Reardon Da scite author profile

Reardon Da

3Publications

25Citation Statements Received

61Citation Statements Given

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Affiliations

University of Michigan–Ann Arbor, St. Jude Children's Research Hospital

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Detection of circulating donor white blood cells in patients receiving multiple transfusions

Adams

Davenport

et al. 1992

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Significant morbidities are associated with the routine administration of blood products. Although the exact etiology of these complications may be unknown, many are thought to arise from the incidental cotransfusion of “donor” lymphocytes. We have developed an assay to detect small numbers of male white blood cells (WBCs) circulating in female patients who have received multiple blood transfusions using the polymerase chain reaction (PCR). Twenty female patients undergoing major surgical procedures were studied and received an average of 9.3 U of packed red blood cells (4.8 U from male donors) and 11.7 U of platelets (6.1 U from male donors). DNA was extracted from whole blood or peripheral blood buffy coats posttransfusion and PCR performed using oligonucleotides designed to amplify a segment within the repetitive Y- chromosome DYZ1 locus. Posttransfusion, 15 of 20 women showed evidence of circulating male WBCs for an average of 2.0 days (range, 1 to 6). We conclude that (1) DYZ1 PCR analysis is a useful approach for the detection of small numbers of circulating transfused male WBCs in female patients; and (2) circulating donor WBCs persist for a mean of 2.0 days in the majority of women receiving multiple transfusions. Future application of this technique may detect persisting or proliferating WBCs and lead to an improved understanding of common transfusion-related morbidities.

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Novel therapies for high-grade gliomas: A vision for future

Tandon¹,

Mahapatra²,

Mahapatra³

et al. 2012

IJNS

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The treatment for high-grade glioma remains an enigma. The standard treatment using surgery, radiation therapy and chemotherapy for such highly malignant lesions has only yielded modest results, in terms of survival and improving the quality of life of patients. Less than 10% of such patients survive beyond two years. All conventional therapies have failed to increase the survival beyond this extent. There has been a growing interest in the molecular approaches for the treatment of high-grade gliomas which include gene therapy, oncolytic virotherapy, and immunotherapy. These new therapies are in preclinical and investigational stages. They may not substitute the conventional therapies; they may not be the ultimate elixir for this deadly disease. However, in the coming years, they are likely to have synergistic and complimentary roles alongside conventional therapies. Through this paper, we have attempted to highlight the rationale behind gene therapy which can be used for cytotoxic approaches, immunomodulation strategy, and targeted toxin delivery in the tumor cell. We have reviewed current available literature and through this paper focus on reporting such therapeutic options, their potential usage, benefits and limitations.

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Chromosomal Localization of the Human Smoothened Gene (SMOH) to 7q32.3 by Fluorescencein SituHybridization and Radiation Hybrid Mapping

Sublett

et al. 1998

Genomics

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Reardon Da

Detection of circulating donor white blood cells in patients receiving multiple transfusions

Novel therapies for high-grade gliomas: A vision for future

Chromosomal Localization of the Human Smoothened Gene (SMOH) to 7q32.3 by Fluorescencein SituHybridization and Radiation Hybrid Mapping

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