Jacqueline C. Simonet scite author profile

Mesothelin is a cell-surface molecule over-expressed on a large fraction of carcinomas, and thus is an attractive target of immunotherapy. A molecularly targeted therapy for these cancers was created by engineering T cells to express a chimeric receptor with high affinity for human mesothelin. Lentiviral vectors were used to express a single-chain variable fragment that binds mesothelin and that is fused to signaling domains derived from T-cell receptor zeta, CD28, and CD137 (

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Reconstituted IMPDH polymers accommodate both catalytically active and inactive conformations

Anthony

Burrell

Johnson

et al. 2017

MBoC

142

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IMPDH1 retinal variants control filament architecture to tune allosteric regulation

Burrell

Nie

Said

et al. 2022

Nat Struct Mol Biol

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Osterix/Sp7 limits cranial bone initiation sites and is required for formation of sutures

Kague

Roy

Asselin

et al. 2016

Developmental Biology

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During growth, individual skull bones overlap at sutures, where osteoblast differentiation and bone deposition occur. Mutations causing skull malformations have revealed some required genes, but many aspects of suture regulation remain poorly understood. We describe a zebrafish mutation in osterix/sp7, which causes a generalized delay in osteoblast maturation. While most of the skeleton is patterned normally, mutants have specific defects in the anterior skull and upper jaw, and the top of the skull comprises a random mosaic of bones derived from individual initiation sites. Osteoblasts at the edges of the bones are highly proliferative and fail to differentiate, consistent with global changes in gene expression. We propose that signals from the bone itself are required for orderly recruitment of precursor cells and growth along the edges. The delay in bone maturation caused by loss of Sp7 leads to unregulated bone formation, revealing a new mechanism for patterning the skull and sutures.

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