Danielle M. Shields scite author profile

Danielle M. Shields

4Publications

5Citation Statements Received

152Citation Statements Given

How they've been cited

How they cite others

141

Affiliations

Rutgers, The State University of New Jersey, Carver Bible College, Tuskegee University

Publications

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Stonewalling in the Brick City: Perceptions of and Experiences with Seeking Police Assistance among LGBTQ Citizens

Shields

2021

Social Sciences

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Extant research has documented police interactions between racial and ethnic minority populations, including negative perceptions of and experiences with the police; police corruption and misconduct; and the deleterious effects of negative relationships with the police, such as reduced legitimacy and mistrust. Comparatively, exchanges between lesbian, gay, bisexual, trans, and queer (LGBTQ) populations and the police have received limited attention. This is despite work suggesting that LGBTQ citizens face an elevated risk of victimization, and a possible reticence in reporting their victimization, resulting from negative perceptions of police, fear of mistreatment, or even experiences of harassment and abuse by police. To extend the research in this area, I analyze 12 focus groups with LGBTQ participants (N = 98) in an urban setting to examine the circumstances in which LGBTQ people would seek assistance from the police, when they would avoid doing so, and their justifications for avoiding or contacting the police. I also considered intersectionality in shaping police–citizen interactions between sexual and/or gender minority citizens of color, as the sample was almost exclusively LGBTQ persons of color. I conclude by discussing implications for policing practices and policies.

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Police brutality

Shields¹,

Lewandowski²,

Bumgarner³

2020

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Stonewalling in the Brick City: Perceptions of and Experiences with Seeking Police Assistance among LGBTQ Citizens

Shields¹

2022

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IP‐10 fragment is the functional motif that blocks endothelial cell motility and vessel formation

et al. 2009

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Angiogenesis plays a critical role in optimum healing of a cutaneous wound. It requires well‐orchestrated integration of soluble and matrix factors and timely recognition of such signals to regulate this process. Previous work has shown that endothelial cells express CXC receptor 3 (CXCR3) late in wound regeneration and its ligand IP‐10 (CXCL10) which influences the cells ability to migrate and form vessels in vitro and in vivo resulting in inhibition and regression in the vascular network. To identify the functional domain of IP‐10 to develop new therapeutic agents to promote or inhibit blood vessel formation we isolated a 21 amino acid fragment, residues 78‐98, which we believe is the functional domain, of IP‐10 and analyzed its ability to modulate endothelial cell tube formation. Treatment of the endothelial cells with the IP‐10 fragment significantly inhibited VEGF‐induced endothelial motility and tube formation, a response critical for angiogenesis. Furthermore, simulation of CXCR3 by the IP‐10 fragments induced an increase in cAMP production and activation of PKA that leads to the inhibition of VEGF‐mediated m‐calpain activation and thereby limits cell motility. This activity is embodied in the minimal IP‐10 fragment. We posit that peptide design provides a novel system to provide desired functions of promoting and inhibiting signaling pathways and angiogenesis in human microvascular endothelial cells.

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