Your search keyword '"Crow, Jennifer"' showing total 22 results

1. National Clinical Guideline for Stroke for the United Kingdom and Ireland: Part I – An overview of the updated recommendations.

Author

Crow, Jennifer and Smith, Alexander

Subjects

ARM physiology, STROKE prognosis, HEALTH services accessibility, STROKE, AFFECT (Psychology), SERIAL publications, CONVALESCENCE, MEDICAL screening, EVIDENCE-based medicine, MEDICAL protocols, OCCUPATIONAL therapy, LABOR supply, PHYSICAL activity, STROKE rehabilitation, INDEPENDENT living, OCCUPATIONAL therapy services, REHABILITATION, WORKING hours, FATIGUE (Physiology), COGNITIVE testing, EMPLOYMENT reentry, MOTOR ability

Abstract

An editorial is presented on marking a new ambition for stroke rehabilitation launched in April 2023. Topics include proposing a raft of recommendations transforming occupational therapy provided to people with stroke and their families; and recommended staffing levels provided for hyperacute, acute and rehabilitation units adjusted to reflect 7days working and the increased intensity of therapy provision in the rehabilitation phase.

Published

2023

2. Lasting impairments following transient ischemic attack and minor stroke: a systematic review protocol.

Author

Ebbesen, Birgitte Hede, Modrau, Boris, Kontou, Eirini, Finch, Emma, Crowfoot, Gary, Crow, Jennifer, Heron, Neil, Hodson, Tenelle, Skrubbeltrang, Conni, and Turner, Grace

Subjects

TRANSIENT ischemic attack, STROKE, SOCIAL anxiety, MEDICAL personnel, SOCIAL participation

Abstract

Introduction: The focus on medical management and secondary prevention following Transient Ischemic Attack (TIA) and minor stroke is well-established. Evidence is emerging that people with TIA and minor stroke can experience lasting impairments as fatigue, depression, anxiety, cognitive impairment, and communication difficulties. These impairments are often underrecognized and inconsistently treated. Research in this area is developing rapidly and an updated systematic review is required to evaluate new evidence as it emerges. This living systematic review aims to describe the prevalence of lasting impairments and how they affect the lives of people with TIA and minor stroke. Furthermore, we will explore whether there are differences in impairments experienced by people with TIA compared to minor stroke. Methods: Systematic searches of PubMed, EMBASE, CINAHL, PsycINFO, Cochrane Libraries will be undertaken. The protocol will follow the Cochrane living systematic review guideline with an update annually. A team of interdisciplinary reviewers will independently screen search results, identify relevant studies based on the defined criteria, conduct quality assessments, and extract data. This systematic review will include quantitative studies on people with TIA and/or minor stroke that report on outcomes in relation to fatigue, cognitive and communication impairments, depression, anxiety, quality of life, return to work/education, or social participation. Where possible, findings will be grouped for TIA and minor stroke and collated according to the time that follow-up occurred (short-term < 3 months, medium-term 3-12 months, and long-term > 12 months). Sub-group analysis on TIA and minor stroke will be performed based on results from the included studies. Data from individual studies will be pooled to perform meta-analysis where possible. Reporting will follow the Preferred Reporting Items for Systematic review and Meta-Analysis Protocol (PRISMA-P) guideline. Perspectives: This living systematic review will collate the latest knowledge on lasting impairments and how these affect the lives of people with TIA and minor stroke. It will seek to guide and support future research on impairments emphasizing distinctions between TIA and minor stroke. Finally, this evidence will allow healthcare professionals to improve follow-up care for people with TIA and minor stroke by supporting them to identify and address lasting impairments. [ABSTRACT FROM AUTHOR]

Published

2023

3. National Clinical Guideline for Stroke for the UK and Ireland: Part ll – The challenges and opportunities posed for occupational therapists.

Author

Crow, Jennifer and Smith, Alexander

Subjects

ARM physiology, OCCUPATIONAL roles, CULTURE, ATTITUDES of medical personnel, FUNCTIONAL status, SERIAL publications, COGNITION, MEDICAL protocols, LABOR supply, PHYSICAL activity, STROKE rehabilitation, WORKING hours, EMPLOYMENT reentry, OCCUPATIONAL therapists

Abstract

An editorial discusses the challenges and opportunities for occupational therapists presented by the new recommendations from the National Clinical Guideline for Stroke (2023). It emphasizes cultural shifts, changes in stroke services, and workforce implications, with specific recommendations for motor recovery, physical effects, and psychological effects of stroke. It further encourages occupational therapists to familiarize themselves with the guidelines.

Published

2023

4. Stroke and TIA Survivors' Perceptions of the COVID-19 Vaccine and Influences on Its Uptake: Cross Sectional Survey.

Author

Turner, Grace M., Heron, Neil, Crow, Jennifer, Kontou, Eirini, and Hughes, Sally

Published

2022

5. MicroRNA Content of Ewing Sarcoma Derived Extracellular Vesicles Leads to Biomarker Potential and Identification of a Previously Undocumented EWS-FLI1 Translocation.

Author

Crow, Jennifer, Samuel, Glenson, Farrow, Emily, Gibson, Margaret, Johnston, Jefferey, Guest, Erin, Miller, Neil, Pei, Dong, Koestler, Devin, Pathak, Harsh, Liang, Xiaobo, Mangels, Cooper, and Godwin, Andrew K

Subjects

EWING'S sarcoma, EXTRACELLULAR vesicles, NON-coding RNA, MICRORNA, BIOMARKERS, CIRCULATING tumor DNA

Abstract

Objective: Ewing Sarcoma Family of Tumors (ESFT) are a highly aggressive pediatric bone and soft tissue malignancy with poor outcomes in the refractory and recurrent setting. Over 90% of Ewing Sarcoma (ES) tumors are driven by the pathognomonic EWS-ETS chimeric transcripts and their corresponding oncoproteins. It has been suggested that the EWS-ETS oncogenic action can mediate microRNA (miRNA) processing. Importantly, small extracellular vesicles (sEVs), including those frequently referred to as exosomes have been shown to be highly enriched with tumor-derived small RNAs such as miRNAs. We hypothesized that ESFT-specific sEVs are enriched with certain miRNAs which could be utilized toward an exo-miRNA biomarker signature specific to this disease. Methods: We performed miRNAseq to compare both the exo-derived and cell-derived miRNA content from 8 ESFT, 2 osteosarcoma, 2 non-cancerous cell lines, and pediatric plasma samples. Results: We found that sEVs derived from ESFT cells contained nearly 2-fold more number of unique individual miRNAs as compared to non-ESFT samples. Quantitative analysis of the differential enrichment of sEV miRNAs resulted in the identification of 62 sEV-miRNAs (exo-miRNAs) with significant (P <.05) enrichment variation between ESFT and non-ESFT sEV samples. To determine if we could utilize this miRNA signature to diagnose ESFT patients via a liquid biopsy, we analyzed the RNA content of total circulating sEVs isolated from 500 µL plasma from 5 pediatric ESFT patients, 2 pediatric osteosarcoma patients, 2 pediatric rhabdomyosarcoma patients, and 4 non-cancer pediatric controls. Pearson's clustering of 60 of the 62 candidate exo-miRNAs correctly identified 80% (4 of 5) of pathology confirmed ESFT patients. Importantly, RNAseq analysis of tumor tissue from the 1 outlier, revealed a previously uncharacterized EWS-FLI1 translocation. Conclusions: Taken together, these findings support the development and validation of an exo-miRNA-based liquid biopsy to aid in the diagnosis and monitoring of ESFT. [ABSTRACT FROM AUTHOR]

Published

2022

6. MicroRNA Content of Ewing Sarcoma Derived Extracellular Vesicles Leads to Biomarker Potential and Identification of a Previously Undocumented EWS-FLI1 Translocation.

Author

Crow, Jennifer, Samuel, Glenson, Farrow, Emily, Gibson, Margaret, Johnston, Jefferey, Guest, Erin, Miller, Neil, Dong Pei, Koestler, Devin, Pathak, Harsh, Xiaobo Liang, Mangels, Cooper, and Godwin, Andrew K.

Subjects

EWING'S sarcoma, EXTRACELLULAR vesicles, MICRORNA, BIOMARKERS, EXOSOMES

Abstract

Objective: Ewing Sarcoma Family of Tumors (ESFT) are a highly aggressive pediatric bone and soft tissue malignancy with poor outcomes in the refractory and recurrent setting. Over 90% of Ewing Sarcoma (ES) tumors are driven by the pathognomonic EWS-ETS chimeric transcripts and their corresponding oncoproteins. It has been suggested that the EWS-ETS oncogenic action can mediate microRNA (miRNA) processing. Importantly, small extracellular vesicles (sEVs), including those frequently referred to as exosomes have been shown to be highly enriched with tumor-derived small RNAs such as miRNAs. We hypothesized that ESFT-specific sEVs are enriched with certain miRNAs which could be utilized toward an exo-miRNA biomarker signature specific to this disease. Methods: We performed miRNAseq to compare both the exo-derived and cell-derived miRNA content from 8 ESFT, 2 osteosarcoma, 2 noncancerous cell lines, and pediatric plasma samples. Results: We found that sEVs derived from ESFT cells contained nearly 2-fold more number of unique individual miRNAs as compared to non-ESFT samples. Quantitative analysis of the differential enrichment of sEV miRNAs resulted in the identification of 62 sEV-miRNAs (exo-miRNAs) with significant (P < .05) enrichment variation between ESFT and non-ESFT sEV samples. To determine if we could utilize this miRNA signature to diagnose ESFT patients via a liquid biopsy, we analyzed the RNA content of total circulating sEVs isolated from 500 µL plasma from 5 pediatric ESFT patients, 2 pediatric osteosarcoma patients, 2 pediatric rhabdomyosarcoma patients, and 4 non-cancer pediatric controls. Pearson's clustering of 60 of the 62 candidate exo-miRNAs correctly identified 80% (4 of 5) of pathology confirmed ESFT patients. Importantly, RNAseq analysis of tumor tissue from the 1 outlier, revealed a previously uncharacterized EWS-FLI1 translocation. Conclusions: Taken together, these findings support the development and validation of an exo-miRNA-based liquid biopsy to aid in the diagnosis and monitoring of ESFT. [ABSTRACT FROM AUTHOR]

Published

2022

7. A qualitative systematic review and thematic synthesis exploring the impacts of clinical academic activity by healthcare professionals outside medicine.

Author

Newington, Lisa, Wells, Mary, Adonis, Adine, Bolton, Lee, Bolton Saghdaoui, Layla, Coffey, Margaret, Crow, Jennifer, Fadeeva Costa, Olga, Hughes, Catherine, Savage, Matthew, Shahabi, Lillie, and Alexander, Caroline M.

Subjects

MEDICAL personnel, WEB search engines, GREY literature, INFORMATION sharing

Abstract

Background: There are increasing opportunities for healthcare professionals outside medicine to be involved in and lead clinical research. However, there are few roles within these professions that include time for research. In order to develop such roles, and evaluate effective use of this time, the range of impacts of this clinical academic activity need to be valued and understood by healthcare leaders and managers. To date, these impacts have not been comprehensively explored, but are suggested to extend beyond traditional quantitative impact metrics, such as publications, citations and funding awards.Methods: Ten databases, four grey literature repositories and a naïve web search engine were systematically searched for articles reporting impacts of clinical academic activity by healthcare professionals outside medicine. Specifically, this did not include the direct impacts of the research findings, rather the impacts of the research activity. All stages of the review were performed by a minimum of two reviewers and reported impacts were categorised qualitatively according to a modified VICTOR (making Visible the ImpaCT Of Research) framework.Results: Of the initial 2704 identified articles, 20 were eligible for inclusion. Identified impacts were mapped to seven themes: impacts for patients; impacts for the service provision and workforce; impacts to research profile, culture and capacity; economic impacts; impacts on staff recruitment and retention; impacts to knowledge exchange; and impacts to the clinical academic.Conclusions: Several overlapping sub-themes were identified across the main themes. These included the challenges and benefits of balancing clinical and academic roles, the creation and implementation of new evidence, and the development of collaborations and networks. These may be key areas for organisations to explore when looking to support and increase academic activity among healthcare professionals outside medicine. The modified VICTOR tool is a useful starting point for individuals and organisations to record the impact of their research activity. Further work is needed to explore standardised methods of capturing research impact that address the full range of impacts identified in this systematic review and are specific to the context of clinical academics outside medicine. [ABSTRACT FROM AUTHOR]

Published

2021

8. Beyond tumor mutational burden: potential and limitations in using exosomes to predict response to immunotherapy.

Author

Crow, Jennifer, Samuel, Glenson, and Godwin, Andrew K.

Abstract

Introduction: Immune checkpoint blockade (ICB) has ushered in a new era of cancer therapeutics. The standard for determining which patients might benefit from ICB-based therapies is through the assessment of tumor mutational burden using formalin-fixed paraffin-embedded (FFPE) tumor tissue samples; however, this strategy is imperfect. The discovery of exosomal PD-L1 has placed these nano-vesicles to the forefront of immunotherapy biomarker development. Exosomes and other extracellular vesicles contain proteins and nucleic acids specific to their cell of origin and their production is increased in disease state such as cancer and can be isolated from most types of liquid biopsy. Given this opportunity, a large-scale bioengineering effort has centered on developing technologies capable of isolating distinct subsets of exosomes and interrogating their content for biomarker discovery. Areas covered: This review investigates the current state of small extracellular vesicles (sEVs), focusing on exosomes, as they relate to biomarkers of IBC. We will discuss technologies being developed to both capture and evaluate exosomal cargo and as some of the challenges they face. Expert opinion: The advancement of microfluidic technologies, along with rapidly evolving methodologies in RNAseq and proteomics, are making the potential of utilizing exosomes as prognostic and diagnostic biomarkers of ICB into a likely reality. [ABSTRACT FROM AUTHOR]

Published

2019

9. Targeted inhibition of histone deacetylase leads to suppression of Ewing sarcoma tumor growth through an unappreciated EWS-FLI1/HDAC3/HSP90 signaling axis.

Author

Ma, Yan, Baltezor, Michael, Rajewski, Lian, Crow, Jennifer, Samuel, Glenson, Staggs, Vincent S., Chastain, Katherine M., Toretsky, Jeffrey A., Weir, Scott J., and Godwin, Andrew K.

Subjects

HISTONE deacetylase, TUMOR growth, SOFT tissue tumors, SARCOMA, THERAPEUTICS, CELL cycle

Abstract

Ewing sarcoma (ES) are aggressive pediatric bone and soft tissue tumors driven by EWS-ETS fusion oncogenes, most commonly EWS-FLI1. Treatment of ES patients consists of up to 9 months of alternating courses of 2 chemotherapeutic regimens. Furthermore, EWS-ETS-targeted therapies have yet to demonstrate clinical benefit, thereby emphasizing a clinical responsibility to search for new therapeutic approaches. Our previous in silico drug screening identified entinostat as a drug hit that was predicted to reverse the ES disease signatures and EWS-FLI1-mediated gene signatures. Here, we establish preclinical proof of principle by investigating the in vitro and in vivo efficacy of entinostat in preclinical ES models, as well as characterizing the mechanisms of action and in vivo pharmacokinetics of entinostat. ES cells are preferentially sensitive to entinostat in an EWS-FLI1 or EWS-ERG-dependent manner. Entinostat induces apoptosis of ES cells through G0/G1 cell cycle arrest, intracellular reactive oxygen species (ROS) elevation, DNA damage, homologous recombination (HR) repair impairment, and caspase activation. Mechanistically, we demonstrate for the first time that HDAC3 is a transcriptional target of EWS-FLI1 and that entinostat inhibits growth of ES cells through suppressing a previously unexplored EWS-FLI1/HDAC3/HSP90 signaling axis. Importantly, entinostat significantly reduces tumor burden by 97.4% (89.5 vs. 3397.3 mm3 of vehicle, p < 0.001) and prolongs the median survival of mice (15.5 vs. 8.5 days of vehicle, p < 0.001), in two independent ES xenograft mouse models, respectively. Overall, our studies demonstrate promising activity of entinostat against ES, and support the clinical development of the entinostat-based therapies for children and young adults with metastatic/relapsed ES. Key messages: • Entinostat potently inhibits ES both in vitro and in vivo. • EWS-FLI1 and EWS-ERG confer sensitivity to entinostat treatment. • Entinostat suppresses the EWS-FLI1/HDAC3/HSP90 signaling. • HDAC3 is a transcriptional target of EWS-FLI1. • HDAC3 is essential for ES cell viability and genomic stability maintenance. [ABSTRACT FROM AUTHOR]

Published

2019

10. Hanged Men.

Author

Crow, Jennifer

Published

2024

11. Ultrasensitive quantification of tumor mRNAs in extracellular vesicles with an integrated microfluidic digital analysis chip.

Author

Zhang, Peng, Crow, Jennifer, Lella, Divya, Zhou, Xin, Samuel, Glenson, Godwin, Andrew K., and Zeng, Yong

Subjects

MICRORNA, VESICLES (Cytology), MICROFLUIDICS, POLYMERASE chain reaction, NUCLEIC acid hybridization

Abstract

Extracellular vesicles (EVs) present a promising liquid biopsy for cancer diagnosis. However, it remains a daunting challenge to quantitatively measure molecular contents of EVs including tumor-associated mRNAs. Herein, we report a configurable microwell-patterned microfluidic digital analysis platform combined with a dual-probe hybridization assay for PCR-free, single-molecule detection of specific mRNAs in EVs. The microwell array in our device is configurable between the flow-through assay mode for enhanced hybridization capture and tagging of mRNAs and the digital detection mode based on femtoliter-scale enzymatic signal amplification for single-molecule counting of surface-bound targets. Furthermore, a dual-probe hybridization assay has been developed to enhance the sensitivity of the digital single-molecule detection of EV mRNAs. Combining the merits of the chip design and the dual-probe digital mRNA hybridization assay, the integrated microfluidic system has been demonstrated to afford quantitative detection of synthetic GAPDH mRNA with a LOD as low as 20 aM. Using this technology, we quantified the level of GAPDH and EWS-FLI1 mRNAs in EVs derived from two cell lines of peripheral primitive neuroectodermal tumor (PNET), CHLA-9 and CHLA-258. Our measurements detected 64.6 and 43.5 copies of GAPDH mRNA and 6.5 and 0.277 copies of EWS-FLI1 fusion transcripts per 105 EVs derived from CHLA-9 and CHLA-258 cells, respectively. To our knowledge, this is the first demonstration of quantitative measurement of EWS-FLI1 mRNA copy numbers in Ewing Sarcoma (EWS)-derived EVs. These results highlight the ultralow frequency of tumor-specific mRNA markers in EVs and the necessity of developing highly sensitive methods for analysis of EV mRNAs. The microfluidic digital mRNA analysis platform presented here would provide a useful tool to facilitate quantitative analysis of tumor-associated EV mRNAs for liquid biopsy-based cancer diagnosis and monitoring. [ABSTRACT FROM AUTHOR]

Published

2018

12. A 2-week stroke review identifies unmet needs in patients discharged home from a hyperacute stroke unit.

Author

Crow, Jennifer

Abstract

Patients assessed as having made a full recovery following their stroke are discharged home within 72 hours of admission from the hyper-acute stroke unit (HASU). An onward referral is made to those boroughs offering a 6-month review. Patient feedback revealed that those assessed as not needing any further input on discharge may experience difficulties when back in the community, and accessing appropriate services can be difficult. In this pilot project, 21 patients were reviewed 2 weeks after discharge by a stroke support worker (SSW) using the post-stroke checklist (PSC). The data revealed that 11 of the 21 participants identified unmet needs. The domains of mood and information about stroke prevention had the highest unmet needs. This project raises questions about the assessment processes and education provided on the HASU, and demonstrates the need for joined-up working between acute and community organisations to ensure stroke survivors are able to access ongoing support, information and advice. [ABSTRACT FROM AUTHOR]

Published

2018

13. A Catalog of Shade.

Author

Crow, Jennifer

Subjects

CATALOG of Shade, A (Poem), CROW, Jennifer

Abstract

The poem "A Catalog of Shade" by Jennifer Crow is presented. First Line: We lift our palms to the light, new green cells; Last Line: more truly siblings with every bite.

Published

2023

14. Blast Phase in Chronic Myelogenous Leukemia Is Skewed Toward Unusual Blast Types in Patients Treated With Tyrosine Kinase Inhibitors.

Author

Yang Shi, Rand, Andrew J., Crow, Jennifer H., Moore, Joseph O., and Lagoo, Anand S.

Subjects

CHRONIC myeloid leukemia, CHRONIC leukemia, MYELOID leukemia, PROTEIN-tyrosine kinases, PROTEIN kinases

Abstract

Objectives: To compare the features of the blast phase of chronic myelogenous leukemia (CML) in patients treated with tyrosine kinase inhibitors (TKIs) with those in the pre-TKI era. Methods: Sixty-seven patients with blast phase CML were identified in the Duke Pathology database from 1991 to 2011. The morphology and immunophenotype of blasts were evaluated, along with cytogenetic studies and associated findings in the peripheral blood and bone marrow. Results: In the TKI era, the blasts were more frequently of a type other than the usual myeloid or lymphoid types when compared with the pre-TKI era. Blast phase in TKI-treated patients was associated with a higher peripheral WBC count and a lower blast percentage in the bone marrow. Of the 23 patients with cytogenetic studies during blast phase, additional cytogenetic changes more frequently occurred in patients with an unusual blast type, and some patients showed these changes months before the onset of blast phase. Conclusions: Blast phase CML in TKI- and non-TKI-treated patients differs in the morphology and immunophenotype of blasts, cytogenetic findings, and associated findings in the peripheral blood and bone marrow. [ABSTRACT FROM AUTHOR]

Published

2015

15. Integrated immunoisolation and protein analysis of circulating exosomes using microfluidic technology.

Author

He, Mei, Crow, Jennifer, Roth, Marc, Zeng, Yong, and Godwin, Andrew K.

Subjects

EXOSOMES, VESICLES (Cytology), ORGANELLES, AUTOPHAGY, COATED vesicles

Abstract

Developing blood-based tests is appealing for non-invasive disease diagnosis, especially when biopsy is difficult, costly, and sometimes not even an option. Tumor-derived exosomes have attracted increasing interest in non-invasive cancer diagnosis and monitoring of treatment response. However, the biology and clinical value of exosomes remains largely unknown due in part to current technical challenges in rapid isolation, molecular classification and comprehensive analysis of exosomes. Here we developed a new microfluidic approach to streamline and expedite the exosome analysis pipeline by integrating specific immunoisolation and targeted protein analysis of circulating exosomes. Compared to the conventional methods, our approach enables selective subpopulation isolation and quantitative detection of surface and intravesicular biomarkers directly from a minimally invasive amount of plasma samples (30 μL) within ~100 min with markedly improved detection sensitivity. Using this device, we demonstrated phenotyping of exosome subpopulations by targeting a panel of common exosomal and tumor-specific markers and multiparameter analyses of intravesicular biomarkers in the selected subpopulation. We were able to assess the total expression and phosphorylation levels of IGF-1R in non-small-cell lung cancer patients by probing plasma exosomes as a non-invasive alternative to conventional tissue biopsy. We foresee that the microfluidic exosome analysis platform will form the basis for critically needed infrastructures for advancing the biology and clinical utilization of exosomes. [ABSTRACT FROM AUTHOR]

Published

2014

16. Oncogenic KIT-containing exosomes increase gastrointestinal stromal tumor cell invasion.

Author

Atay, Safinur, Banskota, Samagya, Crow, Jennifer, Sethi, Geetika, Rink, Iori, and Godwin, Andrew K.

Subjects

GASTROINTESTINAL stromal tumors, STROMAL cells, EXOSOMES, ONCOGENIC proteins, PROTEIN-tyrosine kinases, MUSCLE cells, EXTRACELLULAR matrix

Abstract

During tumor development, constant interplay occurs between tumor cells and surrounding stromal cells. We report evidence that gastrointestinal stromal tumor (GIST) cells invade the interstitial stroma through the release of the oncogenic protein tyrosine kinase (KIT)-containing exosomes, which triggers the phenotypic conversion of progenitor smooth muscle cells to tumor-promoting cells. These recipient cells display morphologic changes and acquire tumor-associated phenotypes, including enhanced adhesion to extracellular matrix proteins, activation of intracellular pathways downstream of KIT, expression of Interstitial Cell of Cajal–like markers, and release of various matrix metal- loproteinases (MMPs), particularly MMP1. This report shows stimulation of MMP1 production by stromal cells via uptake of tumor-derived exosomes, which leads to tumor cell invasion. Exosomes derived from GIST patients but not healthy donors show enhanced MMP1 secretion by smooth muscle cells and tumor cell invasion, whereas selective blocking of exosome-mediated MMP1 secretion decreases tumor invasiveness. Our study indicates that exosome release and subsequent MMP1 induction creates a positive feedback mechanism established between tumor and stromal cells that drives GIST development and offers unique insights for potential therapeutic strategies to block GIST progression and metastatic spread. [ABSTRACT FROM AUTHOR]

Published

2014

17. Epimorphin-Induced MET Sensitizes Ovarian Cancer Cells to Platinum.

Author

Yew, Kok-Hooi, Crow, Jennifer, Hirst, Jeff, Pressetto, Ziyan, and Godwin, Andrew K.

Subjects

OVARIAN cancer, CANCER cells, PLATINUM, EPITHELIAL cells, DRUG resistance in cancer cells, DISEASE relapse, CANCER chemotherapy

Abstract

Distinctive genotypic and phenotypic features of ovarian cancer via epithelial-mesenchymal transition (EMT) have been correlated with drug resistance and disease recurrence. We investigated whether therapeutic reversal of EMT could re-sensitize ovarian cancer cells (OCCs) to existing chemotherapy. We report that epimorphin, a morphogenic protein, has pivotal control over mesenchymal versus epithelial cell lineage decision of the putative OCCs. Exposure to epimorphin induced morphological changes reminiscent of mesenchymal-to-epithelial transition (MET), but in a dose dependent manner, i.e., at 10 µg/mL of epimorphin cells obtain a more mesenchymal-like morphology while at 20 µg/mL of epimorphin cells display an epithelial morphology. The latter changes were accompanied by suppression of mesenchymal markers, such as vimentin (∼8-fold↓, p<0.02), Twist1 (∼7-fold↓, p<0.03), dystroglycan (∼4-fold↓, p<0.01) and palladin (∼3-fold↓, p<0.01). Conversely, significant elevations of KLF4 (∼28-fold↑, p<0.002), β-catenin (∼6-fold↑, p<0.004), EpCAM (∼6-fold↑, p<0.0002) and occludin (∼15-fold↑, p<0.004) mRNAs as part of the commitment to the epithelial cell lineage were detected in response to 20 µg/mL of exogenous epimorphin. Changes in occludin mRNA levels were accompanied by a parallel, albeit weaker expression at the protein level (∼5-fold↑, p<0.001). Likewise, acquisition of epithelial-like properties, including mucin1, CK19, and β-catenin gene expression, was also obtained following epimorphin treatment. Further, MMP3 production was found to be reduced whereas laminin secretion was strongly amplified upon epimorphin-induced MET. These results suggest there is a dosage window for actions of epimorphin on cellular differentiation, wherein it can either suppress or enhance epithelial differentiation of OCCs. Importantly, induction of epithelial-like phenotypes by epimorphin led to an enhanced sensitivity to carboplatin. Overall, we demonstrate that epimorphin can revert OCCs away from their mesenchymal phenotype and toward an epithelial phenotype, thereby enhancing their sensitivity to a front-line chemotherapeutic agent. [ABSTRACT FROM AUTHOR]

Published

2013

18. Donor Cell--Derived Leukemias/Myelodysplastic Neoplasms in Allogeneic Hematopoietic Stem Cell Transplant Recipients.

Author

Endi Wang, Hutchinson, Charles Blake, Qin Huang, Lu, Chuanyi Mark, Crow, Jennifer, Wang, Frances F., Sebastian, Siby, Rehder, Catherine, Lagoo, Anand, Horwitz, Mitchell, Rizzieri, David, Jingwei Yu, Goodman, Barbara, Datto, Michael, and Buckley, Patrick

Subjects

LEUKEMIA, ORGAN donation, MYELODYSPLASTIC syndromes, HEMATOPOIETIC stem cell transplantation, ANEMIA, NEUTROPENIA

Abstract

We report 10 cases of donor cell leukemia (DCL). All cases except the case of chronic lymphocytic leukemia had anemia, neutropenia, and/ or thrombocytopenia when DCL was diagnosed. Eight cases with sex-mismatched hematopoietic stem cell transplant (HCT) showed donor gonosomal complements, suggesting DCL. Clonal cytogenetic abnormalities were detected in 8 cases: 6 were monosomy 7/del(7q). In all 10 cases, engraftment studies confirmed donor cell origin. Retrospective fluorescence in situ hybridization in archived donor cells in 4 cases showed a low level of abnormalities in 2. Of 7 patients with clinical follow-up of 5 months or more, 1 (with acute myeloid leukemia) died of disease; 6 are alive, including 1 with myelodysplastic syndrome with spontaneous remission. Similar to reported cases, we found disproportional sex-mismatched HCTs, suggesting probable underdetection of DCL in sex-matched HCTs. The latency between HCT and DCL ranged from 1 to 193 months (median, 24 months), in keeping with the literature. Analyzing our cases, pooled with reported cases, with survival models showed much shorter latency for malignancy as primary disease, for T-cell large granular lymphocyte leukemia as type of DCL, and for umbilical cord blood as stem cell source. [ABSTRACT FROM AUTHOR]

Published

2011

19. A clinical prediction tool to estimate the number of units of red blood cells needed in primary elective coronary artery bypass surgery

Author

Welsby, Ian, Crow, Jennifer, Bandarenko, Nicholas, Lappas, George, Phillips-Bute, Barbara, and Stafford-Smith, Mark

Subjects

RED blood cell transfusion, CARDIAC surgery, CORONARY artery bypass, BLOOD transfusion, MYOCARDIAL revascularization, MULTIVARIATE analysis

Abstract

Red blood cell (RBC) transfusion is common during cardiac surgical procedures. Empiric crossmatching, without attempting to estimate individual transfusion requirements is typical. We hypothesized that a clinical prediction tool could be developed to estimate the number of units of RBCs needed for coronary artery bypass grafting (CABG) surgery. With institutional review board approval, detailed demographic, risk factor, and transfusion data of primary elective CABG procedures (n = 5887) from September 1, 1993, to June 20, 2002, were studied and the data set was divided into development and validation subgroups. Multivariable ordinal logistic regression was used to develop and validate transfusion risk factors, assign them a relative weight, and create a model to stratify patients into groups depending on predicted need for 0, 2, 4, or more than 4 RBC units. The model was compared with current standard practice of crossmatching 4 RBC units in terms of observed blood product usage over the study period. Demographic and transfusion risk factor variables in the development (n = 3876) and validation (n = 2011) data sets were similar. The predictive value of the model was good for the development and validation groups, with a c-index of 0.79 and 0.78, respectively. Applying the predictive model reduced the number of crossmatches by 30% without underproviding RBC units and increased the percentage of patients crossmatched exactly for the required number of units from 11% to 21%. Predictive factors for RBC transfusion were identified and used to construct a clinical tool to conserve blood bank resources without increasing patient risk. [ABSTRACT FROM AUTHOR]

Published

2010

20. Exhibition review.

Author

Crow, Jennifer Fields

Subjects

EXHIBITIONS

Abstract

Reviews the exhibitions `Sir William Chambers: Architect to George III,' edited by John Harris and Michael Snodin, and `Houghton Hall: The Prime Minister, The Empress and The Heritage,' edited by Andrew Moore.

Published

1997

21. Across a Storm-Dark Sky.

Author

Crow, Jennifer

Subjects

ACROSS a Storm-Dark Sky (Poem), CROW, Jennifer

Abstract

The poem "Across a Storm-Dark Sky," by Jennifer Crow is presented. First Line: You saw a dragon, etched like fire; Last Line: to catch another glimpse.

Published

2016

22. Correlation of Treg Prevalence and Function in Head and Neck Melanoma SLNs to Clinical Outcome.

Author

Ryan, Marisa A., Crow, Jennifer, Fisher, Samuel R., Lee, Walter T., and Proia, Alan

Published

2013