Your search keyword '"Patrick C. Walsh"' showing total 15 results

1. Radical prostatectomy for clinical stage T3a diseaseThe views and opinions of and endorsements by the author(s) do not reflect those of the US Army or the Department of Defense.

Author

Stephen J. Freedland, Alan W. Partin, Elizabeth B. Humphreys, Leslie A. Mangold, and Patrick C. Walsh

Subjects

PROSTATECTOMY, PROSTATE cancer, ONCOLOGIC surgery, CANCER in men

Abstract

Men with clinical stage T3a disease are at high risk and are often encouraged to undergo radiation therapy with concomitant hormonal therapy. The long‐term outcomes among men treated with radical prostatectomy for clinical stage T3a disease were examined.Among 3397 men treated by radical prostatectomy by 1 surgeon between 1987 and 2003, 62 (1.8%) men were identified who had clinical stage T3a disease. Among the 56 men not treated with neoadjuvant or adjuvant therapies before prostate‐specific antigen (PSA) recurrence, the long‐term outcomes of PSA‐free survival, metastasis‐free survival, and prostate cancer specific survival were examined. Median and mean follow‐up after surgery were 10.3 and 13 years, respectively (range, 1–17).Ninety‐one percent of men in this group had pathological T3 disease. PSA‐free survival at 15 years after surgery was 49%. Metastasis‐free survival and cause‐specific survival at 15 years after surgery were 73% and 84%, respectively. Among men with a PSA recurrence, 46% received secondary therapy before metastasis. The only preoperative or pathological feature that predicted risk of prostate cancer death was lymph node metastasis (hazard ratio [HR]: 9.22, 95% confidence interval [CI]: 1.06–80.02, P = .044). Among the 28 men with a PSA recurrence, PSA doubling time (PSADT) data were available for 23, of which 11 (48%) has a PSADT ≥9 months. No patient with a PSADT ≥9 months died of prostate cancer. A PSADT <9 months was significantly associated with increased risk of prostate cancer death (log‐rank, P = .004).In a select cohort of men with clinical stage T3a disease, radical prostatectomy alone provides long‐term cancer control in about half of the men and results in a prostate cancer‐specific survival of 84%. Among men with a PSA recurrence, PSADT at the time of recurrence is a useful determinant of risk of prostate cancer death. Cancer 2007. © 2007 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published

2007

2. Germline ATBF1 mutations and prostate cancer risk.

Author

Junyan Xu, Jurga Sauvageot, Charles M. Ewing, Jielin Sun, Wennuan Liu, Sarah D. Isaacs, Kathleen E. Wiley, Lina Diaz, S. Lilly Zheng, Patrick C. Walsh, and William B. Isaacs

Published

2006

3. Genome-wide screen for prostate cancer susceptibility genes in men with clinically significant disease.

Author

Bao-Li Chang, Sarah D. Isaacs, Kathy E. Wiley, Elizabeth M. Gillanders, S. Lilly Zheng, Deborah A. Meyers, Patrick C. Walsh, Jeffrey M. Trent, Jianfeng Xu, and William B. Isaacs

Published

2005

4. Trefoil factor 3 overexpression in prostatic carcinoma: Prognostic importance using tissue microarrays.

Author

Dennis A. Faith, William B. Isaacs, James D. Morgan, Helen L. Fedor, Jessica L. Hicks, Leslie A. Mangold, Patrick C. Walsh, Alan W. Partin, Elizabeth A. Platz, Jun Luo, and Angelo M. De Marzo

Published

2004

5. Mutational analysis of PINX1 in hereditary prostate cancer.

Author

Gregory A. Hawkins, Bao‐Li Chang, S. Lilly Zheng, Sarah D. Isaacs, Kathleen E. Wiley, Eugene R. Bleecker, Patrick. C. Walsh, Deborah A. Meyers, Jianfeng Xu, and William B. Isaacs

Published

2004

6. Biochemical failure after radical prostatectomy in men with pathologic organ-confined disease: pT2a versus pT2b.

Author

Stephen J. Freedland, Alan W. Partin, Jonathan I. Epstein, and Patrick C. Walsh

Published

2004

7. UROLOGICAL ONCOLOGY: PROSTATE CANCER.

Author

Patrick C. Walsh

Published

2004

8. Quantitative alterations in nuclear structure predict prostate carcinoma distant metastasis and death in men with biochemical recurrence after radical prostatectomy.

Author

Masood A. Khan, Patrick C. Walsh, M. Craig Miller, Wesley D. Bales, Jonathan I. Epstein, Leslie A. Mangold, Alan W. Partin, and Robert W. Veltri

Published

2003

9. Genome-wide scan for prostate cancer susceptibility genes in the Johns Hopkins hereditary prostate cancer families(Jianfeng Xu and Elizabeth M. Gillanders contributed equally to this study.).

Author

Jianfeng Xu, Elizabeth M. Gillanders, Sarah D. Isaacs, Bao-li Chang, Kathy E. Wiley, S. Lilly Zheng, MaryPat Jones, Derek Gildea, Erica Riedesel, Julie Albertus, Diana Freas-Lutz, Carol Markey, Deborah A. Meyers, Patrick C. Walsh, Jeffrey M. Trent, and William B. Isaacs

Published

2003

10. Decreased gene expression of steroid 5 alpha-reductase 2 in human prostate cancer: Implications for finasteride therapy of prostate carcinoma.

Author

Jun Luo, Thomas A. Dunn, Charles M. Ewing, Patrick C. Walsh, and William B. Isaacs

Published

2003

11. Polymorphisms in the CYP1A1 gene are associated with prostate cancer risk.

Author

Bao-li Chang, Siqun L. Zheng, Sarah D. Isaacs, Aubrey Turner, Gregory A. Hawkins, Kathy E. Wiley, Eugene R. Bleecker, Patrick C. Walsh, Deborah A. Meyers, William B. Isaacs, and Jianfeng Xu

Subjects

PROSTATE cancer & genetics, GENETIC polymorphisms, CANCER risk factors, ETIOLOGY of diseases, METABOLITES, XENOESTROGENS

Abstract

CYP1A1 is likely to play an important role in the etiology of CaP through its function in activating environmental procarcinogens and catalyzing the oxidative metabolites of estrogens. To test the hypothesis that genetic polymorphisms in the CYP1A1 gene may be associated with the risk for CaP, we compared the allele, genotype and haplotype frequencies of 3 SNPs (3801T>C, 2455A>G and 2453C>A) of CYP1A1 among 159 HPC probands, 245 sporadic CaP cases and 222 unaffected men. Two SNPs (3801T>C and 2455A>G) were each individually associated with CaP risk when the allele and genotype frequencies were compared between CaP patients and unaffected controls. Furthermore, a combined SNP analysis using a haplotype approach revealed an even stronger association in Caucasians. Specifically, 4 major haplotypes (T-A-C, C-A-C, C-G-C and T-A-A) accounted for 99.8% of all observed haplotypes. These 4 haplotypes correspond to the previously described nomenclature (CYP1A1*1A, CYP1A1*2A, CYP1A1*2B and CYP1A1*4). The frequencies of these 4 haplotypes were significantly different among CaP patients and controls. The haplotype T-A-C (CYP1A1*1A) was significantly associated with increased risk for CaP, and the haplotype C-A-C (CYP1A1*2A) was significantly associated with decreased risk for CaP. These findings suggest that genetic polymorphisms in CYP1A1 may modify the risk for CaP. © 2003 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2003

12. Evaluation of SRD5A2 sequence variants in susceptibility to hereditary and sporadic prostate cancer.

Author

Bao-li Chang, S. Lilly Zheng, Sarah D. Isaacs, Aubrey R. Turner, Eugene R. Bleecker, Patrick C. Walsh, Deborah A. Meyers, William B. Isaacs, and Jianfeng Xu

Published

2003

13. Family history of prostate cancer and obesity in relation to high-grade disease and extraprostatic extension in young men with prostate cancer.

Author

Sabine Rohrmann, William W. Roberts, and Patrick C. Walsh

Published

2003

14. RE: ULTRASENSITIVE SERUM PROSTATE SPECIFIC ANTIGEN NADIR ACCURATELY PREDICTS THE RISK OF EARLY RELAPSE AFTER RADICAL PROSTATECTOMY.

Author

Patrick C Walsh

Published

2005

15. RE: VARIATION IN CONTINENCE AND POTENCY BY DEFINITION.

Author

Patrick C. Walsh

Published

2004