17 results on '"Margaret A. Douglass"'
Search Results
2. Atrial natriuretic peptide increases adrenomedullin in the circulation of healthy humans
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Michael T. McCormick, George Rodriguez-Paz, Mary S. Blankenship, Margaret A. Douglass, David L. Vesely, and Douglas D. Schocken
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Adult ,Male ,medicine.medical_specialty ,Vasodilator Agents ,Prohormone ,Diuresis ,Blood Pressure ,Peptide hormone ,General Biochemistry, Genetics and Molecular Biology ,Adrenomedullin ,Atrial natriuretic peptide ,Internal medicine ,medicine ,Humans ,General Pharmacology, Toxicology and Pharmaceutics ,Chemistry ,General Medicine ,Middle Aged ,NPR1 ,NPR2 ,Blood pressure ,Endocrinology ,Blood Circulation ,cardiovascular system ,Female ,Peptides ,Atrial Natriuretic Factor ,hormones, hormone substitutes, and hormone antagonists ,medicine.drug - Abstract
Adrenomedullin (ADM) is a new 52 amino acid peptide originally isolated from extracts of human pheochromocytoma. ADM's biologic properties are nearly identical to those of atrial natriuretic peptides. Thus, the 4 peptide hormones originating from amino acids 1-30 [long acting natriuretic peptide], 31-67 [vessel dilator], 79-98 [kaliuretic peptide] and 99-126 [atrial natriuretic factor; ANF] of the 126 amino acid ANF prohormone as well as ADM have blood pressure lowering and diuretic properties. The present investigation was designed to determine if one or more of these 4 atrial natriuretic peptides increase adrenomedullin within the circulation of healthy humans. Infusion of 100 ng/kg body weight/minute for 60 minutes of the respective atrial peptides resulted in a 4-fold (P < 0.001) increase in the circulating concentration of adrenomedullin secondary to the ANF infusion but no increase in adrenomedullin with the long acting natriuretic peptide, vessel dilator, or kaliuretic peptide infusions. The four-fold increase of adrenomedullin in the circulation persisted throughout the infusion of ANF, but returned to pre-infusion levels within 30 minutes of stopping the ANF infusion. Infusion of 10 pg/kg body weight/minute for 60 minutes of ANF resulted in a 2 1/2-fold increase (P < 0.05) in the circulating concentration of adrenomedullin. There was a significant (P < 0.01) diuresis and blood pressure lowering effect with each of the atrial natriuretic peptides in the present investigation. This investigation suggests that 1) atrial natriuretic factor increases the release of adrenomedullin and 2) that the diuretic and blood pressure lowering effects previously attributed to atrial natriuretic factor may be partially due to adrenomedullin since both increased during the ANF infusion and both have similar biologic effects. As opposed to atrial natriuretic factor, adrenomedullin was not increased by long acting natriuretic peptide, vessel dilator, or kaliuretic peptide suggesting that their biologic effects do not involve adrenomedullin.
- Published
- 1996
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3. Atrial natriuretic peptides negatively and positively modulate circulating endothelin in humans
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Shirley Chiou, Douglas D. Schocken, Michael T. McCormick, David L. Vesely, Margaret A. Douglass, and George Rodriguez-Paz
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Adult ,Male ,medicine.medical_specialty ,medicine.drug_class ,Endocrinology, Diabetes and Metabolism ,Prohormone ,Peptide ,Vasodilation ,Peptide hormone ,chemistry.chemical_compound ,Endocrinology ,Internal medicine ,Natriuretic peptide ,medicine ,Humans ,Cyclic GMP ,Cyclic guanosine monophosphate ,chemistry.chemical_classification ,Endothelins ,Metabolism ,Middle Aged ,chemistry ,cardiovascular system ,Female ,Endothelin receptor ,Atrial Natriuretic Factor ,medicine.drug - Abstract
The present investigation was designed to examine the effect of four atrial peptide hormones with vasodilatory properties on the circulating immunoreactive (ir) levels of the vasoconstrictive peptide endothelin (ET) in 36 healthy human subjects. Circulating levels of human ET and cyclic guanosine monophosphate ([cGMP], a potential mediator of the effects of atrial peptides), were measured every 30 minutes during 1-hour preinfusion, 1-hour infusion, and 3-hour postinfusion periods. Atrial natriuretic factor ([ANF] amino acid (aa) 99 to 126 of the 126-aa ANF prohormone) and kaliuretic peptide (aa 79 to 98 of this same prohormone) significantly (P
- Published
- 1996
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4. Atrial Natriuretic Peptides and Cyclic Guanosine Monophosphate Metabolism
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Michael T. McCormick, Amy T. Giordano, George Rodriguez-Paz, Douglas D. Schocken, David L. Vesely, and Margaret A. Douglass
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Adult ,Male ,medicine.medical_specialty ,medicine.drug_class ,Prohormone ,Blood Pressure ,Peptide hormone ,chemistry.chemical_compound ,Atrial natriuretic peptide ,Internal medicine ,medicine ,Natriuretic peptide ,Humans ,Cyclic GMP ,Cyclic guanosine monophosphate ,chemistry.chemical_classification ,business.industry ,General Medicine ,Metabolism ,Middle Aged ,NPR2 ,Amino acid ,Endocrinology ,chemistry ,Female ,business ,Atrial Natriuretic Factor ,medicine.drug - Abstract
Atrial natriuretic factor (ANF), consisting of amino acids 99-126 of the 126 amino acid ANF prohormone, increases cyclic guanosine monophosphate (GMP) (thought to be the mediator of its physiologic effects) in plasma and urine of human subjects. Long-acting natriuretic peptide, vessel dilator, and kaliuretic peptide, consisting of amino acid 1-30, 31-67, and 79-98, respectively, of this same prohormone have natriuretic, diuretic, kaliuretic, and blood pressure lowering properties in humans. These three new peptide hormones increase cyclic GMP in vitro but were never investigated to determine whether they also cause extrusion of cyclic GMP from cells, resulting in an increase of cyclic GMP in plasma and/or urine. Infusion of each of these peptide hormones at their 100 ng/kg body weight/min concentrations for 60 minutes into healthy humans resulted in a sevenfold increase in cyclic GMP in plasma and urine secondary to ANF, but no significant increase secondary to the other atrial peptide hormones. Based on the current data, ANF has a unique effect on the metabolism of cyclic GMP, causing it to be extruded from the cell, whereas the other three atrial peptides represent the more classical metabolism of cyclic GMP via cyclic GMP phophodiesterases.
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- 1995
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5. Three peptides from the atrial natriuretic factor prohormone amino terminus lower blood pressure and produce diuresis, natriuresis, and/or kaliuresis in humans
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George Rodriguez-Paz, John R. Dietz, Douglas D. Schocken, David L. Vesely, Margaret A. Douglass, William R. Gower, and Michael T. McCormick
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Adult ,Male ,medicine.medical_specialty ,Prohormone ,Radioimmunoassay ,Natriuresis ,Diuresis ,Hemodynamics ,Blood Pressure ,Peptide hormone ,Atrial natriuretic peptide ,Physiology (medical) ,Internal medicine ,Humans ,Medicine ,Protein Precursors ,business.industry ,Osmolar Concentration ,Middle Aged ,Peptide Fragments ,Blood pressure ,Endocrinology ,Kaliuresis ,Chromatography, Gel ,Potassium ,Female ,Cardiology and Cardiovascular Medicine ,business ,Atrial Natriuretic Factor ,medicine.drug - Abstract
BACKGROUND Three peptides consisting of amino acids 1-30, 31-67, and 79-98 of the 126-amino acid atrial natriuretic factor prohormone (proANF), which have blood pressure-lowering, diuretic, natriuretic, and/or kaliuretic properties in animals, were investigated to determine if they have similar properties in humans. METHODS AND RESULTS Thirty-six healthy, normotensive human volunteers (18 men and 18 women, ages 20 to 58 years) were divided into six similar groups based on age, sex, weight, blood pressure, and heart rate. After a 60-minute baseline period, 100 ng of proANFs 1-30, 31-67, 79-98, or ANF/kg body wt per minute was given intravenously for 60 minutes followed by a 3-hour postinfusion data collection period. Each of the atrial natriuretic peptides decreased systolic and diastolic blood pressures (P < .05), with proANF 31-67 causing the largest decrease. Urine flow increased 4- to 12-fold and was still significantly increased (P < .01) for 2 to 3 hours after stopping the respective infusions of proANFs 1-30, 31-67, and 79-98. Atrial natriuretic factor (ANF) increased urine flow 4- to 11-fold but by 2 hours after infusion was significantly increased in only 1 of 6 subjects. Sodium excretion increased 3- to 8-fold, 3- to 6-fold, 0- to 2-fold (NS), and 3- to 11-fold, respectively, with proANFs 1-30, 31-67, 79-98, and ANF. Natriuretic effects of proANFs 1-30 and 31-67 were significantly prolonged (P < .001) compared with ANF. ProANFs 1-30, 31-67, 79-98, and ANF increased potassium excretion 2- to 3-fold, 0-fold, 3- to 4-fold, and 2-fold, respectively. High-performance gel permeation chromatography followed by the respective radioimmunoassays revealed that proANFs 1-30, 31-67, 79-98, and 68-98, as well as ANF circulate as distinct peptides. CONCLUSIONS ProANFs 1-30, 31-67, and 79-98, as well as ANF have significant blood pressure-lowering and diuretic properties. ProANFs 1-30 and 31-67 also have natriuretic properties in humans that are significantly (P < .001) prolonged compared with ANF. ProANF 79-98, although not possessing any natriuretic property, is the strongest stimulator of potassium excretion of the four atrial natriuretic peptides.
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- 1994
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6. Automated de-identification of free-text medical records
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Gari D. Clifford, Margaret M Douglass, Ishna Neamatullah, George B. Moody, Mauricio Villarroel, Roger G. Mark, Andrew T. Reisner, Peter Szolovits, William J. Long, Li-wei H. Lehman, Harvard University--MIT Division of Health Sciences and Technology, Massachusetts Institute of Technology. Computer Science and Artificial Intelligence Laboratory, Massachusetts Institute of Technology. Department of Electrical Engineering and Computer Science, Harvard--MIT Program in Health Sciences and Technology. Laboratory for Computational Physiology, Lehman, Li-Wei H., Reisner, Andrew T., Villarroel Montoya, Mauricio Christian, Long, William J., Szolovits, Peter, Moody, George B., Mark, Roger Greenwood, Clifford, Gari D., Neamatullah, Ishna, and Douglass, Margaret M.
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020205 medical informatics ,Computer science ,Word count ,Dictionaries as Topic ,Health Informatics ,02 engineering and technology ,lcsh:Computer applications to medicine. Medical informatics ,computer.software_genre ,Health informatics ,Medical Records ,Set (abstract data type) ,03 medical and health sciences ,0302 clinical medicine ,0202 electrical engineering, electronic engineering, information engineering ,Humans ,030212 general & internal medicine ,Natural Language Processing ,Protected health information ,Health Insurance Portability and Accountability Act ,business.industry ,Health Policy ,Medical record ,De-identification ,Patient Discharge ,United States ,3. Good health ,Computer Science Applications ,lcsh:R858-859.7 ,Programming Languages ,Data mining ,Artificial intelligence ,Heuristics ,business ,computer ,Algorithms ,Confidentiality ,Software ,Natural language processing ,Research Article - Abstract
Background: Text-based patient medical records are a vital resource in medical research. In order to preserve patient confidentiality, however, the U.S. Health Insurance Portability and Accountability Act (HIPAA) requires that protected health information (PHI) be removed from medical records before they can be disseminated. Manual de-identification of large medical record databases is prohibitively expensive, time-consuming and prone to error, necessitating automatic methods for large-scale, automated de-identification. Methods: We describe an automated Perl-based de-identification software package that is generally usable on most free-text medical records, e.g., nursing notes, discharge summaries, X-ray reports, etc. The software uses lexical look-up tables, regular expressions, and simple heuristics to locate both HIPAA PHI, and an extended PHI set that includes doctors' names and years of dates. To develop the de-identification approach, we assembled a gold standard corpus of re-identified nursing notes with real PHI replaced by realistic surrogate information. This corpus consists of 2,434 nursing notes containing 334,000 words and a total of 1,779 instances of PHI taken from 163 randomly selected patient records. This gold standard corpus was used to refine the algorithm and measure its sensitivity. To test the algorithm on data not used in its development, we constructed a second test corpus of 1,836 nursing notes containing 296,400 words. The algorithm's false negative rate was evaluated using this test corpus. Results: Performance evaluation of the de-identification software on the development corpus yielded an overall recall of 0.967, precision value of 0.749, and fallout value of approximately 0.002. On the test corpus, a total of 90 instances of false negatives were found, or 27 per 100,000 word count, with an estimated recall of 0.943. Only one full date and one age over 89 were missed. No patient names were missed in either corpus. Conclusion We have developed a pattern-matching de-identification system based on dictionary look-ups, regular expressions, and heuristics. Evaluation based on two different sets of nursing notes collected from a U.S. hospital suggests that, in terms of recall, the software out-performs a single human de-identifier (0.81) and performs at least as well as a consensus of two human de-identifiers (0.94). The system is currently tuned to de-identify PHI in nursing notes and discharge summaries but is sufficiently generalized and can be customized to handle text files of any format. Although the accuracy of the algorithm is high, it is probably insufficient to be used to publicly disseminate medical data. The open-source de-identification software and the gold standard re-identified corpus of medical records have therefore been made available to researchers via the PhysioNet website to encourage improvements in the algorithm., National Institute of Biomedical Imaging and Bioengineering (U.S.), National Institutes of Health (U.S) ( Grant Number R01-EB001659 )
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- 2008
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7. Calciphylaxis: A Cause of Necrotic Ulcers in Renal Failure
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Amer N. Kalaaji, Marsha Chaffins, Margaret C. Douglass, and Lori Lowe
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Pathology ,medicine.medical_specialty ,Fatal outcome ,Biopsy ,medicine.medical_treatment ,Dermatology ,Peritoneal dialysis ,Necrosis ,030207 dermatology & venereal diseases ,03 medical and health sciences ,Fatal Outcome ,0302 clinical medicine ,Skin Ulcer ,medicine ,Humans ,Gynecology ,Calciphylaxis ,business.industry ,Middle Aged ,medicine.disease ,030220 oncology & carcinogenesis ,Kidney Failure, Chronic ,Female ,Surgery ,Dialisis peritoneal ,business ,Kidney disease - Abstract
Background:Calciphylaxis is a rare and life-threatening condition occurring in patients with end-stage renal disease on dialysis. The diagnosis is frequently delayed or missed and therapy is often unsuccessful.Objective:The clinical and pathological components of calciphylaxis are emphasized in a patient that may facilitate early diagnosis and initiation of therapy.Results:Early recognition of the clinical signs and symptoms of calciphylaxis is crucial. The tissue diagnosis requires large elliptical biopsies because histological findings are segmental and often missed.Conclusion:Early diagnosis and intervention in calciphylaxis is critical. Parathyroidectomy should be considered in all cases.
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- 1998
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8. Syringolymphoid hyperplasia with alopecia: two case reports and review of the literature
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Jennifer L. Hobbs, Marsha Chaffins, and Margaret C. Douglass
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Adult ,Male ,medicine.medical_specialty ,Pathology ,Hyperplasia ,integumentary system ,business.industry ,Lymphoid Tissue ,Alopecia ,Dermatology ,Gene rearrangement ,medicine.disease ,Lymphoma, T-Cell ,Skin Diseases ,Lymphoid hyperplasia ,Lymphoma ,medicine.anatomical_structure ,hemic and lymphatic diseases ,Sweat gland ,medicine ,Humans ,medicine.symptom ,business - Abstract
Syringolymphoid hyperplasia with alopecia is an uncommon, but histopathologically distinct, skin disorder that has been reported to occur with and possibly represent a syringotropic variant of cutaneous T-cell lymphoma. We report 2 patients with syringolymphoid hyperplasia with alopecia. Both had CD4-positive infiltrates; 1 also demonstrated loss of CD7. One patient had evidence of T-cell clonality by gene rearrangement studies, but neither had histologic evidence of cutaneous T-cell lymphoma. Because the natural progression of syringolymphoid hyperplasia with alopecia remains to be fully explained, close follow-up of patients is advised.
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- 2003
9. Kaliuretic peptide and long acting natriuretic peptide as well as atrial natriuretic factor inhibit aldosterone secretion
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S Chiou, Douglas D. Schocken, David L. Vesely, Michael T. McCormick, George Rodriguez-Paz, and Margaret A. Douglass
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Adult ,Male ,medicine.medical_specialty ,medicine.drug_class ,Endocrinology, Diabetes and Metabolism ,Prohormone ,Natriuresis ,Peptide hormone ,chemistry.chemical_compound ,Endocrinology ,Atrial natriuretic peptide ,Internal medicine ,Adrenal Glands ,medicine ,Humans ,Secretion ,Protein Precursors ,Diuretics ,Aldosterone ,chemistry.chemical_classification ,Chemistry ,Middle Aged ,Peptide Fragments ,Amino acid ,Mineralocorticoid ,Female ,Atrial Natriuretic Factor ,medicine.drug - Abstract
The present investigation was designed to determine whether atrial natriuretic peptides consisting of amino acids 1–30 (long acting natriuretic peptide), 31–67 (vessel dilator) and 79–98 (kaliuretic peptide) as well as 99–126 (atrial natriuretic factor (ANF)) of the 126 amino acid ANF prohormone inhibit aldosterone secretion. Thirty healthy human subjects were studied following infusion of 100 ng/kg body weight/min for 60 min of each of the respective peptides. Kaliuretic peptide decreased plasma aldosterone concentration by the greatest amount (6-fold) and plasma aldosterone was still significantly decreased (P Journal of Endocrinology (1995) 146, 373–380
- Published
- 1995
10. Negative feedback of atrial natriuretic peptides
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Amy T. Giordano, Margaret A. Douglass, David L. Vesely, Michael T. McCormick, Douglas D. Schocken, George Rodriguez-Paz, and John R. Dietz
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Adult ,Male ,medicine.medical_specialty ,Endocrinology, Diabetes and Metabolism ,Clinical Biochemistry ,Prohormone ,Blood Pressure ,Urine ,Peptide hormone ,Biochemistry ,Feedback regulation ,Feedback ,Endocrinology ,Atrial natriuretic peptide ,Infusion Procedure ,Negative feedback ,Internal medicine ,otorhinolaryngologic diseases ,medicine ,Humans ,Protein Precursors ,chemistry.chemical_classification ,Biochemistry (medical) ,Middle Aged ,musculoskeletal system ,Peptide Fragments ,Amino acid ,chemistry ,embryonic structures ,cardiovascular system ,Female ,hormones, hormone substitutes, and hormone antagonists ,Atrial Natriuretic Factor ,medicine.drug - Abstract
The present investigation was designed to determine whether atrial natriuretic peptides consisting of amino acids 1-30 [i.e. pro-ANF-(1-30)], 31-67 [i.e. pro-ANF(31-67)], 79-98 [i.e. pro-ANF-(79-98)], and 99-126 [i.e. atrial natriuretic factor (ANF)] of 126-amino acid ANF prohormone have a negative feedback on their own and each others' release. Thirty healthy human subjects were studied with infusion of 100 ng/kg BW.min for 60 min of each of the respective peptides. Pro-ANF-(1-30) decreased the circulating concentrations of pro-ANF-(31-67) and ANF 51% and 89%, respectively. Pro-ANF-(31-67) decreased the circulating concentration of ANF by 55% and the peptides immunologically recognized by the pro-ANF-(1-30) RIA by 58% [this assay recognizes pro-ANF-(1-30) (50%) and pro-ANF-(1-98) (50%)]. Pro-ANF-(79-98) decreased the circulating concentration of ANF by 40%, pro-ANF-(31-67) by 31%, and the peptides recognized by the pro-ANF-(1-30) RIA by 46%. ANF decreased the circulating concentration of pro-ANF-(31-67) by 40% and the peptides recognized by pro-ANF-(1-30) RIA by 38%. Infusion of pro-ANF-(1-30), -(31-67), -(79-98), and -(99-126) also decreased the excretion of the other atrial natriuretic peptides measured in the urine by 32-84%. Infusion of vehicle only did not result in any decrease in these atrial natriuretic peptides in either plasma or urine. These data taken together indicate that each of the respective atrial natriuretic peptides inhibits the release, rather than breakdown, of each other, as increased breakdown would have resulted in their urinary concentrations being increased. This study further indicates that because pro-ANF-(1-98) was decreased in the circulation secondary to pro-ANF-(31-67) and pro-ANF-(79-98) infusions, they inhibit their own release, as they are both derived from pro-ANF-(1-98).
- Published
- 1994
11. Chronic cutaneous lupus erythematosus presenting as periorbital edema and erythema
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Margaret C. Douglass, Stanley Cyran, and Judith L. Silverstein
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Pathology ,medicine.medical_specialty ,Erythema ,Periorbital Edema ,Dermatology ,Antimalarials ,Lupus Erythematosus, Discoid ,Edema ,Medicine ,Eyelid Diseases ,Humans ,skin and connective tissue diseases ,Lupus erythematosus ,integumentary system ,business.industry ,Middle Aged ,medicine.disease ,eye diseases ,Cutaneous Involvement ,Cutaneous Lupus Erythematosus ,Female ,medicine.symptom ,business ,Eyelid edema - Abstract
We report two unusual cases of cutaneous lupus erythematosus presenting as dramatic eyelid edema and erythema. Neither patient had evidence of systemic or other significant cutaneous involvement. The eyelid edema and erythema were unilateral in one case and bilateral in the other. Both cases responded to therapy with antimalarial drugs.
- Published
- 1992
12. Thy-1 and T-cell receptor antigen expression in mycosis fungoides and benign inflammatory dermatoses
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Lawrence A. Rheins, David P. Fivenson, Edward A. Krull, Margaret C. Douglass, James J. Nordlund, and Mark Pomaranski
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Cancer Research ,Pathology ,medicine.medical_specialty ,Biopsy ,Receptors, Antigen, T-Cell, alpha-beta ,T-Lymphocytes ,Receptors, Antigen, T-Cell ,Dermatitis ,Mycosis Fungoides ,Antigen ,medicine ,Humans ,Lymphocytes ,Skin ,Mycosis fungoides ,Lupus erythematosus ,Immunoperoxidase ,Parapsoriasis ,medicine.diagnostic_test ,business.industry ,T-cell receptor ,Receptors, Antigen, T-Cell, gamma-delta ,medicine.disease ,Immunohistochemistry ,Lymphoma ,Oncology ,Immunology ,Antigens, Surface ,Thy-1 Antigens ,business - Abstract
We have studied human Thy-1 and T-cell receptor (TCR) antigen expression in mycosis fungoides and benign inflammatory dermatoses. The study included 24 biopsy specimens from 21 patients with mycosis fungoides (nine patch stage from eight patients, 13 plaque stage from 11 patients, and two tumor stage from two patients), six specimens from five patients with premycotic parapsoriasis (pre-mycosis fungoides), three specimens from three patients with lichen planus, 11 specimens from 11 patients with lupus erythematosus, 13 specimens from 13 patients with dermatitis, six specimens from six patients with drug eruptions, nine normal skin specimens from nine subjects, and three specimens from three patients with small plaque (benign) parapsoriasis. Immunoperoxidase studies using the avidin-biotin complex technique on serial frozen sections were performed. Primary antibodies were anti-human Thy-1, anti-alpha heterodimer of the TCR, anti-beta heterodimer of the TCR, and anti-delta heterodimer of the TCR. An extensive dendritic network of Thy-1+ cells was seen in all cases of mycosis fungoides. Epidermotropic cells were Thy-1 negative, and Thy-1 was expressed perivascularly in normal individuals and patients as previously reported. Epidermal gamma/delta cells were seen only in mycosis fungoides, where up to 60% of the epidermal lymphocytes expressed this TCR. The increased numbers of Thy-1 and gamma/delta T cells in mycosis fungoides were statistically significant when compared with normal skin or benign inflammatory dermatoses. The role of these dendritic dermal Thy-1+ cells and epidermal gamma/delta T cells in mycosis fungoides is unclear. The significant numbers of these potentially immunomodulating cells that were seen suggest that they are involved in the pathogenesis of mycosis fungoides.
- Published
- 1991
13. Increased Gamma/Delta T Cells and Thy-1 Cells in Cutaneous T Cell Lymphoma
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Margaret C. Douglass, James J. Nordlund, David P. Fivenson, and Edward A. Krull
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T-Lymphocytes ,General Neuroscience ,Cutaneous T-cell lymphoma ,Receptors, Antigen, T-Cell, gamma-delta ,Biology ,medicine.disease ,Increased gamma/delta T cells ,Molecular biology ,General Biochemistry, Genetics and Molecular Biology ,Lymphoma, T-Cell, Cutaneous ,Interleukin 21 ,History and Philosophy of Science ,Antigens, Surface ,medicine ,Humans ,Thy-1 Antigens - Published
- 1991
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14. Topical photochemotherapy for alopecia areata
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Andrew J. Mitchell and Margaret C. Douglass
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Adult ,Male ,medicine.medical_specialty ,Adolescent ,Alopecia Areata ,medicine.medical_treatment ,Dermatology ,Terminal hair ,Disease course ,Recurrence ,medicine ,Humans ,skin and connective tissue diseases ,PUVA Therapy ,Aged ,integumentary system ,business.industry ,Follow up studies ,Middle Aged ,Alopecia areata ,medicine.disease ,Therapeutic modalities ,Surgery ,medicine.anatomical_structure ,Photochemotherapy ,Scalp ,PUVA therapy ,Female ,business ,After treatment ,Follow-Up Studies - Abstract
Twenty-two patients with alopecia areata were treated with a combination of topical 0.1% 8-methoxypsoralen and UVA (PUVA). Eight of the twenty-two patients (36.3%) responded with excellent regrowth (terminal hair in at least 75% of the treated scalp), and two patients (9.1%) showed good regrowth (terminal hair in 50% to 75% of the treated scalp). The mean total UVA exposure and the mean total number of treatments for the entire treatment course for these responders was 171.7 joules/cm2 and 47.4 treatments, respectively. Eight of the nine responders available for follow-up experienced some degree of relapse when PUVA treatments were tapered or during a follow-up period (mean, 8.3 months) after treatment was discontinued. Despite the failure of topical PUVA to change the long-term course of alopecia, the combination of PUVA with other therapeutic modalities may result in the prolongation of the beneficial effect in selected patients. The mechanism of action of PUVA in alopecia areata might involve an immunomodulatory effect.
- Published
- 1985
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15. Management of Warts in Children
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Raymond V. Caputo, Lionel Boxall, Margaret C. Douglass, Sidney Hurwitz, Peter J. Koblenzer, Gerald N. Goldberg, Brenda Moroz, and Neil S. Heskel
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Male ,medicine.medical_specialty ,Pediatrics ,Adolescent ,business.industry ,media_common.quotation_subject ,Dermatology ,humanities ,Neglect ,Course of action ,Child, Preschool ,Family medicine ,Pediatrics, Perinatology and Child Health ,medicine ,Humans ,Female ,Warts ,Child ,business ,media_common - Abstract
The ubiquitous wart plagues us all-patients, parents, atid physicians. Although some of us probably opt for benign neglect, others believe that a temperate or even aggressive approach to therapy is the most appropriate course of action. In this symposium, several practitioners offer their philosophy of therapy as well as specific favored potions and procedures for tackling this problem in chiWren atid adolescents.
- Published
- 1987
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16. Seborrheic dermatitis in patients with acquired immunodeficiency syndrome
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Barbara Mathes and Margaret C. Douglass
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Adult ,Male ,medicine.medical_specialty ,Population ,Dermatology ,Acquired immunodeficiency syndrome (AIDS) ,Seborrheic dermatitis ,medicine ,Humans ,In patient ,Prospective Studies ,education ,Prospective cohort study ,Immunodeficiency ,education.field_of_study ,Acquired Immunodeficiency Syndrome ,business.industry ,Incidence (epidemiology) ,Infant ,Middle Aged ,medicine.disease ,Control subjects ,Prognosis ,Dermatitis, Seborrheic ,Female ,business - Abstract
Many cutaneous disorders are associated with acquired immunodeficiency syndrome. We prospectively evaluated eighteen patients with acquired immunodeficiency syndrome and twelve patients with the immunodeficiency syndrome-related complex for dermatologic disorders. A high prevalence of seborrheic dermatitis was found in patients with acquired immunodeficiency syndrome--83%, in comparison with 1% to 3% of historic control subjects. Patients with the related complex also had an increased incidence of 42%. Seborrheic dermatitis in this population was often more explosive, inflammatory, and severe than is usually seen in otherwise healthy patients. Severity of seborrheic dermatitis correlated with a poor overall prognosis in our patients. Additionally, seborrheic dermatitis may be one of the most common cutaneous manifestations of acquired immunodeficiency syndrome.
- Published
- 1985
17. Clinical Staging for Cutaneous T-Cell Lymphoma
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Eric C. Vonderheid, Ervin H. Epstein, Margaret C. Douglass, Elizabeth I. McBURNEY, Henry H. Roenigk, Sylvan B. Green, Allan L. Lorincz, Stanford I. Lamberg, William E. Clendenning, Beno Michel, David P. Byar, Zvi Fuks, Jerome B. Block, Loren E. Golitz, and Eugene J. Van Scott
- Subjects
medicine.medical_specialty ,Mycosis fungoides ,Skin Neoplasms ,Lymphoma ,genetic structures ,business.industry ,T-Lymphocytes ,T cell ,Cutaneous T-cell lymphoma ,General Medicine ,Prognosis ,medicine.disease ,Dermatology ,Mycosis Fungoides ,medicine.anatomical_structure ,Internal Medicine ,Humans ,Sezary Syndrome ,Cooperative group ,Medicine ,Lymph Nodes ,business ,Neoplasm Staging - Abstract
The Mycosis Fungoides Cooperative Group has been following patients with cutaneous T-cell lymphoma, including mycosis fungoides and the Sézary syndrome variant. Previous analyses identified the extent of skin involvement and the number of sites of clinically enlarged lymph nodes as important prognostic variables. These two variables were used to classify 340 patients into four clinical stages. Repeat analysis based on additional followup data shows the usefulness of this clinical staging system for identifying patients with differing survival experience. An alternative grouping suggested by fitting a survival model to the data also has been studied. Staging systems based only on skin involvement and lymph nodes are recommended for general use because the information needed is readily available, requiring only physical examination.
- Published
- 1984
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