxial differentiation is promoted with activation, BMP inhibition, and FGF2 signaling. The expression of pluripotency markers OCT4 and NANOG decreases, and the expression of markers Brachyury, T-Box transcription factor 6 (TBX6), and mesogenin 1 (MSGN1) increases. To further characterize paraxial al differentiation, TBX6 is ed. After paraxial induction, the s are embedded with growth factor-reduced Matrigel and transferred to a six-well plate on an orbital shaker. Growth factors are then added to the specification media, and s are cultured until the day of analysis. The orbital shaker improves the viability, survival, and differentiation of hSkMOs by increasing the penetration rate of oxygen and nutrients into the core area of hSkMOs. The gradually grow to more than 1.5 mm in diameter by day 60, appearing round-shaped, uniformly sized, and having relatively homogenous morphology. PAX3 and PAX7 are progenitor markers, and their expression is verified by qRT-PCR and sections. The cells appear as clusters, and approximately 9% of PAX7+ cells are double-positive for Ki67 at day 30, demonstrating that proliferating cells are s in hSkMOs. This indicates that the in vitro is able to recapitulate the features of embryonic skeletal development.

The different types of stem/progenitor cells that are involved in myogenesis, the process of muscle formation.

The researchers used qRT-PCR analysis and to identify and characterize the different types of cells. They found that PAX3 and PAX7 (SC markers) were the major population during the early stage of , and that MYOD (proliferating and activated SC marker) and MYOG (differentiated myocyte marker) increased over time. They also observed that MYOD−/PAX7+, MYOD+/PAX7+, and MYOD+/Ki67+ cells accounted for 29%, 6%, and 8% of the putative quiescent, activated, and proliferating s, respectively. MYOD+/PAX7− cells constituted 39% of differentiating myoblasts, and MYOG−/PAX7+ cells constituted 23% of putative quiescent SCs. MYOG+/PAX7− cells accounted for 30% of differentiated s, and 8% and 6% of the MYOG+ cells in s co-expressed PAX7 and Ki67, respectively. This data shows that the researchers were able to identify and characterize different types of skeletal muscle stem/progenitor cells during .

The text is discussing the results of a research study that used hSkMOs (human skeletal muscle s) to study the development of skeletal muscle . The study found that the s grew exponentially in size within two months, and the growth rate then steadily decreased. The researchers then used scanning electron microscopy (SEM) imaging and confocal microscopy to examine the cytoarchitecture of the hSkMOs. They found that the hSkMOs contained a large population of terminally differentiated cells and a small population of preserved myogenic stem/progenitor cells. They also found that the hSkMOs contained a substantial proportion of TITIN+ muscle cells and MAP2-positive s. To further characterize the presence of sustainable stem cells within the mature hSkMOs, they quantified the amount of dormant stem cells by imaging. The results showed that approximately 56%, 31%, and 5% of PAX7+/Ki67- putative dormant stem cells existed throughout the differentiation of hSkMOs at days 30, 70, and 130, respectively. This indicates that the hSkMOs contained mature skeletal muscle properties and had the potential for .

The researchers wanted to see if the s (human muscle s) had the ability to regenerate after damage. To test this, they treated the hSkMOs with a cardiotoxin (CTX) which is known to induce muscle inflammation and damage. They then observed a decrease in PAX7+ and MYOD+ cells in the hSkMOs. To further test the potential of the s, they added interleukin-4 (IL-4) to the medium to promote . After 14 days, they observed a significant increase in MYOG+ myocytes in the CTX-injured hSkMOs with the treatment of IL-4 compared to the CTX-injured hSkMOs without the treatment. This suggests that the hSkMOs have the potential to regenerate muscle tissue after damage.

Generation of Skeletal Muscle Organoids from Human Pluripotent Stem Cells to Model Myogenesis and Muscle Regeneration

Authors :

Min-Kyoung Shin , Jin Seok Bang , Jeoung Eun Lee , Hoang-Dai Tran , Genehong Park , Dong Ryul Lee and Junghyun Jo

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Joseph P. boosted
Miguel Guhlin 🦉 🇵🇦 🇺🇲

Yikes, my flow diagram is woefully out of date. It has been awhile since I updated it.

Here's the latest (but not last) version with fresh numbers, but looking at it now, I see some problems.

While I still am connected to folks on work social media (the ones I maintain to share work resources through) like Linked In, / , , sharing content once to many social media outlets is still difficult.

IFTTT and Twitter are still at the center of it all and it doesn't play nice with Mastodon as far as I can tell. The Toot Bookmarklet with moa.party cross-poster has proven invaluable in cutting out and , but what I wish was a simple RSS feed to Mastodon, then Mastodon to , , etc.

Of course, this is cross-posting blasphemy on , but posting once and seeing it go everywhere else frees up time for more conversation while meeting people where they are, not where I think they SHOULD be.

Anyone else having fun with this kind of thing?

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Joseph P.

Invitations to http://Lex.Paper 

Hi there folks !

I have some invitations to http://Lex.Paper that you might want.

http://Lex.Paper is an AI-assisted collaborative cloud-document app.

It has features such as real-time collaboration, easy organization, and powerful editing tools.

It helps you to work faster, together with teammates and colleagues, while focusing on what matters most.

We know how valuable a good team collaboration platform can be and want to help everyone take their productivity to the next level.

(Written by http://Lex.paper)

Just comment here, maybe give us a boost if you like, I’ll try to figure out DMs to send the invite links.

here's an invite to the first person that sees this :-) lex.page/invites/XSLMNRLD

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Joseph P. boosted
Text Adventure

@tonic They reply: "We could stop with the tomcat crowdthere’s lots of food and she’s feeling proudshe’s every one’s chunky girl i know she probably won’t a single moment before starting to improve the world."

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