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Institution

Jewish Hospital

HealthcareCincinnati, Ohio, United States
About: Jewish Hospital is a healthcare organization based out in Cincinnati, Ohio, United States. It is known for research contribution in the topics: Antigen & Population. The organization has 3881 authors who have published 3414 publications receiving 123044 citations.


Papers
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Journal ArticleDOI
TL;DR: This review of the 10-year world experience found uniform technical success, immunologic biology, and immunosuppression regimens very similar to solid organ transplants, and success strongly correlated with adherence to guidelines for psychiatric screening, thorough preparation of patient and families, intense postoperative monitoring, and assurance of medication access.

44 citations

Journal ArticleDOI
Samuel Simkins1
TL;DR: The effects of massive doses of vitamin A in hyperthyroidism were tested in two patients, one of which was a woman with menopausal exophthalmic goiter of moderate severity complicated by essential hypertension; the second, a rather severely toxichyperthyroid woman.
Abstract: INVESTIGATIVE work during the last decade and a half has established the close interrelationships existing between hormones and vitamins in their effects on the same organs of the body (19). Of considerable interest is the relationship between thyroxine and vitamin A, concerning which an extensive literature has developed abroad but strangely enough comparatively little in this country. The antagonism between the thyroid hormone and vitamin A was first suggested a half century ago (39) and confirmed between 1930 and 1939 by extensive experimental work in animals. For the present report the effects of massive doses of vitamin A (200,000 to 400,000 i.u. daily) in hyperthyroidism were tested in two patients. One was a woman with menopausal exophthalmic goiter of moderate severity complicated by essential hypertension; the second, a rather severely toxic hyperthyroid woman. Routine studies such as urinalysis, blood count, blood sugar and electrocardiogram were performed in both patients; the metabolic rate an...

44 citations

Journal ArticleDOI
TL;DR: This biodegradable 3DFC patch improves LV function and myocardial blood flow 3 weeks after MI, and is a potentially new approach to cell-based therapy for heart failure after MI.

44 citations

Journal ArticleDOI
TL;DR: The experience with a leiomyosarcoma in the superior vena cava of a 44-year-old white man, who had been locally excised and then recurred 2 1/2 years later, is reported.

44 citations

Journal ArticleDOI
TL;DR: It is concluded that bone‐bound Ga(III) from medium concentrations < 15 μM inhibits osteoclasts reversibly, while irreversible toxicity occurs at solution [Ga3+] > 50 μM, indicating that gallium below ∼150 pg/μg bone acts for a limited time and does not permanently damage the cells.
Abstract: Gallium(III) is a new therapeutic agent for hypercalcemia. Ga3+ reduces osteoclast action, but how it inhibits the cell's physiology is unknown. In vivo, 7-12 microM Ga(III) reduces calcium release from bone, but surprisingly, 10-100 microM Ga3+ added to isolated avian osteoclasts did not reduce their degradation of L-(5-3H)-proline bone. 3H-proline labels bone collagen specifically, and collagenolysis is an excellent indicator of bone dissolution because collagen is the least soluble component of bone. Ga(III) greater than 100 microM inhibited osteoclasts in vitro, but also killed the cells. To resolve this apparent conflict, we measured 67Ga distribution between bone, cells, and media. Gallium binds avidly but slowly to bone fragments. One hundred micrograms of bone clears 60% of 1 microM gallium from 500 microliters of tissue culture medium, with steady state at greater than 24 h. Osteoclasts on bone inhibited gallium binding capacity approximately 40%, indicating a difference in available binding area and suggesting that osteoclasts protect their substrate from Ga binding. Less gallium binds to bone in serum-containing medium than in phosphate-buffered saline; 30% reduction of the affinity constant suggests that the serum containing medium competes with bone binding. Consequently, the effect of [Ga] on bone degradation was studied using accurately controlled amounts of Ga(III) pre-bound to the bone. Under these conditions, gallium sensitivity of osteoclasts is striking. At 2 days, 100 micrograms of bone pre-incubated with 1 ml of 1 microM Ga3+, with 10 pmoles Ga3+/micrograms bone, was degraded at 50% the rate of control bone; over 50 pM Ga3+/micrograms bone, resorption was essentially zero. In contrast, pre-treatment of bone with [Ga3+] as high as 15 microM had no significant effect on bone resorption rate beyond 3 days, indicating that gallium below approximately 150 pg/micrograms bone acts for a limited time and does not permanently damage the cells. We conclude that bone-bound Ga(III) from medium concentrations less than 15 microM inhibits osteoclasts reversibly, while irreversible toxicity occurs at solution [Ga3+] greater than 50 microM.

44 citations


Authors

Showing all 3894 results

NameH-indexPapersCitations
John C. Morris1831441168413
David L. Kaplan1771944146082
Robert H. Purcell13966670366
Nancy J. Cox135778109195
Jennifer S. Haas12884071315
David A. Cheresh12533762252
John W. Kappler12246457541
Philippa Marrack12041654345
Arthur Weiss11738045703
Thomas J. Kipps11474863240
Michael Pollak11466357793
Peter M. Henson11236954246
Roberto Bolli11152844010
William D. Foulkes10868245013
David A. Lynch10871459678
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Performance
Metrics
No. of papers from the Institution in previous years
YearPapers
20232
202217
202148
202039
201944
201828