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17 results on '"Dickman, Paul S."'

1. Indolent course of advanced neuroblastoma in children older than 6 years at diagnosis

Author

Blatt, Julie, Gula, Mary J., Orlando, Salvatore J., Finn, Laura S., Misra, Dhirendra N., and Dickman, Paul S.

Subjects
Neuroblastoma -- Development and progression, Tumors in children -- Development and progression, Health
Abstract

Background. An early observation suggests that children older than 6 years of age at diagnosis of neuroblastoma constitute a favorable prognostic group. Methods. Kaplan-Meier plots of survival of all such patients diagnosed at the Children's Hospital of Pittsburgh 1975-1992 were compared with curves of concurrently treated patients with Stage IV disease who were 1-6 years of age at diagnosis ('younger patients'). Known prognostic features, including stage and primary site of disease, pattern of metastases, histopathology, MYCN gene amplification, and urinary catecholamine metabolite ratios, were reviewed. Results. Of 17 children diagnosed after the age of 6 years ('older patients'), 13 patients had Evans' Stage IV disease and 4 had Stage III disease. The median survival was 3.24 years (range, 0.63-15.04 years) for the entire cohort and 3.07 years for those children with Stage IV disease. This compared with a median survival of 1.05 years in 34 concurrent younger patients (P < 0.01). In most cases, disease in these older patients was characterized by a short-lived complete or partial remission followed by aggressive recurrent disease that was partially and only transiently chemo- or radiosensitive. Only 3 patients (2 with Stage IV disease) are in continuous complete remission at 3, 5 10/12, and 14 1/2 years from diagnosis. Although poor prognostic factors were common, including the presence of bony metastases (12/17), biopsy material from pretreatment tumor specimens demonstrated a single MYCN gene copy number in all patients and favorable histology in 15 of 16 samples. Conclusion. Older children with neuroblastoma have a more indolent course than do younger patients, a finding that appears to be related to favorable histology and the absence of MYCN amplification. Examination of larger numbers of such patients from cooperative groups should lead to a better understanding of what appears to be a subset of pediatric patients with neuroblastoma who may benefit from specifically tailored treatment protocols. Cancer 1995; 76:890-4. Key words: neuroblastoma, pediatric oncology, MYCN, childhood.

Published
1995

2. The Intergroup Rhabdomyosarcoma Study-II

Author

Maurer, Harold M., Gehan, Edmund A., Beltangady, Mohan, Crist, William, Dickman, Paul S., Donaldson, Sarah S., Fryer, Christopher, Hammond, Denman, Hays, Daniel M., Herrmann, Janice, Heyn, Ruth, Jones, Pat Morris, Lawrence, Walter, Newton, William, Ortega, Jorge, Ragab, Abdelsalam H., Raney, R. Beverly, Ruymann, Frederick B., Soule, Edward, Tefft, Melvin, Webber, Bruce, Wiener, Eugene, Wharam, Moody, and Vietti, Teresa J.

Subjects
Rhabdomyosarcoma -- Care and treatment, Cancer in children -- Care and treatment, Health
Abstract

Background. Intergroup Rhabdomyosarcoma Study (IRS)-II, (1978-1984) had the general goals of improving the survival and treatment of children with rhabdomyosarcoma (RMS). Methods. Nine hundred ninety-nine previously untreated eligible patients entered the study after surgery and were randomized or assigned to therapy by IRS Clinical Group (I-IV), tumor site, and histologic type. Outcomes were compared between treatments and with results of IRS-I (1972-1978). Results. Patients in Group I, excluding extremity alveolar (EA) RMS, were randomized to standard vincristine (V), dactinomycin (A), and cyclophosphamide (C) or standard VA. At 5 years, disease-free survival (DFS) and survival (S) rates were similar between VAC and VA (DFS: 80%, 70%, P = 0.47;S: 85%, 84%, P = 0.73). Patients in Group II, excluding EA RMS, received radiation and were randomized to intensive VA or repetitive-pulse VAC. Outcomes were similar for rates of DFS (69%, 74%, P = 0.83) and S (88%, 79%, P = 0.17). Patients in Group III, excluding certain pelvic tumors, received radiation and were randomized to repetitive-pulse VAC or repetitive-pulse VAdrC-VAC (Adr, Adriamycin [doxorubicini]). Complete remission (CR) rates were close at 74%, 78%, respectively (P = 0.32), as were percentages in CR (73%) and S (66%) rates; the latter outcomes were significantly better than IRS-I (CR: 56%, P < 0.001; S: 50%, P < 0.001). Central nervous system prophylaxis for Group III patients with cranial parameningeal sarcoma increased S rate to 67% from 45% in IRS-I (P < 0.001). Patients in Group IV received the same regimens as Group III; the CR rate was 53%, 38% remained in CR and S rate was 27% with and 26% without Adr (P = 0.90). At 5 years, S rate for IRS-II, including EA and all pelvic tumors, was 63%: an 8% increase over IRS-I (P < 0.001). Outcomes by primary site were as good as, or better than, the IRS-I experience. Conclusions. Combining all Groups and treatments in IRS-II, the major improvement in S rate at 5 years between studies was in nonmetastatic patients (71% for IRS-II versus 63% for IRS-I, P = 0.01). Cancer 1993; 71:1904-22.

Published
1993

4. Ewing’s Sarcoma/Primitive Neuroectodermal Tumor of the Proximal Humeral Epiphysis

Author

Morris, Parisa, Dickman, Paul S., and Seidel, Matthew J.

Abstract

Ewing’s sarcoma/primitive neuroectodermal tumor (ES/PNET) of bone is a rare childhood tumor most commonly located in the metadiaphysis. In skeletally immature patients, lesions of the epiphysis are rarely malignant, with the most common diagnosis being chondroblastoma. This article presents a case of ES/PNET of the proximal humeral epiphysis in a 12-year-old boy. To the authors’ knowledge, this is the first reported case of epiphyseal ES/PNET confirmed with molecular testing. Radiographs of the patient’s painful shoulder showed a well-defined lytic lesion within the humeral epiphysis. Magnetic resonance imaging suggested a chondroid tumor with surrounding edema. Based on the imaging characteristics, the patient’s age, and the lesion’s location, a preliminary diagnosis of chondroblastoma was made. A trochar biopsy of the lesion demonstrated a small, round, blue cell tumor on frozen section. Subsequently, immunohistochemical staining was uniformly positive in a membrane pattern for CD99, and molecular diagnostic testing demonstrated a EWSR1/FLI1 fusion transcript, confirming the pathologic diagnosis of ES/PNET. Although metadiaphyseal locations for ES/PNET are most common, this case adds to previously reported cases of epiphyseal ES/PNET, suggesting that the diagnosis be considered for pediatric epiphyseal tumors. This case also demonstrates why following rigorous oncologic treatment algorithms by obtaining a limited trochar biopsy, even in the case of a confident radiographic diagnosis, is critically important; the biopsy results can lead to a major change in treatment and avoid contamination of a larger area of soft tissue and bone.

Published
2013
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5. Ewing Sarcoma/Peripheral Primitive Neuroectodermal Tumor and Related Tumors

Author

Tsokos, Maria, Alaggio, Rita D., Dehner, Louis P., and Dickman, Paul S.

Abstract

Ewing sarcoma/peripheral primitive neuroectodermal tumor (EWS/pPNET) and other tumors with EWS gene rearrangements encompass a malignant and intermediate neoplasm with a broad anatomic distribution and a wide age range but a predilection for soft tissue in children, adolescents, and young adults. The overlapping histologic, immunohistochemical and cytogenetic and molecular genetic features create diagnostic challenges despite significant clinical and prognostic differences. Ewing sarcoma is the 3rd most common sarcoma in children and adolescents, and desmoplastic small round cell tumor is a rare neoplasm that occurs more often in older children, adolescents, and young adults. Pathologic examination is complemented by immunohistochemistry, cytogenetics, and molecular genetics. This article reviews the clinicopathologic features of EWS/pPNET and desmoplastic small round cell tumor in the spectrum of tumors with EWS gene rearrangements. Other tumors with different histopathologic features and an EWS gene rearrangement are discussed elsewhere in this volume.

Published
2012
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6. Therapy-related myelodysplasia and acute myeloid leukemia after Ewing sarcoma and primitive neuroectodermal tumor of bone: a report from the Children's Oncology Group

Author

Bhatia, Smita, Krailo, Mark D., Chen, Zhengjia, Burden, Laura, Askin, Frederic B., Dickman, Paul S., Grier, Holcombe E., Link, Michael P., Meyers, Paul A., Perlman, Elizabeth J., Rausen, Aaron R., Robison, Leslie L., Vietti, Teresa J., and Miser, James S.

Abstract

This study describes the magnitude of risk of therapy-related myelodysplasia and acute myeloid leukemia (t-MDS/AML) in 578 individuals diagnosed with Ewing sarcoma and enrolled on Children's Oncology Group therapeutic protocol, INT-0091. Between 1988 and 1992, patients with or without metastatic disease were randomized to receive doxorubicin, vincristine, cyclophosphamide, and dactinomycin (regimen A) or these 4 drugs alternating with etoposide and ifosfamide (regimen B). Between 1992 and 1994, patients with metastatic disease were nonrandomly assigned to receive high-intensity therapy (regimen C: regimen B therapy with higher doses of doxorubicin, cyclophosphamide, and ifosfamide). Median age at diagnosis of Ewing sarcoma was 12 years, and median length of follow-up, 8 years. Eleven patients developed t-MDS/AML, resulting in a cumulative incidence of 2% at 5 years. While patients treated on regimens A and B were at a low risk for development of t-MDS/AML (cumulative incidence: 0.4% and 0.9% at 5 years, respectively), patients treated on regimen C were at a 16-fold increased risk of developing t-MDS/AML (cumulative incidence: 11% at 5 years), when compared with those treated on regimen A. Increasing exposure to ifosfamide from 90 to 140 g/m2, cyclophosphamide from 9.6 to 17.6 g/m2, and doxorubicin from 375 to 450 mg/m2 increased the risk of t-MDS/AML significantly.

Published
2007
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7. The Frozen Section Yesterday and Today: Pediatric Solid Tumors—Crucial Issues

Author

Fisher, John E., Burger, Peter C., Perlman, Elizabeth J., Dickman, Paul S., Parham, David M., Savell, Van H., Hutchison, Robert E., Paidas, Charles N., and Lev, Elaine Rappaport

Abstract

This article is the offshoot of a Pediatric Oncology Group (POG) seminar presented at the Adams Mark Hotel, Denver, Colorado, Friday, May 21, 1999, titled “The Frozen Section in Pediatric Solid Tumors—Crucial Issues.” There were eight presenters who spoke on a wide range of topics that included historical perspectives of the frozen section and discussion of the following systems: brain, renal, germ cell, bone, soft tissue, and lymph nodes. To complement these presentations, a pediatric surgeon explained his concern and philosophy regarding the use of frozen sections, and a lawyer tackled the issues and risks in rendering a frozen section diagnosis. We think that this review covers all the important aspects of the frozen section in our current practice of pediatric pathology.

Published
2001
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8. Ewing's SarcomaPrimitive Neuroectodermal Tumor

Author

Dickman, Paul S.

Abstract

Ewing's sarcomaprimitive neuroectodermal tumor ESPNET is a neoplasm that typically occurs in the first and second decades of life but may present from infancy to late middle age. ESPNET generally arises in bone or soft tissue, and examples have been described at most sites. The pathologic nature is defined by a combination of histology, immunohistochemistry, ultrastructure, and molecular genetic abnormalities. The lesions variously termed Ewing's sarcoma, peripheral primitive neuroectodermal tumor, peripheral neuroepithelioma, peripheral neuroblastoma, and Askin tumor have been characterized in the past as distinct entities. However, currently all are considered to be members of a common tumor family, the ESPNET group, which share a limited set of genetic abnormalities defined by fusions of the EWS gene on chromosome 22 with a member of the ets family of transcription factors, most commonly the FLI1 gene on chromosome 11. Neural differentiation is often expressed by ESPNET, representing the PNET end of the morphologic spectrum. This feature has been linked with clinical outcome, but differences in behavior on the basis of histology are largely overshadowed by clinical prognostic factors older age, larger size, central site, and presence of metastases all correlate much more powerfully with poor outcome than any single pathologic feature. Recently, specific differences in chromosomal breakpoint fusion type have been closely related to clinical outcome, and this relationship holds great promise for prognostication in the future.

Published
2000

9. A Sibship With Hypokalemic Alkalosis and Renal Proximal Tubulopathy

Author

Güllner, Hans-Georg, Bartter, Frederic C., Gill, John R., Dickman, Paul S., Wilson, Curtis B., and Tiwari, Jawahar L.

Abstract

• A new syndrome, characterized by hypokalemic alkalosis, hyperreninemia, aldosterone, high urinary prostaglandin E2 excretion, normal BP, and resistance of BP to angiotensin II is described in three of four siblings. Histologic examination of tissue obtained by biopsy from the kidneys showed an intense staining of the proximal tubular cells, as well as an extreme hypertrophy of the proximal tubular basement membranes, features that previously have not been observed. On electron microscopic examination, the characteristic changes of the tubular cells consisted of very dense cytoplasm, compact mitochondria, and pyknotic nuclei. In contrast to Bartter's syndrome, the juxtaglomerular apparatus were of normal appearance. Glomerular filtration rate and renal plasma flow were within normal limits. Fractional distal delivery of proximal tubular solute and fractional chloride reabsorption in the thick ascending limb of the loop of Henle were normal. The findings of a genetic linkage between the syndrome and the major histocompatibility system suggests that this familial tubulopathy is an inherited disorder.(Arch Intern Med 1983;143:1534-1540)

Published
1983
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12. Gonadoblastoma

Author

Reuben, Blair I., Dickman, Paul S., Koyle, Martin, and Rajfer, Jacob

Abstract

We report a patient with a disorder of sexual differentiation who presented with a 46, XY karyotype, absent internal Müüllerian ducts, a vaginal pouch, hypospadias, and bilateral cryptorchidism with a gonadoblastoma in one testis. A human chorionic gonadotropin stimulation test and tissue 5-alpha-reductase and androgen receptor assays were normal. Except for the absence of internal Müüllerian ducts, this patient most closely resembles the disorder of dysgenetic male pseudohermaphroditism (DMP). On this basis, we hypothesize that the internal Müüllerian ducts in DMP may manifest anywhere along a spectrum that extends from normal to complete absence of structures depending on the degree of gonadal dysgenesis. This case also illustrates the importance of testicular biopsy in patients with dysgenetic testes because of the high likelihood of germ cell neoplasms in these gonads.

Published
1987
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15. Neuroblastoma Mimicking Rhabdoid Tumor of the Kidney

Author

Shaw, Peter H. and Dickman, Paul S.

Abstract

Rhabdoid tumor of the kidney (RTK) has mimicked other renal tumors histologically, but there has been only one previous report of neuroblastoma mimicking RTK. The authors present the case of a 17-month-old boy who presented with a large left renal mass that was diagnosed as RTK. At the completion of therapy he was found to have residual masses. They were biopsied and found to be viable neuroblastoma.

Published
2003

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