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Featured researches published by Allan Schuss.


Breast Cancer Research and Treatment | 2002

The Long Island Breast Cancer Study Project: Description of a multi-institutional collaboration to identify environmental risk factors for breast cancer

Marilie D. Gammon; Alfred I. Neugut; Regina M. Santella; Susan L. Teitelbaum; Julie A. Britton; Mary Beth Terry; Sybil M. Eng; Mary S. Wolff; Steven D. Stellman; Geoffrey C. Kabat; Bruce Levin; H. Leon Bradlow; Maureen Hatch; Jan Beyea; David Camann; Martin Trent; Ruby T. Senie; Gail C. Garbowski; Carla Maffeo; Pat Montalvan; Ger trud S. Berkowitz; Margaret Kemeny; Marc L. Citron; Freya Schnabel; Allan Schuss; Steven I. Hajdu; Vincent Vincguerra; Gwen W. Collman; G. Iris Obrams

The Long Island Breast Cancer Study Project is a federally mandated, population-based case-control study to determine whether breast cancer risk among women in the counties of Nassau and Suffolk, NY, is associated with selected environmental exposures, assessed by blood samples, self-reports, and environmental home samples. This report describes the collaborative projects background, rationale, methods, participation rates, and distributions of known risk factors for breast cancer by case-control status, by blood donation, and by availability of environmental home samples. Interview response rates among eligible cases and controls were 82.1% (n, = 1,508) and 62.8% (n = 1,556), respectively. Among case and control respondents who completed the interviewer-administered questionnaire, 98.2 and 97.6% self-completed the food frequency questionnaire; 73.0 and 73.3% donated a blood sample; and 93.0 and 83.3% donated a urine sample. Among a random sample of case and control respondents who are long-term residents, samples of dust (83.6 and 83.0%); soil (93.5 and 89.7%); and water (94.3 and 93.9%) were collected. Established risk factors for breast cancer that were found to increase risk among Long Island women include lower parity, late age at first birth, little or no breast feeding, and family history of breast cancer. Factors that were found to be associated with a decreased likelihood that a respondent would donate blood include increasing age and past smoking; factors associated with an increased probability include white or other race, alcohol use, ever breastfed, ever use of hormone replacement therapy, ever use of oral contraceptives, and ever had a mammogram. Long-term residents (defined as 15+ years in the interview home) with environmental home samples did not differ from other long-term residents, although there were a number of differences in risk factor distributions between long-term residents and other participants, as anticipated.


Cancer Epidemiology, Biomarkers & Prevention | 2002

Environmental Toxins and Breast Cancer on Long Island. I. Polycyclic Aromatic Hydrocarbon DNA Adducts

Marilie D. Gammon; Regina M. Santella; Alfred I. Neugut; Sybil M. Eng; Susan L. Teitelbaum; Andrea Paykin; Bruce Levin; Mary Beth Terry; Tie Lan Young; Lian Wen Wang; Qiao Wang; Julie A. Britton; Mary S. Wolff; Steven D. Stellman; Maureen Hatch; Geoffrey C. Kabat; Ruby T. Senie; Gail C. Garbowski; Carla Maffeo; Pat Montalvan; Gertrud S. Berkowitz; Margaret Kemeny; Marc L. Citron; Freya Schnabel; Allan Schuss; Steven I. Hajdu; Vincent Vinceguerra

Polycyclic aromatic hydrocarbons (PAH) are potent mammary carcinogens in rodents, but their effect on breast cancer development in women is not clear. To examine whether currently measurable PAH damage to DNA increases breast cancer risk, a population-based case-control study was undertaken on Long Island, NY. Cases were women newly diagnosed with in situ and invasive breast cancer; controls were randomly selected women frequency matched to the age distribution of cases. Blood samples were donated by 1102 (73.0%) and 1141 (73.3%) of case and control respondents, respectively. Samples from 576 cases and 427 controls were assayed for PAH-DNA adducts using an ELISA. The geometric mean (and geometric SD) of the log-transformed levels of PAH-DNA adducts on a natural scale was slightly, but nonsignificantly, higher among cases [7.36 (7.29)] than among controls [6.21 (4.17); P = 0.51]. The age-adjusted odds ratio (OR) for breast cancer in relation to the highest quintile of adduct levels compared with the lowest was 1.51 [95% confidence interval (CI), 1.04-2.20], with little or no evidence of substantial confounding (corresponding multivariate-adjusted OR, 1.49; 95% CI, 1.00-2.21). There was no consistent elevation in risk with increasing adduct levels, nor was there a consistent association between adduct levels and two of the main sources of PAH, active or passive cigarette smoking or consumption of grilled and smoked foods. These data indicate that PAH-DNA adduct formation may influence breast cancer development, although the association does not appear to be dose dependent and may have a threshold effect.


Breast Cancer Research and Treatment | 1986

A comparison of tumor-related antigens in male and female breast cancer.

Joel Lundy; Yousri Mishriki; Michael V. Viola; Sylvia Chao; Barbara Kasa; Sheila Oravez; Allan Schuss

SummaryA retrospective analysis was undertaken in which 15 female and 15 male breast cancers were matched by age, stage, estrogen receptor status, and histologic type. Our protocol compares male and female breast cancers for reactivity with antibodies against tumor-associated antigens known to be present on female breast cancer cells. Formalin-fixed sections of each primary tumor were reacted in the ABC immunoperoxidase assay against antibodies B72.3 and DF.3 and an antibody to theras p21 antigen. Reactivity to B72.3 and DF.3 was similar. However, the ras p21 antigen was expressed to a significantly greater extent in female breast cancers (p = .0008). Thus, although there are similarities in antigenic phenotype of male and female breast cancers, some female breast cancers may have a different pathogenesis as demonstrated by increased amounts of a specific oncogene product.


Cancer Investigation | 1988

Reactivity of the monoclonal antibody B72.3 with fetal antigen: correlation with expression of TAG-72 in human carcinomas.

Doris Stanick; Allan Schuss; Yousri Mishriki; Sylvia Chao; Ann Thor; Joel Lundy

The monoclonal antibody (MAb) B72.3 recognizes a mucin-like glycoprotein, TAG-72, which has been detected in a spectrum of human carcinomas, but not in the normal tissue counterparts. Using avidin-biotin-peroxidase complex (ABC) immunohistochemical techniques, MAb B72.3 was reacted with formalin-fixed, paraffin-embedded fetal and pediatric tissue sections to determine the extent of expression of the recognized antigen in these tissues. First trimester fetal tissues failed to express detectable antigen. Gastrointestinal epithelia from 13 to 34 weeks gestation demonstrated the most immunoreactivity with B72.3 although bronchial respiratory epithelium of the lung, transitional epithelium from the kidney, Hassalls corpuscles of the thymus, and gonadal tissues from fetuses of both sexes were also reactive. The TAG-72 antigen was not detected in fetal breast, pancreas, liver, spleen, adrenal, or heart. Expression of the TAG-72 antigen in malignancy appears to correlate well with fetal tissue reactivity with B72.3.


Clinical Imaging | 2004

Lymphomatoid granulomatosis in a pediatric patient

Joseph P. Mazzie; Anita P. Price; Poonam Khullar; Carlos H Montoya; Jon E. Roberts; Haesoon Lee; Lewis Williams; Allan Schuss; Douglas S. Katz

We report the radiology and pathology of a pediatric patient with lymphomatoid granulomatosis (LG) and review the literature, with an emphasis on the radiological findings and on the small subset of pediatric patients with this rare condition.


Diseases of The Colon & Rectum | 1988

Phenotypic markers for a spectrum of colonic polyps and cancers

Joel Lundy; Allan Schuss; Sergey Lyubsky; Darya Sadri; Doris Stanick

The purpose of this study was to determine if a panel of monoclonal antibodies could define phenotypic markers that could be used in risk assessment of a spectrum of colonic polypes and colon cancers. Using the ABC immunoperoxidase technique on formalin-fixed sections of surgical specimens, the following results were obtained: 1) Mab B72.3 demonstrated increased reactivity in villous lesions and cancers compared with hyperplastic polyps and tubular adenomas; 2) Mab anti-CAA demonstrated increased reactivity in polyps compared with colon cancers; and 3) using the two antibodies (Mab B72.3 and Mab anti-CAA), a malignancy ratio was obtained that determined malignancy risk for individual polyps. No hyperplastic polyp gave a positive ratio, but about 30 percent of villous lesions were positive. Over 50 percent of villous lesions greater than 2 cm in size had a positive ratio. The malignancy potential ratio may be a valuable marker in assessing risk of malignancy in an individual case.


Cancer Epidemiology, Biomarkers & Prevention | 2002

Environmental toxins and breast cancer on Long Island. II. Organochlorine compound levels in blood

Marilie D. Gammon; Mary S. Wolff; Alfred I. Neugut; Sybil M. Eng; Susan L. Teitelbaum; Julie A. Britton; Mary Beth Terry; Bruce Levin; Steven D. Stellman; Geoffrey C. Kabat; Maureen Hatch; Ruby T. Senie; Gertrud S. Berkowitz; H. Leon Bradlow; Gail C. Garbowski; Carla Maffeo; Pat Montalvan; Margaret Kemeny; Marc L. Citron; Freya Schnabel; Allan Schuss; Steven I. Hajdu; Vincent Vinceguerra; Nancy J. Niguidula; Karen Ireland; Regina M. Santella


Clinical Imaging | 2006

Acinar cell carcinoma of the pancreas

Michael Khalili; Bobbi N. Wax; William P. Reed; Allan Schuss; Steven Drexler; Shiobhan R. Weston; Douglas S. Katz


Clinical Imaging | 2006

Radiology–Pathology Conference: sclerosing hemangioma of the lung

Jeremy Neuman; Alex Rosioreanu; Allan Schuss; George K. Turi; Elizabeth Yung; Terence K. Trow; Lewis Williams; Douglas S. Katz


American Journal of Roentgenology | 2002

Thoracic Epidural Castleman's Disease

Recha S. Eisenstat; Donald B. Price; Alan D. Rosenthal; Allan Schuss; Douglas S. Katz

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Douglas S. Katz

Winthrop-University Hospital

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Joel Lundy

Stony Brook University

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Doris Stanick

Winthrop-University Hospital

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Geoffrey C. Kabat

Albert Einstein College of Medicine

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Haesoon Lee

SUNY Downstate Medical Center

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Julie A. Britton

Icahn School of Medicine at Mount Sinai

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