Kristin Anderson scite author profile

The body's response to tissue injury in a healthy individual is an intricate, sequential physiologic process that results in timely healing with full re-epithelialization, resolution of drainage, and return of function to the affected tissue. Chronic wounds, however, do not follow this sequence of events and can challenge the most experienced clinician if the underlying factors that are impairing wound healing are not identified. The purpose of this article is to present recent information about factors that impair wound healing with the underlying pathophysiological mechanism that interferes with the response to tissue injury. These factors include co-morbidities (diabetes, obesity, protein energy malnutrition), medications (steroids, non-steroidal anti-inflammatory drugs or NSAIDs, anti-rejection medications), oncology interventions (radiation, chemotherapy), and life style habits (smoking, alcohol abuse). Successful treatment of any chronic wound depends upon identification and management of the factors for each individual.

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Family history of breast and ovarian cancer and triple negative subtype in hispanic/latina women

Anderson

Thompson

Wertheim

et al. 2014

SpringerPlus

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Familial breast and ovarian cancer prevalence was assessed among 1150 women of Mexican descent enrolled in a case-only, binational breast cancer study. Logistic regression was conducted to compare odds of triple negative breast cancer (TNBC) to non-TNBC according to family history of breast and breast or ovarian cancer among 914 of these women.Prevalence of breast cancer family history in a first- and first- or second-degree relative was 13.1% and 24.1%, respectively; that for breast or ovarian cancer in a first-degree relative was 14.9%. After adjustment for age and country of residence, women with a first-degree relative with breast cancer were more likely to be diagnosed with TNBC than non-TNBC (OR=1.98; 95% CI, 1.26–3.11). The odds of TNBC compared to non-TNBC were 1.93 (95% CI, 1.26–2.97) for women with a first-degree relative with breast or ovarian cancer. There were non-significant stronger associations between family history and TNBC among women diagnosed at age <50 compared to ≥50 years for breast cancer in a first-degree relative (P-interaction = 0.14) and a first- or second-degree relative (P-interaction = 0.07).Findings suggest that familial breast cancers are associated with triple negative subtype, possibly related to BRCA mutations in Hispanic/Latina women, which are strongly associated with TNBC. Family history is an important tool to identify Hispanic/Latina women who may be at increased risk of TNBC, and could benefit from prevention and early detection strategies.Electronic supplementary materialThe online version of this article (doi:10.1186/2193-1801-3-727) contains supplementary material, which is available to authorized users.

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Heterozygous congenital Factor VII deficiency with the 9729del4 mutation, associated with severe spontaneous intracranial bleeding in an adolescent male

Cramer

Anderson

Navaz

et al. 2016

Blood Cells, Molecules, and Diseases

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Background In congenital Factor (F) VII deficiency bleeding phenotype and intrinsic FVII activity levels don’t always correlate. Patients with FVII activity levels <30% appear to have a higher bleeding propensity, but bleeding can also occur at higher FVII activity levels. Reasons for bleeding at higher FVII activity levels are unknown, and it remains challenging to manage such patients clinically. Case A 19 year old male with spontaneous intracranial hemorrhage and FVII activity levels of 44%, requiring emergent surgical intervention and a strategy for FVII replacement. Genotyping showed the rare heterozygous FVII 9729del4 mutation. Bleed evacuation was complicated by epidural abscess requiring craniectomy, bone graft procedures, and prolonged administration of recombinant human (rh) activated FVII (FVIIa). The patient recovered without neurological deficits, and remains on prophylactic low dose treatment with rhFVIIa in relation to risky athletic activities. Conclusion For clinicians, it is important to recognize that effects of rhFVIIa within these pathways are independent of its contribution to blood clot formation and cannot be assessed by clotting assays. Reduced FVII levels should therefore not be dismissed, as even a mild reduction may result in spontaneous bleeding. Treatment of mild FVII deficiency requires a careful case-by-case approach, based on the clinical scenario.

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Malignant Brenner tumor of the ovary: A population-based study

Bean

Anderson

Taylor

et al. 2016

Gynecologic Oncology

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Mithramycin Impairs the Release of <sup>45</sup>Ca from Bone Induced by Prostaglandin E<sub>2</sub> or Multiple Myeloma Sera

Anderson¹,

Rubenstein²,

Sky-Peck³

1982

Oncology

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Some tumors release factors able to activate host osteoclasts. Mithramycin at sub-tumoricidal doses inhibits the release of calcium mediated by osteoclasts. If invasion of bone by a cancer requires activation of these cells, their intermittent ‘blockade’ might impede the development of metastases to bone or their local extension. Fetal rat bones prelabelled with ⁴⁵Ca were cultured in the presence of 10^––⁷M prostaglandin E₂, sera from normal individuals, or from patients with multiple myeloma. Additional samples preincubated for 3 h with 1 μg/ml of mithramycin, were washed before culture. Compared with controls, prostaglandin E₂ stimulated the release of ⁴⁵Ca by 28% (5 experiments) and mithramycin inhibited release by 15% (3 experiments). Pre-exposure to this cytotoxic antibiotic before culture withPGE₂ reduced the augmented release. Sera from 4 patients with multiple myeloma were incubated with ⁴⁵Ca-labelled bones, some pretreated with mithramycin. An additional 29% release of ⁴⁵Ca (4 experiments) was prevented by mithramycin. These results are consistent with the hypothesis that augmented release of ⁴⁵Ca due to stimulatory factors such as prostaglandins or factors in sera from patients with multiple myeloma can be partially inhibited by pretreatment with mithramycin. Possibly, intermittent blockade of host osteoclasts can impair formation of metastases to bone by cancers dependent upon their activation for this event, or reduce the extent of local invasion by established metastases. Modifying the behavior of a cancer by altering the host-response to factors which it releases represents a potential alternative to cytotoxic chemotherapy.

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