Persistence of targetable lesions, predicted therapy sensitivity and proteomes through disease evolution in pediatric acute lymphoblastic leukemia

Lorentzian, Amanda; Guo, Meiyun; Ergin, Enes K.; Akella, Neha M.; Rolf, Nina; Lim, C. J.; Reid, Gregor S. D.; Maxwell, Christopher A.; Lange, Philipp F.

doi:10.1101/2022.03.04.22271927

Cited by 2 publications

(3 citation statements)

References 45 publications

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“…Gene ontology enrichment analysis was performed using g:Profiler with an FDR of 5%. A list of pediatric cancer-associated proteins was derived from the sequencing panel used for the genome and transcriptome analyses of pediatric leukemias and solid tumors − as detailed in Lorentzian et al (preprint) . The mass spectrometry proteomics data have been deposited to the ProteomeXchange Consortium via the PRIDE partner repository with the data set identifier PXD036910.…”

Section: Methodsmentioning

confidence: 99%

ASAP─Automated Sonication-Free Acid-Assisted Proteomes─from Cells and FFPE Tissues

et al. 2023

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Formalin-fixed, paraffin-embedded (FFPE) tissues are an invaluable resource for retrospective studies, but protein extraction and subsequent sample processing steps have been shown to be challenging for mass spectrometry (MS) analysis. Streamlined high-throughput sample preparation workflows are essential for efficient peptide extraction from complex clinical specimens such as fresh frozen tissues or FFPE. Overall, proteome analysis has gained significant improvements in the instrumentation, acquisition methods, sample preparation workflows, and analysis pipelines, yet even the most recent FFPE workflows remain complex and are not readily scalable. Here, we present an optimized workflow for automated sonication-free acid-assisted proteome (ASAP) extraction from FFPE sections. ASAP enables efficient protein extraction from FFPE specimens, achieving similar proteome coverage as established methods using expensive sonicators, resulting in reduced sample processing time. The broad applicability of ASAP on archived pediatric tumor FFPE specimens resulted in high-quality data with increased proteome coverage and quantitative reproducibility. Our study demonstrates the practicality and superiority of the ASAP workflow as a streamlined, time- and cost-effective pipeline for high-throughput FFPE proteomics of clinical specimens.

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Section: Methodsmentioning

confidence: 99%

ASAP─Automated Sonication-Free Acid-Assisted Proteomes─from Cells and FFPE Tissues

et al. 2023

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“…1F). Among these, we quantified 154 of a set of 349 cancer-associated proteins that we had previously assembled with a focus on drivers and therapeutic targets in pediatric malignancies (28), confirming comprehensive coverage of the most relevant drivers and pathways (Fig. 1F).…”

Section: Proteomics Reveals Potentially Actionable Targets Of Settlementioning

confidence: 53%

“…This study sets up the basis to implement proteomics into molecular tumor profiling of patients under PROFYLE and other pediatric precision medicine initiatives. Previous retrospective cohort studies have demonstrated that proteome analysis can identify drug targets and contribute to rational treatment choices in pediatric cancers (28,44). Pediatric precision medicine initiatives such as ZERO and INFORM have showcased the application of functional precision oncology during diagnosis for various cancer types, thereby potentially offering more suitable treatment options.…”

Section: Discussionmentioning

confidence: 99%

Proteomics and personalized patient-derived xenograft models identify treatment opportunities for a progressive malignancy within a clinically actionable timeframe and change care

Barnabas,

Bhat,

Goebeler

et al. 2024

Preprint

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Increased access to high-throughput DNA sequencing platforms has transformed the diagnostic landscape of pediatric malignancies by identifying and integrating actionable genomic or transcriptional features that refine diagnosis, classification, and treatment. Yet less than 10% of treated patients show a positive response and translating precision oncology data into feasible and effective therapies for hard-to-cure childhood, adolescent, and young adult malignancies remains a significant challenge. Combining the identification of therapeutic targets at the protein and pathway levels with demonstration of treatment response in personalized models holds great promise. Here we present the case for combining proteomics with patient-derived xenograft (PDX) models to identify personalized treatment options that were not apparent at genomic and transcriptomic levels. Proteome analysis with immunohistochemistry (IHC) validation of formalin-fixed paraffin-embedded sections from an adolescent with primary and metastatic spindle epithelial tumor with thymus-like elements (SETTLE) was completed within two weeks of biopsy.The results identified an elevated protein level of SHMT2 as a possible target for therapy with the commercially available anti-depressant sertraline. Within 2 months and ahead of a molecular tumor board, we confirmed a positive drug response in a personalized chick chorioallantoic membrane (CAM) model of the SETTLE tumor (CAM-PDX). Following the failure of cytotoxic chemotherapy and second-line therapy, a treatment of sertraline was initiated for the patient. After 3 months of sertraline treatment the patient showed decreased tumor growth rates, albeit with clinically progressive disease.Significance: Overall, we demonstrate that proteomics and fast-track personalized xenograft models can provide supportive pre-clinical data in a clinically meaningful timeframe to support medical decision-making and impact the clinical practice. By this we show that proteome-guided and functional precision oncology are feasible and valuable complements to the current genome-driven precision oncology practices.

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Persistence of targetable lesions, predicted therapy sensitivity and proteomes through disease evolution in pediatric acute lymphoblastic leukemia

Cited by 2 publications

References 45 publications

ASAP─Automated Sonication-Free Acid-Assisted Proteomes─from Cells and FFPE Tissues

ASAP─Automated Sonication-Free Acid-Assisted Proteomes─from Cells and FFPE Tissues

Proteomics and personalized patient-derived xenograft models identify treatment opportunities for a progressive malignancy within a clinically actionable timeframe and change care

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