Kelli M. Bullard scite author profile

The early-gestation fetus heals dermal wounds rapidly and scarlessly. This phenomenon appears to be intrinsic to fetal skin and independent of the intrauterine environment. Unique properties of fetal cells, extracellular matrix, cytokine profile, and gene expression contribute to scarless repair. An intensive research effort has focused on unraveling the mechanisms that underlie scarless fetal wound healing in an attempt to improve the quality of healing in both children and adults.

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Impaired Wound Contraction in Stromelysin-1–Deficient Mice

Bullard

Lund²,

Mudgett³

et al. 1999

Annals of Surgery

201

148

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Surgical Therapy for Anorectal Melanoma

et al. 2003

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Correction of congenital diaphragmatic hernia in utero VII: A prospective trial

Harrison

Adzick

Bullard

et al. 1997

Journal of Pediatric Surgery

253

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Wound size and gestational age modulate scar formation in fetal wound repair

Cass

Bullard

Sylvester

et al. 1997

Journal of Pediatric Surgery

129

103

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Hyaluronan Facilitates Invasion of Colon Carcinoma Cells in Vitro via Interaction with CD44

Kim¹,

Wheeler²,

Wilson

et al. 2004

117

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Hyaluronan (HA) and its biosynthetic enzymes, HA synthases (HAS1, 2, and 3) are thought to participate in cancer progression. We have shown previously that HA production and HAS3 expression are increased in metastatic colon carcinoma cells (SW620) when compared with cells isolated from a primary tumor (SW480). Because invasion of the extracellular matrix is a fundamental event in tumor growth and metastasis, we hypothesized that SW620 cells would show greater invasive capability than SW480 cells, that invasion is HA dependent, and that HA mediates invasion via interaction with a cell-surface receptor. Invasion into artificial basement membrane (Matrigel) was assessed in vitro. To assess HA functionality, HAS expression was inhibited in SW620 cells by transfection with antisense HAS constructs. Decreased HA secretion and retention in the transfectants were confirmed using competitive binding and particle exclusion assays. SW620 cells demonstrated greater invasion through Matrigel than did SW480 cells. Antisense transfection decreased Matrigel invasion by SW620 cells by >60%; addition of exogenous HA restored invasion. Because the cell-surface HA receptor CD44 has been implicated in cancer progression, HA-CD44 interaction was then inhibited by incubation with an anti-CD44 antibody. Anti-CD44 antibody impaired invasion into Matrigel by 95%. Taken together, these data suggest that pericellular HA is critical for colon carcinoma cell invasion and that this invasive capability is dependent on interaction with CD44.

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Salvage abdominoperineal resection after failed Nigro protocol: modest success, major morbidity

et al. 2006

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Kelli M. Bullard

Primary Perineal Wound Closure After Preoperative Radiotherapy and Abdominoperineal Resection has a High Incidence of Wound Failure

Fetal Wound Healing: Current Biology

Impaired Wound Contraction in Stromelysin-1–Deficient Mice

Surgical Therapy for Anorectal Melanoma

Correction of congenital diaphragmatic hernia in utero VII: A prospective trial

Wound size and gestational age modulate scar formation in fetal wound repair

Hyaluronan Facilitates Invasion of Colon Carcinoma Cells in Vitro via Interaction with CD44

Salvage abdominoperineal resection after failed Nigro protocol: modest success, major morbidity

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