Frequency of Certain Established Risk Factors in Soft Tissue Sarcomas in Adults: A Prospective Descriptive Study of 658 Cases

Penel, Nicolas; Grosjean, Jessica; Robin, Yves Marie; Vanseymortier, Luc; Clisant, Stéphanie; Adenis, Antoine

doi:https://doi.org/10.1155/2008/459386

Sarcoma

On this page

Abstract Introduction Methods Results Discussion References Copyright Related Articles

Clinical Study | Open Access

Volume 2008 | Article ID 459386 | https://doi.org/10.1155/2008/459386

Frequency of Certain Established Risk Factors in Soft Tissue Sarcomas in Adults: A Prospective Descriptive Study of 658 Cases

Nicolas Penel,¹Jessica Grosjean,¹Yves Marie Robin,²Luc Vanseymortier,^1,3Stéphanie Clisant,⁴and Antoine Adenis³

Academic Editor: Ole Nielsen

Received19 Jun 2007

Revised20 Jan 2008

Accepted06 Mar 2008

Published11 May 2008

Abstract

Soft tissue sarcomas are rare tumours with infrequent identified aetiological factors. Several genetic syndromes as well as previous radiation therapy and/or chronic lymphoedema have been suspected to predispose to some soft tissue sarcomas. Between January 1997 and September 2005, we carried out a prospective descriptive study to estimate the frequency of some particular etiological factors among 658 patients with soft tissue sarcomas. Sarcomas associated with a clinically identified genetic disease represent 2.8% out of all cases (95%CI: 1.5–3.8%). Most of these cases (14/19) are related to Recklinghausen neurofibromatosis. Radiation-induced sarcomas represent 3.3% out of all cases (95%CI: 1.7–5.1%). Most of these cases (9/22) are related to prior breast cancer treatment. We had observed only 1 case of Stewart-Treves syndrome. Liposarcoma, the most frequent histological subtype observed, is not associated with any particular aetiological entity. Finally, most of the adult soft tissue sarcomas are not related to any classical clinically identified genetic disease or previous radiation therapy and/or chronic lymphoedema risk factors. Frequency of underlying genetic syndrome which may predispose to soft tissue sarcomas could be higher than previously reported.

1. Introduction

Soft tissue sarcomas (STS) are rare tumours. Their estimated incidence is close to 3–4.5/100 000 [1, 2]. Most of these cancers had no clearly defined cause but several infrequent predisposing factors have been described, such as genetic predisposition (including mainly Recklinghausen disease and bilateral retinoblastoma) and iatrogenic factors (postirradiation sarcoma and postoperative chronic lymphoedema) [1, 2]. Several previous studies have been conducted on this topic, but have been focused on only one of these particular risk factors. There is no recent study analyzing the frequency of all these risk factors on the same cohort of patients. In order to estimate the frequency of these specific factors in adults with STS, we carried out along a 105-month period a prospective study on all new consecutive cases treated in a single institution located in Northern France area (4 millions inhabitants).

2. Patients and Methods

2.1. Patients

We have prospectively collected some clinical characteristics of all new consecutive cases of adult (over 18 years old) (STS) treated at the Northern France Comprehensive Cancer centre (namely, Centre Oscar Lambret) between January 1997 and September 2005. Three kinds of tumours were excluded from this study, because these cases were not (Kaposi tumours, mixed mullerian tumours of uterus) or very recently (GIST) treated in our institution.

2.2. Data Collection

The database included age at diagnosis, gender, tumour location, histological subtype, grade (according to the Fédération Nationale des Centres de Lutte Contre le Cancer System [3]), association with genetic syndrome, previous or synchronous other malignancy, postoperative lymphoedema (Stewart-Treves Syndrome), or postirradiation sarcoma.

A pathological review or a histological diagnosis established in a reference centre is available in all cases (658). The grade is available in 384 cases (58%).

2.3. Definitions

The diagnosis of genetic syndrome was based on familial history criteria and clinical and phenotypic criteria [4–9]. For example, a patient meeting two or more of the following criteria can be diagnosed as suffering from Recklinghausen’s neurofibromatosis: (i) neurofibromas (two or more, or one plexiform neurofibroma), (ii) “café-au-lait” macules (six or more measuring 1.5 cm in their greatest dimension), (iii) freckling in the axillary’s or inguinal areas, (iv) optic glioma, (v) iris hamartomas (two or more), (vi) sphenoid dysplasia (or thinning of the cortex of the long bones), and (vii) first-degree relative [4]. The other syndromes expected were: Li-Fraumeni syndrome [5], bilateral retinoblastoma syndrome [6], Gardner syndrome or familial polyposis adenomatous [7], adult progeria [8], and Gorlin syndrome [9].

The diagnosis of radiation-induced sarcoma was based on Arlen et al. [10] criteria: (i) histological diagnosis of sarcoma, (ii) different histological diagnosis of the previous cancer, (iii) tumour in the border of radiation field, and (iv) a minimal time interval of 3 years.

2.4. Statistical Analysis

The description of population is based on crude incidence with 95%-confidence interval for categorical parameters, median and extreme values, or mean and standard deviation for continuous parameters. The comparisons are based on Fisher exact test for categorical data and Mann-Whitney test for continuous parameters. The significance was set up at 5%.

3. Results

3.1. All New Cases Treated between January 1997 and October 2005

The entire population included 658 cases. The sex ratio male/female was 309/349 (excluding uterus sarcoma, the sex ratio was 309/308). At diagnosis, the median age was 52 (range, 18–99). The most common histological subtypes were liposarcomas (20%), leiomyosarcomas (17%), malignant fibrous histiocytofibromas (11%), and undifferentiated sarcomas (10%). The grade was 1 in 25% of cases, 2 in 26%, and 3 in 48%. The tumour locations are listed in Table 1. The main locations were lower limbs (34%), chest wall (15%), upper limbs (13%), and retroperitoneum (10%).

3.2. STS Associated with Genetic Syndrome

Nineteen patients suffered from a genetic syndrome and represented 2.8% out of all cases (IC95%: 1.5–3.8%). Most common genetic syndromes were Recklinghausen neurofibromatosis (14 cases) and bilateral retinoblastoma (2 cases). In this subpopulation, the sex ratio was 13/6 and the median age at diagnosis was 37.5 (range, 18–64). Locations, histological subtype, and grade are listed in Table 2.

At diagnosis, these STS associated with genetic syndrome were significantly younger than the entire cohort (Median age 37.5 versus 53 years, ). In comparison with other cases, these patients were more frequently located on trunk and were more frequently peripheral malignant nerve sheath tumours . On the contrary, liposarcomas were significantly less frequent in STS associated with genetic syndrome .

3.3. Stewart-Treves Syndrome

We had observed only one case of angiosarcoma associated with previous lymphoedema as a consequence of surgical treatment of a previous breast cancer.

3.4. Radiation-Induced Soft Tissue Sarcomas

Twenty two radiation-induced STSs were observed. Location, histological subtypes, and grade are listed in Table 3. The mean interval from the first cancer was 10 years (range, 3–45 years). The most common previous cancers were breast cancers (10 cases) and non-Hodgkin lymphomas (4 cases). At diagnosis, the patients were significantly older than the entire cohort (median age 66 versus 53 years, ). In comparison with other cases, the radiation-induced were more frequently located on chest wall and were more frequently undifferentiated spindle cell sarcoma or angiosarcoma . On the contrary, liposarcomas were significantly less frequent in radiation-induced sarcoma group .

4. Discussion

In this prospective study of 658 adult STS, about 6% of patients present a well-established risk factor: a genetic syndrome (2.8%) or an iatrogenic factor such as previous radiation therapy (3.3%) or a postoperative chronic lymphoedema (1 case). The characteristics of our entire group of patients are consistent literature; the sex ratio is closed to 1 [1, 2], the median age is 55 years [1], lower and upper limbs locations are the most frequent, liposarcomas and leiomyosarcoma are the most common histological subtypes (after excluding malignant fibrous histiocytofibroma), and grade 3 tumours are the most frequent [11, 12].

Twenty two cases out of 658 (3.3%, 95% CsI: 1.7–5.1%) present a radiation-induced STS. In longitudinal studies, the prevalence of radiation-induced sarcomas is very low, close to 0.14–0.20% [13–15]. After treatment by radiotherapy, the relative risk for development of STS is comprised between 8 and 50 [10, 13, 14]. As previously published [16], in our series, breast cancers and lymphomas were the most frequent previous primaries treated with radiation therapy. Radiation-induced sarcomas are more frequently STS (70%) than osseous sarcomas (30%) [16]. Malignant fibrous histiocytofibromas (16% in the Brady et al. series) and angiosarcomas (15%) are the most common histological subtype of radiation-induced STS. The liposarcomas are exceptional [16]. In the Weiss and Enzinger series, about 10% of angiosarcomas are radio-induced [17]. Radiation-induced STS are usually high-grade tumours, for example, in the Brady’s series, less than 6% of radio-induced sarcomas are grade 1 [18]. The radiation-induced sarcomas are usually developed at the peripheral borders of radiation fields. The mean interval from the first cancer treatment is about 10 years (range, 2 and 67 years) [10, 13–16]. Angiosarcomas seem occur after a shorter interval (about 5 years) [10, 13–15]. The interval is also shorter in cases associated with Bilateral Retinoblastoma [6].

The Stewart-Treves syndrome is defined as the development of angiosarcoma or lymphangiosarcoma on chronic lymphoedema whatever its cause (congenital, postsurgical, or caused by filariosis, ...) [18]. The Stewart-Treves syndrome is exceptional and about 300 cases are known in literature. Most of cases (168/186) are observed after axillary’s clearance for breast cancer [19]. In the Connecticut Registry, 8 cases are diagnosed after the treatment of more than 41000 breast cancers [20]. The mean interval is about 10 years (4–27) for cases secondary to breast cancer treatment [18, 19, 21]. The Stewart-Treves syndrome represents about 5% of all angiosarcomas [18, 19, 21].

In contrast to literature that describes STS are classically related to genetic syndromes in less than 1% [1] this study shows that 2.8% [1.5–3.8] of our patients suffered from a clinically-diagnosed genetic syndrome. Recklinghausen neurofibromatosis and bilateral retinoblastoma predominate. Other genetic syndromes (Li-Fraumeni syndrome, Gardner syndrome, ataxia-telangiectasia, and progeria) appear exceptional. We had no clear explanation to the present higher than previously described frequency of genetic syndrome.

The estimated incidence of Recklinghausen Neurofibromatosis is about 1/3,000–1/5,000. Fifty percent of cases are sporadic [4, 20]. These patients had a relative risk of cancers (including STS and other sarcomas) about 4 in comparison with general population [4, 20]. Cancers are the first cause of precocious deaths in such population. About 5% of patients affected by Recklinghausen Neurofibromatosis develop malignant peripheral nerve sheath tumour (MPNST). The MPNST are usually developed on a neurofibroma [4, 22] and can be multiple [4, 22]. The male predominance is well established (sex ratio 4/1 [23]). The median age at diagnosis of STS is about 32–36, clearly inferior to age diagnosis in general population [22, 23]. Classically, about 40% of MPNST is associated with Recklinghausen Neurofibromatosis [23]. In our experience, 8 out of 24 MPNST are associated with Recklinghausen Neurofibromatosis. The prognosis of MPNST is not influenced by the presence of Recklinghausen Neurofibromatosis; the 5-year overall survival is about 40% [23]. In our study, all findings are consistent with the literature data (male predominance, young age, mainly MPNST).

The present study presents several limitations. Firstly, our study is not exhaustive; because according to estimated incidence (3–4.4/100 000) [1, 2] of adult STS in Western countries, a total number comprised between 1140 and 1670 cases are expected in our region in the same period. In consequence, we estimate that our cohort represent between 44% and 65% of all cases. Secondly, it is a single-centre study and our results may not be directly applicable to other areas in France or abroad. The malignant nature of aggressive fibromatosis is still debated, but more recent reports suggest that a part of these tumours must be considered as a particular form of low-grade fibrosarcoma [24, 25]. Because of recent progress in histology, the proportion of the different histological subtypes must be considered with caution. For example, the “malignant fibrous histiocytofibroma” actually disappears and this diagnosis is modified into dedifferentiated liposarcoma and dedifferentiated leiomyosarcoma [26]. Moreover, the diagnosis of genetic syndromes were based on clinical criteria, a systematic genetic testing can possibly modify those results.

4.1. Conclusion

Most cases of adult STS (94% in our experience) are not related to well-established risk factors (radiation, genetic disease, and chronic lymphedema). Liposarcoma is the most frequent histological subtype, but it is rarely associated with genetic disease or postirradiation. New epidemiological explorations are necessary to analyze, for example, the environmental and occupational risk factors (such as arsenic, phenoxy-herbicides) and new iatrogenic factors (such as new chemotherapy agents and new techniques of radiation therapy) [27–29].

References

S. H. Zahm and J. F. Fraumeni, Jr., “The epidemiology of soft tissue sarcoma,” Seminars in Oncology, vol. 24, no. 5, 504 pages, 1997.
View at: Google Scholar
F. Levi, C. La Vecchia, L. Randimbison, and V.-C. Te, “Descriptive epidemiology of soft tissue sarcomas in Vaud, Switzerland,” European Journal of Cancer, vol. 35, no. 12, 1711 pages, 1999.
View at: Publisher Site | Google Scholar
J.-M. Coindre, P. Terrier, L. Guillou et al., “Predictive value of grade for metastasis development in the main histologic types of adult soft tissue sarcomas: a study of 1240 patients from the French Federation of Cancer Centers Sarcoma Group,” Cancer, vol. 91, no. 10, 1914 pages, 2001.
View at: Publisher Site | Google Scholar
B. Samuelsson and S. Samuelsson, “Neurofibromatosis in Gothenburg, Sweden. I. Background, study design and epidemiology,” Neurofibromatosis, vol. 2, no. 1, 6 pages, 1989.
View at: Google Scholar
T. Frebourg, A. Abel, C. Bonaiti-Pellie et al., “Le syndrome de Li-Fraumeni: mise au point, données nouvelles et recommandations pour la prise en charge,” Bulletin du Cancer, vol. 88, no. 6, 581 pages, 2001.
View at: Google Scholar
R. A. Kleinerman, M. A. Tucker, D. H. Abramson, J. M. Seddon, R. E. Tarone, and J. F. Fraumeni, Jr., “Risk of soft tissue sarcomas by individual subtype in survivors of hereditary retinoblastoma,” Journal of the National Cancer Institute, vol. 99, no. 1, 24 pages, 2007.
View at: Publisher Site | Google Scholar
J. A. Greer, Jr., K. D. Devine, and D. C. Dahlin, “Gardner's syndrome and chondrosarcoma of the hyoid bone,” Archives of Otolaryngology, vol. 103, no. 7, 425 pages, 1977.
View at: Google Scholar
M. Goto, R. W. Miller, Y. Ishikawa, and H. Sugano, “Excess of rare cancers in Werner syndrome (adult progeria),” Cancer Epidemiol Biomarker & Prevention, vol. 5, no. 4, 239 pages, 1996.
View at: Google Scholar
L. Lo Muzio, P. Nocini, P. Bucci, G. Pannone, U. Consolo, and M. Procaccini, “Early diagnosis of nevoid basal cell carcinoma syndrome,” Journal of the American Dental Association, vol. 130, no. 5, 669 pages, 1999.
View at: Google Scholar
M. Arlen, N. L. Higinbotham, A. G. Huvos, R. C. Marcove, T. Miller, and I. C. Shah, “Radiation-induced sarcoma of bone,” Cancer, vol. 28, no. 5, 1087 pages, 1971.
View at: Publisher Site | Google Scholar
W. Lawrence, Jr., W. L. Donegan, N. Natarajan, C. Mettlin, R. Beart, and D. Winchester, “Adult soft tissue sarcomas: a pattern of care survey of the American College of Surgeons,” Annals of Surgery, vol. 205, no. 4, 349 pages, 1987.
View at: Publisher Site | Google Scholar
M. F. Brennan, “The surgeon as a leader in cancer care: lessons learned from the study of soft tissue sarcoma,” Journal of the American College of Surgeons, vol. 182, no. 6, 520 pages, 1996.
View at: Google Scholar
P. Karlsson, E. Holmberg, K.-A. Johansson, L.-G. Kindblom, J. Carstensen, and A. Wallgren, “Soft tissue sarcoma after treatment for breast cancer,” Radiotherapy and Oncology, vol. 38, no. 1, 25 pages, 1996.
View at: Publisher Site | Google Scholar
G. K. Jacobsen, A. Mellemgaard, S. A. Engelholm, and H. Moller, “Increased incidence of sarcoma in patients treated for testicular seminoma,” European Journal of Cancer, vol. 29, no. 5, 664 pages, 1993.
View at: Publisher Site | Google Scholar
F. E. van Leeuwen, W. J. Klokman, A. Hagenbeek et al., “Second cancer risk following Hodgkin's disease: a 20-year follow-up study,” Journal of Clinical Oncology, vol. 12, no. 2, 312 pages, 1994.
View at: Google Scholar
M. S. Brady, J. J. Gaynor, and M. F. Brennan, “Radiation-associated sarcoma of bone and soft tissue,” Archives of Surgery, vol. 127, no. 12, 1379 pages, 1992.
View at: Google Scholar
S. W. Weiss and F. M. Enzinger, “Malignant fibrous histiocytoma. An analysis of 200 cases,” Cancer, vol. 41, no. 6, 2250 pages, 1978.
View at: Publisher Site | Google Scholar
P. Roy, M. A. Clark, and J. M. Thomas, “Stewart-Treves syndrome—treatment and outcome in six patients from a single centre,” European Journal of Surgical Oncology, vol. 30, no. 9, 982 pages, 2004.
View at: Publisher Site | Google Scholar
Y. M. Kirova, L. Gambotti, Y. De Rycke, J. R. Vilcoq, B. Asselain, and A. Fourquet, “Risk of second malignancies after adjuvant radiotherapy for breast cancer: a large-scale, single-institution review,” International Journal of Radiation Oncology Biology Physics, vol. 68, no. 2, 359 pages, 2007.
View at: Publisher Site | Google Scholar
S. A. Sorensen, J. J. Mulvihill, and A. Nielsen, “Long-term follow-up of von Recklinghausen neurofibromatosis. Survival and malignant neoplasms,” New England Journal of Medicine, vol. 314, no. 16, 1010 pages, 1986.
View at: Google Scholar
E. B. Harvey and L. A. Brighton, “Second cancer following cancer of the breast in Connecticut, 1935–82,” Journal of the National Cancer Institute, vol. 68, 99 pages, 1985.
View at: Google Scholar
J. G. Guccion and F. M. Enzinger, “Malignant schwannoma associated with von Recklinghausen's neurofibromatosis,” Virchows Archiv, vol. 383, no. 1, 43 pages, 1979.
View at: Publisher Site | Google Scholar
R. H. Hruban, M. H. Shiu, R. T. Senie, and J. M. Woodruff, “Malignant peripheral nerve sheath tumors of the buttock and lower extremity. A study of 43 cases,” Cancer, vol. 66, no. 6, 1253 pages, 1990.
View at: Publisher Site | Google Scholar
D. Kotiligam, A. J. Lazar, R. E. Pollock, and D. Lev, “Desmoid tumor: a disease opportune for molecular insights,” Histology and Histopathology, vol. 23, no. 1, 117 pages, 2008.
View at: Google Scholar
M. Gega, H. Yanagi, R. Yoshikawa et al., “Successful chemotherapeutic modality of doxorubicin plus dacarbazine for the treatment of desmoid tumors in association with familial adenomatous polyposis,” Journal of Clinical Oncology, vol. 24, no. 1, 102 pages, 2006.
View at: Publisher Site | Google Scholar
J. A. Bridge and A. A. Sandberg, “Cytogenetic and molecular genetic techniques as adjunctive approaches in the diagnosis of bone and soft tissue tumors,” Skeletal Radiology, vol. 29, no. 5, 249 pages, 2000.
View at: Publisher Site | Google Scholar
M. Kogevinas, T. Kauppinen, R. Winkelmann et al., “Soft tissue sarcoma and non-Hodgkin's lymphoma in workers exposed to phenoxy herbicides, chlorophenols, and dioxins: two nested case-control studies,” Epidemiology, vol. 6, no. 4, 396 pages, 1995.
View at: Publisher Site | Google Scholar
P. C. Valery, G. Williams, A. C. Sleigh, E. A. Holly, N. Kreiger, and C. Bain, “Parental occupation and Ewing's sarcoma: pooled and meta-analysis,” International Journal of Cancer, vol. 115, no. 5, 799 pages, 2005.
View at: Publisher Site | Google Scholar
B. D. Cheson, D. A. Vena, J. Barrett, and B. Freidlin, “Second malignancies as a consequence of nucleoside analog therapy for chronic lymphoid leukemias,” Journal of Clinical Oncology, vol. 17, no. 8, 2454 pages, 1999.
View at: Google Scholar

Copyright

Copyright © 2008 Nicolas Penel et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

PDF Download Citation

Download other formats

Order printed copies

Views

2030

Downloads

1524

Citations