Danielle Soldin scite author profile

Danielle Soldin

5Publications

63Citation Statements Received

150Citation Statements Given

How they've been cited

How they cite others

128

Affiliations

University of Maryland, Baltimore, Georgetown University

Publications

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Distinct Adsorption Configurations and Self-Assembly Characteristics of Fibrinogen on Chemically Uniform and Alternating Surfaces including Block Copolymer Nanodomains

et al. 2014

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Understanding protein–surface interactions is crucial to solid-state biomedical applications whose functionality is directly correlated with the precise control of the adsorption configuration, surface packing, loading density, and bioactivity of protein molecules. Because of the small dimensions and highly amphiphilic nature of proteins, investigation of protein adsorption performed on nanoscale topology can shed light on subprotein-level interaction preferences. In this study, we examine the adsorption and assembly behavior of a highly elongated protein, fibrinogen, on both chemically uniform (as-is and buffered HF-treated SiO2/Si, and homopolymers of polystyrene and poly(methyl methacrylate)) and varying (polystyrene-block-poly(methyl methacrylate)) surfaces. By focusing on high-resolution imaging of individual protein molecules whose configurations are influenced by protein–surface rather than protein–protein interactions, fibrinogen conformations characteristic to each surface are identified and statistically analyzed for structural similarities/differences in key protein domains. By exploiting block copolymer nanodomains whose repeat distance is commensurate with the length of the individual protein, we determine that fibrinogen exhibits a more neutral tendency for interaction with both polystyrene and poly(methyl methacrylate) blocks relative to the case of common globular proteins. Factors affecting fibrinogen–polymer interactions are discussed in terms of hydrophobic and electrostatic interactions. In addition, assembly and packing attributes of fibrinogen are determined at different loading conditions. Primary orientations of fibrinogen and its rearrangements with respect to the underlying diblock nanodomains associated with different surface coverage are explained by pertinent protein interaction mechanisms. On the basis of two-dimensional stacking behavior, a protein assembly model is proposed for the formation of an extended fibrinogen network on the diblock copolymer.

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A Case of Acute Myeloid Leukemia-Associated Necrotizing Sweet Syndrome

et al. 2022

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Sweet syndrome (SS), or acute febrile neutrophilic dermatosis, is a rare painful skin condition that is characterized by hyperpyrexia, peripheral blood and skin neutrophilia, and edematous skin lesions. Necrotizing SS (NSS) is a severe and locally aggressive condition that histopathologically resembles a necrotizing soft tissue infection. As opposed to necrotizing soft tissue infections, NSS responds to systemic steroids. SS is divided into three subtypes: classical SS, malignancy-associated SS, and drug-induced SS. Within the malignancy-associated SS subtype, both solid tumor and hematologic malignancies have been precursors to developing SS. Here, we present a case of acute myeloid leukemia-associated NSS.

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Dexamethasone and Baracitinib: A Recipe for HSV Reactivation in Covid-19 Treatment

Soldin

Grier

Bowers

et al. 2022

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Left ventricular systolic dysfunction during acute pulmonary embolism

Cires-Drouet

LaRocco

Soldin

et al. 2023

Thrombosis Research

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Screening Beyond the Nodule: Annual LDCT as a Screening Tool for Other Comorbid Conditions

Herring

Park

Hossain

et al. 2023

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Danielle Soldin

Distinct Adsorption Configurations and Self-Assembly Characteristics of Fibrinogen on Chemically Uniform and Alternating Surfaces including Block Copolymer Nanodomains

A Case of Acute Myeloid Leukemia-Associated Necrotizing Sweet Syndrome

Dexamethasone and Baracitinib: A Recipe for HSV Reactivation in Covid-19 Treatment

Left ventricular systolic dysfunction during acute pulmonary embolism

Screening Beyond the Nodule: Annual LDCT as a Screening Tool for Other Comorbid Conditions

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