WKD Hellboy | πŸ΄σ §σ ’σ ³σ £σ ΄σ ΏπŸ³οΈβ€πŸŒˆπŸ‡ΊπŸ‡¦'s Avatar

WKD Hellboy | πŸ΄σ §σ ’σ ³σ £σ ΄σ ΏπŸ³οΈβ€πŸŒˆπŸ‡ΊπŸ‡¦

@wkdhellboy.bsky.social

I am who, I am, and I am not, who I am not. He/Him, They/Them, Gay, 21

49 Followers  |  114 Following  |  5 Posts  |  Joined: 05.08.2023  |  2.0188

Latest posts by wkdhellboy.bsky.social on Bluesky

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From me, a list of Trump supporters who killed, or tried to kill, Democrats and opponents of Trump in recent years (since the right are now claiming all the political violence is from the left!)

Receipts:
zeteo.com/p/charlie-ki...

11.09.2025 15:22 β€” πŸ‘ 12700    πŸ” 5748    πŸ’¬ 337    πŸ“Œ 276

I am horrified. If you use US material, download all old reports you use. The record will be erased. Even that might not save you: every report sourced from the US will now have to be suspected of politicised manipulation and will in the future the same credibility as Iran’s human rights reports

08.08.2025 08:37 β€” πŸ‘ 536    πŸ” 341    πŸ’¬ 27    πŸ“Œ 14

Betelgeuse and Beeblebrox!

23.07.2025 00:05 β€” πŸ‘ 4    πŸ” 0    πŸ’¬ 0    πŸ“Œ 0
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pokΓ©mon logos i made

15.05.2025 15:06 β€” πŸ‘ 6534    πŸ” 1829    πŸ’¬ 87    πŸ“Œ 12

Define β€œBeautiful”

The Tale of Princess Kaguya

09.05.2025 19:21 β€” πŸ‘ 3    πŸ” 0    πŸ’¬ 0    πŸ“Œ 0

Watch Barbie come to life like never before!

14.04.2025 07:06 β€” πŸ‘ 2    πŸ” 0    πŸ’¬ 0    πŸ“Œ 0

I don’t know if he could be but I want to see Gen return so bad!

28.03.2025 17:30 β€” πŸ‘ 1    πŸ” 0    πŸ’¬ 0    πŸ“Œ 0
IMPORTANT THINGS TO NOTE !! β€’ KEEP IN MIND THESE ARE RESULTS THAT HAVE HELD UP APPROXIMATELY THREE YEARS showing that benefits demonstrated years ago have held up over time. That is ASTOUNDING. β€’ Researchers say the results of a Phase I trial of an therapeutic cancer vaccine aimed at preventing kidney cancer show promise. β€’ This new study found that ALL patients with ADVANCED stage kidney cancer had successful anti-cancer immune responses AND have remained CANCER-FREE approximately THREE years after treatment. β€’ The study, demonstrates the potential of personalized vaccines to change the course of certain cancer types, but larger, longer trials are needed to confirm this approach. β€’ Cancer vaccines developed with different molecular recipes are still in their early stages, before strong conclusions can be made. β€’ While the findings are encouraging, the vaccine is still in early testing and will likely take years before it becomes widely available.

IMPORTANT THINGS TO NOTE !! β€’ KEEP IN MIND THESE ARE RESULTS THAT HAVE HELD UP APPROXIMATELY THREE YEARS showing that benefits demonstrated years ago have held up over time. That is ASTOUNDING. β€’ Researchers say the results of a Phase I trial of an therapeutic cancer vaccine aimed at preventing kidney cancer show promise. β€’ This new study found that ALL patients with ADVANCED stage kidney cancer had successful anti-cancer immune responses AND have remained CANCER-FREE approximately THREE years after treatment. β€’ The study, demonstrates the potential of personalized vaccines to change the course of certain cancer types, but larger, longer trials are needed to confirm this approach. β€’ Cancer vaccines developed with different molecular recipes are still in their early stages, before strong conclusions can be made. β€’ While the findings are encouraging, the vaccine is still in early testing and will likely take years before it becomes widely available.

How personalized peptide cancer vaccines work Scientists identify neoantigens, abnormal proteins produced by cancer cells. They take a sample of the patient's mutated cancer cells. The neoantigens are used to create a vaccine tailored to the patient's tumor. The vaccine is administered, prompting the immune system to target the cancer cells with those proteins. The immune system's T-cells attack and destroy the tumor cells, shrinking the cancer.

How personalized peptide cancer vaccines work Scientists identify neoantigens, abnormal proteins produced by cancer cells. They take a sample of the patient's mutated cancer cells. The neoantigens are used to create a vaccine tailored to the patient's tumor. The vaccine is administered, prompting the immune system to target the cancer cells with those proteins. The immune system's T-cells attack and destroy the tumor cells, shrinking the cancer.

ABSTRACT Personalized cancer vaccines (PCVs) can generate circulating immune responses against predicted neoantigens. However, whether such responses can target cancer driver mutations, lead to immune recognition of a patient's tumour and result in clinical activity are largely unknown. These questions are of particular interest for patients who have tumours with a low mutational burden. Here we conducted a phase l trial (ClinicalTrials.gov identifier NCTO2950766) to test a neoantigen-targeting PCV in patients with high-risk, fully resected clear cell renal cell carcinoma (RCC; stage Ill or IV) with or without ipilimumab administered adjacent to the vaccine. At a median follow-up of 40.2 months after surgery, none of the 9 participants enrolled in the study had a recurrence of RCC. No dose-limiting toxicities were observed. All patients generated T-cell immune responses against the PCV antigens, including to RCC driver mutations in VHL, PBRM1, BAP1, KDM5C and PIK. Following vaccination, there was a durable expansion of peripheral T-cell clones. Moreover, T-cell reactivity against autologous tumours was detected in seven out of nine patients. Our results demonstrate that neoantigen-targeting PCVs in high-risk RCC are highly immunogenic, capable of targeting key driver mutations and can induce antitumour immunity. These observations, in conjunction with the absence of recurrence in all nine vaccinated patients, highlights the promise of PCVs as effective adjuvant therapy in RCC.

ABSTRACT Personalized cancer vaccines (PCVs) can generate circulating immune responses against predicted neoantigens. However, whether such responses can target cancer driver mutations, lead to immune recognition of a patient's tumour and result in clinical activity are largely unknown. These questions are of particular interest for patients who have tumours with a low mutational burden. Here we conducted a phase l trial (ClinicalTrials.gov identifier NCTO2950766) to test a neoantigen-targeting PCV in patients with high-risk, fully resected clear cell renal cell carcinoma (RCC; stage Ill or IV) with or without ipilimumab administered adjacent to the vaccine. At a median follow-up of 40.2 months after surgery, none of the 9 participants enrolled in the study had a recurrence of RCC. No dose-limiting toxicities were observed. All patients generated T-cell immune responses against the PCV antigens, including to RCC driver mutations in VHL, PBRM1, BAP1, KDM5C and PIK. Following vaccination, there was a durable expansion of peripheral T-cell clones. Moreover, T-cell reactivity against autologous tumours was detected in seven out of nine patients. Our results demonstrate that neoantigen-targeting PCVs in high-risk RCC are highly immunogenic, capable of targeting key driver mutations and can induce antitumour immunity. These observations, in conjunction with the absence of recurrence in all nine vaccinated patients, highlights the promise of PCVs as effective adjuvant therapy in RCC.

This study involved a large and collaborative team across multiple institutions, with key leadership from co-senior authors Toni Choueiri, Derin Keskin, Patrick Ott, and Catherine Wu from DFCI. Research reported in this release was supported by the National Institutes of Health under award numbers 1R37CA279822-01 and P30CA016359. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. The research was also funded by the Gateway for Cancer Research, U.S. Department of Defense, Louis Goodman and Alfred Gilman Yale Scholar Fund, Yale Cancer Center, Dana-Farber/ Harvard Cancer Center, Harvard Medical School, Trust Family Foundation, Michael Brigham, Pan Mass Challenge, Hinda L. and Arthur Marcus Foundation, The Loker Pinard Fund for Kidney Cancer Research at Dana-Farber Cancer Institute, and Conquer Cancer Foundation/Sontag Foundation.

This study involved a large and collaborative team across multiple institutions, with key leadership from co-senior authors Toni Choueiri, Derin Keskin, Patrick Ott, and Catherine Wu from DFCI. Research reported in this release was supported by the National Institutes of Health under award numbers 1R37CA279822-01 and P30CA016359. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. The research was also funded by the Gateway for Cancer Research, U.S. Department of Defense, Louis Goodman and Alfred Gilman Yale Scholar Fund, Yale Cancer Center, Dana-Farber/ Harvard Cancer Center, Harvard Medical School, Trust Family Foundation, Michael Brigham, Pan Mass Challenge, Hinda L. and Arthur Marcus Foundation, The Loker Pinard Fund for Kidney Cancer Research at Dana-Farber Cancer Institute, and Conquer Cancer Foundation/Sontag Foundation.

The study has been published in Nature. YES, it is PEER-REVIEWED.
β€’ www.nature.com/articles/s41...

IMPORTANT THINGS TO NOTE ‼️

26.02.2025 17:02 β€” πŸ‘ 752    πŸ” 143    πŸ’¬ 6    πŸ“Œ 6

The Awefull Battle of the Pekes and the Pollicles scene was totally unexpected, did not expect a reenactment of the almost war of red squirrels vs grey squirrels, such a fun little piece of meta-theatre .

21.02.2025 11:40 β€” πŸ‘ 2    πŸ” 0    πŸ’¬ 0    πŸ“Œ 0
Preview
11-year-old took her own life over deportation threats, family says β€˜I waited a whole week for a miracle that my daughter would be well, but unfortunately, nothing could be done,’ despaired her mother

An 11-year-old girl took her own life in Texas after she was tormented for weeks by her sixth-grade classmates at Gainesville Intermediate School, who threatened to call ICE authorities and have her family deported from the US, her grieving parents have said. πŸ’” πŸ’”

19.02.2025 23:06 β€” πŸ‘ 5308    πŸ” 2013    πŸ’¬ 661    πŸ“Œ 321

@wkdhellboy is following 20 prominent accounts