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至今,GenScript的服務及產(chǎn)品已被Cell, Nature, Science, PNAS等1300多家生物醫(yī)藥類雜志引用近萬次,處于行業(yè)領先水平。NIH、哈佛、耶魯、斯坦福、普林斯頓、杜克大學等約400家全球著名機構使用GenScript的基因合成、多肽服務、抗體服務和蛋白服務等成功地發(fā)表科研成果,再次證明GenScript 有能力幫助業(yè)內(nèi)科學家Make research easy.

A model of human?neural networks reveals NPTX2?pathology?in ALS and FTLD

Nature. 2024-02; 
Marian Hruska-Plochan,?Vera I Wiersma,?Katharina M Betz,?Izaskun Mallona,?Silvia Ronchi,?Zuzanna Maniecka,?Eva-Maria Hock,?Elena Tantardini,?Florent Laferriere,?Sonu Sahadevan,?Vanessa Hoop,?Igor Delvendahl,?Manuela Pérez-Berlanga,?Beatrice Gatta,?Martina Panatta,?Alexander van der Bourg,?Dasa Bohaciakova,?Puneet Sharma?,?Laura De Vos,?Karl Frontzek?,?Adriano Aguzzi,?Tammaryn Lashley?,?Mark D Robinson,?Theofanis Karayannis,?Martin Mueller,?Andreas Hierlemann?4,?Magdalini Polymenidou?13
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Gene Synthesis To generate lentivirus transfer vectors for constitutive EF‐1α-driven expression of TDP-43–HA (with or without 3′ UTR), NPTX2–HA and HA–FUS; using HiFi Kit, first the EF‐1α?promoter from custom synthetic sequence from GenScript was cloned into mTREAuto-TDP-43–HA vector substituting TRE promoter, generating pLVX-EF‐1α-TDP-43–HA vector Get A Quote

摘要

Human cellular models of neurodegeneration require reproducibility and longevity, which is necessary for simulating age-dependent diseases. Such systems are particularly needed for TDP-43 proteinopathies1, which involve human-specific mechanisms2,3,4,5?that cannot be directly studied in animal models. Here, to explore the emergence and consequences of TDP-43 pathologies, we generated induced pluripotent stem cell-derived, colony morphology neural stem cells (iCoMoNSCs) via manual selection of neural precursors6. Single-cell transcriptomics and comparison to independent neural stem cells7?showed that iCoMoNSCs are uniquely homogenous and self-renewing. Differentiated iCoMoNSCs formed a self-organized multicell... More

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