Mark R. Berardi scite author profile

Mark R. Berardi

4Publications

24Citation Statements Received

148Citation Statements Given

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129

Affiliations

Rutgers, The State University of New Jersey

Publications

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Renal Changes Associated with Naproxen Sodium Administration in Cynomolgus Monkeys

Leach¹,

Frank²,

Berardi³

et al. 1999

Toxicol Pathol

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Naproxen sodium was administered to cynomolgus monkeys (Macaca fascicularis) by oral gavage at daily doses of 44, 88, or 176 mg/kg for 2 wk (2 monkeys/gender) or of 44 mg/kg for 13 wk (4 monkeys/gender). Body weight loss occurred in at least one monkey in all naproxen sodium-dosed groups in the 2-wk (up to 16% loss) and 13-wk (up to 22% loss) studies. Increases in plasma naproxen concentrations were dose proportional between 44 and 88 mg/kg but were less than dose proportional between 88 and 176 mg/kg. Up to 2-fold increases in creatinine and/or serum urea nitrogen values as well as higher renal weights occurred in monkeys receiving 176 mg/kg for 2 wk or 44 mg/kg for 13 wk. Microscopically, renal changes were observed in all naproxen sodium-dosed groups. Renal findings after 2 wk of exposure included increased interstitial ground substance, tubular dilatation, and tubulointerstitial nephritis; in the 13-wk study, cortical tubular atrophy and interstitial fibrosis were also observed. These studies identify the kidney as the target organ of naproxen sodium in cynomolgus monkeys.

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Development of Hibernomas in Rats Dosed with Phentolamine Mesylate During the 24-Month Carcinogenicity Study

Poulet¹,

Berardi²,

Halliwell³

et al. 2004

Toxicol Pathol

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Phentolamine is a reversible competitive alpha-adrenergic antagonist with similar affinities for alphal and alpha2 receptors. It has a long history of safe clinical use, and was developed as a potential therapy for male erectile dysfunction because of its capacity to increase the arteriolar blood flow to the corpora cavernosa. Phentolamine mesylate was administered to rats by oral gavage at daily doses of 10, 50, and 150 mg/kg for 24 months. A dose-related increase in mortality, ascribed to an exaggerated pharmacologic effect, was seen at high doses. Systemic exposure as measured by plasma drug concentration increased with dose and duration of dosing and slight drug accumulation occurred, particularly in high-dose males. In the treated groups, 10 males and 1 female were diagnosed with hibernomas, neoplasms of brown adipose tissue, which appeared in the thoracic cavity or retroperitoneal area as circumscribed, tan to reddish-brown lobulated masses. Histologically, the masses were well circumscribed with variably sized lobules defined by a rich capillary network and consisted of closely apposed oval to polygonal cells with large amounts of cytoplasm and a centrally located nucleus. The cytoplasm's appearance varied from multivacuolated to univacuolated to granular eosinophilic. In a few cases, neoplastic emboli were observed in capsular vessels. Ultrastructurally, the neoplastic cells contained numerous mitochondria with transverse parallel cristae that occupied over 60% of the cytoplasm and lipid droplets. This study documents the previously unreported development of hibernomas in rats treated with phentolamine mesylate.

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Effect of chlorine and monochloramine in drinking water on the developing rat fetus

Abdel‐Rahman

Berardi

Bull

1982

J of Applied Toxicology

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Chlorine dioxide (C102) or monochloramine (NH2C1) may be considered as an alternative to chlorine (HOCl) as a disinfectant in public water supplies, since chlorination produces trihalomethanes. This study was conducted to determine the effect of chlorine and monochloramine on rat fetuses. Female rats were administered 0, 1, 10 or 100 mg 1-I NHzCl or HOCl daily in the drinking water for 23months prior to and throughout gestation. Rats were sacrificed on Day 20 of gestation and fetuses were preserved for soft-tissue and skeletal examination. No significant increase in fetal resorptions was found in any treated group. A slight increase in skeletal variants (such as incompletely ossified or missing sternebrae, or rudimentary ribs) was seen in 10 and 100 mg 1-' HOCl groups. Soft-tissue defects, mainly improper orientation of the heart or adrenal agenesis, were observed in the 100 mg 1-' HOCl group. The percentage of total defects (skeletal and soft-tissue) was increased significantly over control in the 100 mg 1-' HOCl group; however, monochloramine did not produce any significant changes in rat fetuses at any dose level.

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Monochloroacetic acid toxicity in the mouse associated with blood-brain barrier damage1, 2

Berardi¹

1987

Fundamental and Applied Toxicology

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Mark R. Berardi

Renal Changes Associated with Naproxen Sodium Administration in Cynomolgus Monkeys

Development of Hibernomas in Rats Dosed with Phentolamine Mesylate During the 24-Month Carcinogenicity Study

Effect of chlorine and monochloramine in drinking water on the developing rat fetus

Monochloroacetic acid toxicity in the mouse associated with blood-brain barrier damage1, 2

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Mark R. Berardi

Renal Changes Associated with Naproxen Sodium Administration in Cynomolgus Monkeys

Development of Hibernomas in Rats Dosed with Phentolamine Mesylate During the 24-Month Carcinogenicity Study

Effect of chlorine and monochloramine in drinking water on the developing rat fetus

Monochloroacetic acid toxicity in the mouse associated with blood-brain barrier damage*1, *2

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Monochloroacetic acid toxicity in the mouse associated with blood-brain barrier damage1, 2