Fanying Tang

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Fanying Tang

Fanying Tang

@FanyingTang

Cambridge, MA Beigetreten Ağustos 2017
1.3K Folgt263 Follower
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Elizabeth McKenna
Elizabeth McKenna@ElizSMcKenna·
Now online in @CD_AACR: Machine Learning Predicts Hepatocellular Carcinoma Risk from Routine Clinical Data: A Large Population-Based Multicentric Study - by @JClusmann, @jnkath, @C_V_Schneider, and colleagues @RWTH @tudresden_de
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Cancer Discovery@CD_AACR

Now online: Machine learning predicts hepatocellular carcinoma risk from routine clinical data: a large population-based multicentric study doi.org/10.1158/2159-8…

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Jainam Parmar
Jainam Parmar@aiwithjainam·
BREAKING: Claude can now research like a Stanford PhD student. Here are 9 insane Claude prompts that turn 40+ research papers into structured literature reviews, knowledge maps, and research gaps in minutes (Save this)
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Ming "Tommy" Tang
Ming "Tommy" Tang@tangming2005·
Integration of imaging-based and sequencing-based spatial omics mapping on the same tissue section via DBiTplus nature.com/articles/s4159…
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Ming "Tommy" Tang@tangming2005·
Fragmentomic liquid biopsy enables early breast cancer detection, molecular subtyping and lymph node assessment nature.com/articles/s4146…
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JNM
JNM@JournalofNucMed·
Mutations in certain genes are associated with worse survival outcomes among patients treated with Lu-PSMA; this suggests a role for more intensive surveillance to capture early progression. ow.ly/OXQP50YmVv6 #NuclearMedicine #ProstateCancer @AbbyPepinMD
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Oscar Tahuahua
Oscar Tahuahua@OscarTahuahua·
Retrospective real-world clinicogenomic study in @Nature 5893 pts with mCRPC 37% HRR pathogenic variants. 13% BRCA1/2. 389 received olaparib: BRCA2: median OS 17.5 mo BRCA1: 8.1 mo HR 2.23 (P=0.008) BRCA1 clearly worse. Within BRCA2, subtype defines benefit ⚠️ BRCA2 loss: median OS 24.3 mo HR 0.42 (P<0.001) This is intra-BRCA functional heterogeneity ‼️ Not all BRCA alterations are biologically or therapeutically equivalent. rdcu.be/e6mxn @OncoAlert
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Cancer Discovery
Cancer Discovery@CD_AACR·
Now online: A Circulating GPNMB-Based Multimodal Model Integrates Tumor-Immune Crosstalk to Predict Immunotherapy Response in Esophageal Cancer doi.org/10.1158/2159-8…
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Dr. Jean Fan
Dr. Jean Fan@JEFworks·
Changing training data alone can improve deep learning prediction of spatial transcriptomics gene expression from histology images by 38% (without any changes to model architecture). We've updated our preprint showing this with expanded results: biorxiv.org/content/10.110… 🧵👇 1/4
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Lung Cancer Europe
Lung Cancer Europe@LungCancerEu·
‼️Major step forward for multicancer blood testing. A new Nature Cancer study shows that layering fragment patterns on top of DNA methylation makes these blood tests significantly more accurate. At very high specificity, detection improved from 63% to 77%. #Lungcancer survival depends heavily on stage at diagnosis. Earlier & more accurate detection could be transformative. #LCSM nature.com/articles/s4301…
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𝗿𝗮𝗺𝗮𝗸𝗿𝘂𝘀𝗵𝗻𝗮— 𝗲/𝗮𝗰𝗰
𝗔 𝗧𝗶𝗺𝗲 𝗦𝗲𝗿𝗶𝗲𝘀 𝗙𝗼𝘂𝗻𝗱𝗮𝘁𝗶𝗼𝗻 𝗠𝗼𝗱𝗲𝗹 𝗕𝘆 𝗚𝗼𝗼𝗴𝗹𝗲 This has been pre-trained on a time series corpus of 100 billion data points, & shows impressive performance on various benchmarks from diverse domains. 𝗧𝗶𝗺𝗲𝘀𝗙𝗠 𝗚𝗶𝘁𝗵𝘂𝗯 𝗽𝗮𝗴𝗲: github.com/google-researc… 𝗟𝗲𝗮𝗿𝗻 𝗠𝗟 𝗮𝗻𝗱 𝗙𝗼𝗿𝗲𝗰𝗮𝘀𝘁𝗶𝗻𝗴: leanpub.com/pycaretbook/
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Sadegh Marzban
Sadegh Marzban@S_Marzban·
The Nature Genetics paper is out today (!!) This one is honestly a dream for me. We review and add our perspective on how mathematical & computational modeling can help quantify and predict the evolutionary dynamics of clonal hematopoiesis (CH). nature.com/articles/s4158…
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Dr Rishabh Jain
Dr Rishabh Jain@DrRishabhOnco·
ESMO 2026 reshapes advanced prostate cancer care From de novo mCSPC to molecularly defined mCRPC, treatment is now earlier, intensified, and genotype-driven. 🧬 mCSPC 🟢 Low volume → ADT + ARPI is standard 🟣 High volume → Fit patients: ADT + docetaxel + ARPI (triplet) → Unfit for docetaxel: ADT + ARPI ⚠️ ADT alone is obsolete except in frail patients ❌ Zoledronic acid / denosumab NOT recommended in mCSPC 🧠 Relapsed mCSPC • Low volume: ADT + ARPI • High volume: ADT + ARPI ± docetaxel (selected) 🧬 mCRPC without known mutations • Prior ADT only: ARPI or docetaxel • Post-ARPI: docetaxel or ¹⁷⁷Lu-PSMA-617 • Post-docetaxel + ARPI: ¹⁷⁷Lu-PSMA-617 or cabazitaxel 🧬 mCRPC with genetic alterations • BRCA: PARP inhibitor ± ARPI > chemotherapy • PALB2 / CDK12: selective PARPi use • dMMR: PD-1 / PD-L1 inhibitor early • Aggressive variant / NEPC: platinum-based chemotherapy 🦴 Bone health ✅ All mCRPC with bone mets must receive BPA ❌ Not for mCSPC 💡 Takeaway Earlier intensification. Mandatory genomics. Radioligand therapy mainstream. 🔖 Save this for daily OPD decisions 📖 Full paper in comment ⬇️ #OncoTwitter #MedTwitter #ProstateCancer #GUOncology @OncoAlert @myesmo @esmo_open @asco @Annals_Oncology
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Cancer Cell
Cancer Cell@Cancer_Cell·
Circulating tumor DNA as a biomarker in early phase clinical trials dlvr.it/TQxjNB
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Stephen SIMON
Stephen SIMON@codewithsimon·
If CS224n teaches transformers, CS25 explores where they break and how they evolve. Highly recommended if you already understand the basics. They have an enitire playlist.
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Fanying Tang
Fanying Tang@FanyingTang·
Clonal evolution and transcriptional plasticity shape metastatic dissemination routes in prostate cancer | Nature Communications nature.com/articles/s4146…
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Fabian Theis
Fabian Theis@fabian_theis·
CellRank protocol now in @NatureProtocols! 🎉 @PhilippWeiler's detailed guide shows how to: - Integrate velocity, pseudotime & time points - Infer cell fate probabilities - Analyze lineage priming at scale Great complement to our CellRank 2 paper! 📖 nature.com/articles/s4159…
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Yale Department of Genetics
Yale Department of Genetics@YaleGenetics·
A study proposes combining genetic association data with Perturb-seq to infer causal links from genes to traits through regulatory mechanisms, offering a genome-scale framework to bridge genetic signals and biological function. nature.com/articles/s4158…
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