Epidemiological and clinical aspects of pelvic endometriosis: series of cases

Bellelis, Patrick; Dias Jr, João Antônio; Podgaec, Sergio; Gonzales, Midgley; Baracat, Edmund Chada; Abrão, Maurício Simões

doi:10.1590/S0104-42302010000400022

Abstracts

OBJECTIVE: To describe clinical and epidemiological aspects of patients with pelvic endometriosis who were operated in our service. METHODS: A retrospective study was made of 892 patients submitted to laparoscopy with histological confirmation of diagnosis of endometriosis. RESULTS: The mean age was 33.2 ± 6.3 years and 78.7% were Caucasian. We found that 76.9% of women had higher education. 56.5% of patients were nulliparous and 62.2% reported dysmenorrhea as the main complaint. Chronic pelvic pain was the most prevalent symptom, followed by deep dyspareunia, mentioned by 56.8% and 54.7% of patients, respectively. Infertility was reported by 39.8% of the 892 patients. CONCLUSION: Endometriosis is a disease diagnosed in the 4th decade of life, of patients who have multiple complaints . They must always be questioned to properly orient diagnosis and monitor results of treatment.

Endometriosis; Epidemiology; Dyspareunia; Pelvic Pain

OBJETIVO: Descrever aspectos clínicos e epidemiológicos das pacientes portadoras de endometriose pélvica operadas em nosso serviço. MÉTODOS: Estudo retrospectivo de 892 pacientes submetidas a videolaparoscopia com confirmação histológica do diagnóstico de endometriose. RESULTADOS: A média de idade foi de 33,2 ± 6,3 anos, sendo 78,7% brancas. Observamos 76,9% de mulheres com 2º ou 3º graus completos; 56,5% das pacientes eram nulíparas e 62,2% relataram dismenorreia como principal queixa. A dor pélvica crônica foi o sintoma mais prevalente, seguido pela dispareunia de profundidade, sendo referidos por 56,8% e 54,7% das pacientes, respectivamente. A infertilidade foi referida por 39,8% das 892 pacientes. CONCLUSÃO: A endometriose é uma doença geralmente diagnosticada na 4º década da vida das pacientes, as quais apresentam queixas clínicas relacionadas com frequência à dor pélvica e infertilidade, que devem sempre ser questionadas para orientar a hipótese diagnóstica.

Endometriose; Epidemiologia; Dispareunia; Dor pélvica

ORIGINAL ARTICLE

Epidemiological and clinical aspects of pelvic endometriosis a case series

Patrick Bellelis^I,^*; João Antônio Dias Jr^I; Sergio Podgaec^I,II; Midgley Gonzales^I,II; Edmund Chada Baracat^III; Maurício Simões Abrão^IV

^IMédicos Assistentes do Setor de Endometriose da disciplina de Ginecologia do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo HCFMUSP, São Paulo, SP

^IIDoutor em ginecologia pela Faculdade de Medicina da Universidade de São Paulo HCFMUSP, São Paulo, SP

^IIILivre-docente - Professor Titular da Disciplina de Ginecologia da Faculdade de Medicina da Universidade de São Paulo FMUSP, São Paulo, SP

^IVProfessor Livre-docente e Chefe do Setor de Endometriose da Disciplina de Ginecologia da Faculdade de Medicina da Universidade de São Paulo FMUSP, São Paulo, SP

ABSTRACT

OBJECTIVE: To describe clinical and epidemiological aspects of patients with pelvic endometriosis who underwent laparoscopy at our service.

METHODS: Retrospective study of 892 post-laparoscopy patients with histologically confirmed diagnosis of endometriosis.

RESULTS: Mean age was 33.2 ± 6.3 years, and 78.7% of patients were Caucasian. We found that 76.9% of women in the sample had a higher education. Most (56.5%) patients were nulliparous, and 62.2% reported dysmenorrhea as the chief complaint. Chronic pelvic pain was the most prevalent symptom, followed by deep dyspareunia, reported by 56.8% and 54.7% of patients respectively. Infertility was reported by 39.8% of the 892 patients in the sample.

CONCLUSION: Endometriosis is most often diagnosed in the fourth decade of life. Patients with this condition present with multiple complaints, and must always undergo thorough questioning to properly guide diagnosis and monitor treatment results.

Key words: endometriosis. epidemiology. dyspareunia. pelvic pain.

INTRODUCTION

Endometriosis is a common gynecologic condition that affects 5% to 15% of reproductive-age women and up to 3%-5% of postmenopausal women.¹ The number of women with endometriosis is estimated at 7 million in the United States and over 70 million worldwide² and, in industrialized nations, it is one of the foremost gynecologic causes of hospital admission.³

Endometriosis is defined as the implantation of endometrial stroma and;or glandular epithelium at extrauterine sites,⁴ and may involve several structures, including the ovaries, peritoneum, uterosacral ligaments, retrocervical area, rectovaginal septum, rectum, sigmoid colon, terminal ileum, vermiform appendix, bladder, and ureters.^2,3,5,6,7 Although some patients are asymptomatic, most have clinical manifestations of varying intensity. The main symptoms of endometriosis are dysmenorrhea, chronic pelvic pain, infertility, deep dyspareunia, cyclic intestinal and urinary symptoms (such as pain or bleeding on defecation/urination during the menstrual period). Delays in diagnosis may be explained by the nonspecific nature of symptoms and, in some cases, by impaired access to specialized diagnostic modalities..^2,5,8-12. Although some patients are asymptomatic, most have clinical manifestations of varying intensity. The main symptoms of endometriosis are dysmenorrhea, chronic pelvic pain, infertility, deep dyspareunia, cyclic intestinal and urinary symptoms (such as pain or bleeding on defecation/urination during the menstrual period). Delays in diagnosis may be explained by the nonspecific nature of symptoms and, in some cases, by impaired access to specialized diagnostic modalities.^8,13-16 Furthermore, practices that may decrease exposure to estrogen, such as physical exercise and smoking, appear to confer protection^3,17

Some aspects of endometriosis are still the subject of research. Investigations have placed particular emphasis on the etiology and pathogenesis of the condition, as an understanding of the causal mechanisms behind formation of endometriotic lesions would help direct efforts towards improved diagnosis and management.^18,19. For nearly one hundred years, two main etiological hypotheses have sought to explain the pathogenesis of endometriosis:

the coelomic metaplasia theory, which hypothesizes that mesothelial tissue can undergo transformation into endometrial tissue;²⁰.

the retrograde menstruation theory, which posits that retrograde flow of menstrual blood into the abdominal cavity through the Fallopian tubes deposits endometrial cells in extrauterine locations;²¹ implantation would be due to the influence of a favorable hormonal environment and to the failure of immune mechanisms to eliminate these cells from extraneous sites.^22,23.

Furthermore, in recent years, the influence of immunological factors in the pathogenesis of endometriosis has been the subject of extensive research, and many abnormalities have been found; the main immunological mechanism investigated thus far is complementary to the theory of retrograde menstruation. For some as yet unclear reason, endometrial cells entering the endometrial cavity would fail to be eliminated; their permanence would allow migration and implantation, with subsequent development of endometriosis.²⁴

Thus far, few robust studies have attempted to characterize patients with endometriosis. Studies have shown that 2% to 18% of asymptomatic women undergoing tubal ligation are found to meet diagnostic criteria for endometriosis.²⁵ However, much can be learned from characterization of endometriosis patients, as family history, personal history, habits, and lifestyle are all likely to influence disease development. The present study therefore sought to describe the epidemiological and clinical aspects of endometriosis that may help draw an outline of patients with this condition.

METHODS

This case series assessed epidemiological and clinical data from 892 consecutive patients that underwent laparoscopy with histological confirmation of endometriosis at the Endometriosis clinic of the Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo Department of Gynecology between July 1999 and December 2009. The study was approved by the local Research Ethics Committee.

All patients who underwent laparoscopy and received a histologically confirmed diagnosis of endometriosis were enrolled in the series.

Women with chief complaints suggesting endometriosis were assessed by complete history and physical examination. Clinical assessment was supported by complementary imaging tests (transvaginal ultrasound and/or magnetic resonance imaging) as appropriate for suspected endometriomas (chocolate cysts) or deep infiltrating endometriosis. When history and imaging data suggested either type of endometriosis, or when clinical complaints suggested peritoneal endometriosis but imaging modalities failed to confirm the diagnosis, laparoscopy was indicated. Intraoperative biopsy was performed to allow histological confirmation of the clinical diagnosis.

All patients filled out a preoperative questionnaire on demographic data, clinical presentation, chief complaint, prior treatment (when applicable), and personal, obstetric, and family history. The present study focused specifically on objective symptoms, such as dysmenorrhea, chronic pelvic pain, deep dyspareunia, infertility, and cyclical bowel and urinary complaints. Pain was classified into four subtypes: mild, moderate, severe, or incapacitating. Mild pain was defined as that not requiring analgesics for management. Moderate pain was that adequately controlled by home use of over-the-counter analgesics, whereas severe pain required parenteral administration of analgesics in a hospital setting. Incapacitating pain was defined as any pain preventing patients from carrying out their usual activities. Only "severe" and "incapacitating" symptoms were included for statistical analysis purposes. Infertility was defined as couple not being able to conceive after one year of regular, contraceptive-free intercourse. Cyclical intestinal or urinary symptoms were defined as bowel and/or urinary pain and/or bleeding coinciding with menstrual periods.

Data were stored and tabulated with intraoperative and postoperative findings in a Microsoft Office Access® 2004 for Windows database. Statistical analysis was performed with the SPSS 17.0 (2008) software package, using descriptive methods.

RESULTS

Mean patient age was 33.2 ± 6.3 years (mean ± SD). Most patients were white (78.7%) and married or in stable domestic partnerships (69.5%). The prevalence of higher levels of educational attainment was remarkably high; as shown in Table 1, 76.9% of patients in the sample had completed secondary education or obtained a higher degree.

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Approximately 5.3% of patients reported a family history of endometriosis in first-degree relatives. Analysis of obstetric history showed that 56.5% of patients were nulliparous and that, of the 387 remaining patients (43.4%), 191 had been pregnant only once (49.3%).

Tables 2 and 3 show the presenting complaints reported by the 892 patients in the study sample. Table 2 shows the most common chief complaint of patients with endometriosis, whereas Table 3 lists all objective symptoms reported.

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Table 2 shows dysmenorrhea as the most common presenting symptom, with a prevalence of 62.2%. However, when all symptoms were considered rather than the chief complaint alone, chronic pelvic pain and collision dyspareunia were most prevalent, reported by 56.8% and 54.7% of patients respectively. Infertility was also a prevalent symptom, reported by 355 patients (39.8%); however, 237 patients (26.6%) claimed they had never tried to become pregnant.

Table 4 shows the surgical staging of patients in the sample. The prevalence of advanced (stage III and IV) disease was 66.4%, showing the severity of endometriosis in patients treated at our service.

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DISCUSSION

Endometriosis is rare before menarche, and its frequency tends to decrease after menopause.^11,16 Mean patient age in the present series was 33.2 years, which is consistent with prior reports⁵, of women presenting with infertility and those presenting with pain and related complaints. In a 2003 study, Arruda et al. found a mean age at diagnosis of 30 years for women presenting with infertility and 33 years for those presenting with pain.

In the present study, most affected women were white. A review of the literature shows endometriosis prevalence rates of up to 97% in Caucasian women; some studies have also reported predominance in Japanese women.^1,9,10. A major difference in prevalence was also found between black and Asian women, with the latter accounting for only 4.6% of the study sample. Most studies have found ethnic differences in prevalence, but not statistically significant ones⁸, which suggests that race differences do not play a role as risk factors for endometriosis.

In 2002, Kuohung et al. found a similar patient age range in endometriosis patients from the United States and United Kingdom, but reported a significant predominance of white (88%) versus non-white patients (13%).²⁶.

Women with endometriosis tend to have higher educational attainment and socioeconomic level^8,9. Accordingly, 51.9% of women in the study sample had a college- or university-level education. This may simply be due to bias, as women of higher socioeconomic standing have greater access to medical care and are more concerned with personal health in the event of pelvic pain or infertility.^8,16,27,28.

Regarding obstetric history, nulliparity has consistently been reported as having a strong association with endometriosis²⁶. In fact, it is impossible to determine whether nulliparity is a risk factor for the condition or if women with endometriosis find it harder to conceive¹. Miscarriage does not appear to correlate with endometriosis or risk of endometriosis^8,16, in the present sample, prevalence rates of nulligravid and nulliparous women and those who had never experienced pregnancy loss were highest.

Endometriosis is associated with twentyfold odds of infertility², interestingly, analysis of extracted data shows that approximately 40% of patients have primary or secondary infertility. These scenarios are known to lead to lower estrogen exposure, creating more favorable conditions for the development of endometriosis. Furthermore, it has been associated with other estrogen-dependent diseases, such as uterine leiomyomata or endometrial cancer⁹.

Evidence is mounting for a genetic, hereditary basis for endometriosis. In the present sample, 5.3% of patients had affected relatives. Studies have shown endometriosis rates of 4.8% to 8.8% in sisters of affected patients²⁹. Evidence is mounting for a genetic, hereditary basis for endometriosis. In the present sample, 5.3% of patients had affected relatives. Studies have shown endometriosis rates of 4.8% to 8.8% in sisters of affected patients^10,30-34, and twin studies have shown concordance rates twice as high in monozygotic twins than in dizygotic pairs³⁵.

The main symptom reported was dysmenorrhea (62.2%). It bears stressing that patients' complaints were only considered when they were reported as being severe or incapacitating. Endometriosis may be classified as superficial, when lesions are less than 5 mm in depth, or deep, when lesions are more than 5 mm in depth. Lesion depth is also known to correlate with symptom severity, and helps guide management.³⁶. As the setting of the present case series was a referral center, in which most surgical patients have advanced-stage disease and many have deep infiltrating endometriosis, the high prevalence of markedly severe symptoms may have been due to selection bias.

In addition to dysmenorrhea, endometriosis is closely associated with deep dyspareunia, chronic pelvic pain, and infertility. With a prevalence of 54.7%, deep dyspareunia was quite frequently associated with endometriosis in our sample, and can be a useful indicator of deep infiltrating disease, with likely involvement of the retrocervical region or rectovaginal fascia

³⁷. Affecting approximately 57% of patients, chronic pelvic pain is also a very common symptom, and is refractory to clinical management.

Intestinal endometriosis may be found in 6% to 30% of women with deep infiltrating endometriosis. In a minority of cases, it is asymptomatic, but the vast majority of patients thus affected report abdominal pain, constipation, a feeling of pressure on defecation, pain, bleeding, or even bowel stenosis and obstruction^38,39. In our sample, 48.3% of patients reported cyclical intestinal complaints, including bleeding and/or pain on defecation during the menstrual period. Only 3.7% of patients had intestinal symptoms as their chief complaint, however. Most had other associated symptoms, which they felt to be of greater relevance, as mentioned above. Another possible explanation for the low rate of patients with intestinal symptoms may be difficulty in distinguishing blood in feces from menstrual bleeding.

Urinary tract endometriosis is a rare entity, affecting approximately 1% of all patients with endometriosis; symptoms are wide-ranging and nonspecific. Bladder involvement is usually associated with symptoms of urinary irritation, such as dysuria, hematuria, and recurrent urinary tract infection. Ureteral involvement, however, has a remarkably nonspecific clinical picture, and patients may progress silently to renal failure. Only 11.7% of patients in our sample reported urinary symptoms; only 0.1% had them as a chief or presenting complaint. Bladder and ureteral endometriosis are now believed to be distinct clinical entities, with the latter being a manifestation of lateral extension of retrocervical disease^40,41.

CONCLUSION

Systematic assessment of a large sample of patients followed at a single specialized service showed that endometriosis is most often diagnosed in the fourth decade of life. Patients present with pelvic pain and infertility-related complaints, and must always be questioned thoroughly to guide the diagnostic process..

Conflicts of interest: No conflicts of interest declared concerning the publication of this article

REFERENCES

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2. Vinatier D, Orazi G, Cosson M, Dofour P. Theories of endometriosis. Eur J Obstet Gynecol Reprod Biol. 2001;96: 21-34.
3. Vercellini P, Fedele L, Aimi G, Pietropaolo G, Consonni D, Crosignani PG. Association between endometriosis stage, lesion type, patient characteristics and severity of pelvic pain symptoms: a multivariate analysis of over 1000 patients. Hum Reprod. 2007;22:266-71.
4. Gao X, Yeh YC, Outley J, Simon J, Botteman M, Spalding J. Health-related quality of life burden of women with endometriosis: a literature review. Curr Med Res Opin. 2006;22:1787-97.
5. Arruda MS, Petta CA, Abrão MS, Benetti-Pinto CL. Time elapsed from the onset of symptoms to diagnosis of endometriosis in a cohort study of Brazilian women. Hum Reprod. 2003;18:756-59.
6. Abrao MS, Podgaec S, Dias JA Jr, Averbach M, Garry R, Ferraz Silva LF, Carvalho FM. Deeply infiltrating endometriosis affecting the rectum and lymph nodes. Fertil Steril. 2006;86:543-7.
7. Podgaec S, Gonçalves MO, Klajner S, Abrão MS. Epigastric pain relating to menses can be a symptom of bowel endometriosis. São Paulo Med J. 2008;126:242-4.
8. Stefansson H, Geirsson RT, Steinthorsdottir V, Jonsson H, Manolescu A, Kong A, et al. Genetic factors contribute to the risk of developing endometriosis. Hum Reprod. 2002;17:555-9.
9. Hemmings R, Rivard M, Olive DL, Poliquin-Fleury J, Gagné D, Hugo P, et al. Evaluation of risk factors associated with endometriosis. Fertil Steril. 2004;81:1513-21.
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12. Petta CA, Matos AM, Bahamondes L, Faúndes D. Current practice in the management of symptoms of endometriosis: a survey of Brazilian gynecologists. Rev Assoc Med Bras. 2007;53:525-9
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16. Parazzini F, Chiaffarino F, Surace M, Chatenoud L, Cipriani S, Chiantera V, et al. Selected food intake and risk of endometriosis. Hum Reprod. 2004;19:1755-9.
17. Lebovic DI, Mueller MD, Taylor, RN. Immunobiology of endometriosis. Fertil Steril. 2001;75:1.
18. Abrão MS, Podgaec S. Endometriose: aspectos atuais do diagnóstico e tratamento. Rev Assoc Med Bras. 2004;61:41-6.
19. Podgaec S, Abrão MS. Endometriose. In: Fonseca AM, Bagnoli VR, Pinotti JA, editores. Ginecologia endócrina. São Paulo: Atheneu; 2004. p.195-202.
20. Meyer R. Uber den staude der frage der adenomyosites adenomyoma in allgemeinen und adenomyonetitis sarcomatosa. Zentralbl Gynakol. 1919;36:745-59.
21. Sampson JA. Perforating hemorrhagic cysts of the ovary, their importance and especially their relation to pelvic adenomas of endometrial type. Arch Surg. 1921; 3:245-7.
22. Podgaec S, Abrão MS, Dias Jr JA, Rizzo LV, Oliveira RM, Baracat EC. Endometriosis: an inflammatory disease with a Th2 immune response component. Hum Reprod. 2007;22:1373-9.
23. Podgaec S, Abrão MS, Aldrighi JM. Aspectos hormonais da endometriose. In: Aldrighi JM, editor. Endocrinologia ginecológica - aspectos contemporâneos. São Paulo: Atheneu; 2005. p.221-8.
24. Podgaec S, Dias Junior JA, Chapron C, Oliveira RM, Baracat EC, Abrão MS. Th1 and Th2 immune responses related to pelvic endometriosis. Rev Assoc Med Bras. 2010;56:92-8.
25. Missmer SA, Cramer DW. The epidemiology of endometriosis. Obstet Gynecol Clin North Am. 2003;30:1-19.
26. Kuohung W, Jones GL, Vitonis AF. Characteristics of patients with endometriosis in the United States and the United Kingdom. Fertil Steril. 2002;78:767-72.
27. Makhlouf OC, Armenian HK, Azoury R. Endometriosis in Lebanon. A case-control study. Am J Epidemiol. 1986;124: 762-7.
28. Van Langendonckt, A, Casanas-Roux, F, Donnez, J. Oxidative stress and peritoneal endometriosis. Fertil Steril. 2002;77:861.
29. Schenken, R. Treatment of endometriosis. Up To Date. 2008 Oct [cited 2008 Nov 24].). Available from: http://www.uptodate.com/home/store/index.do
30. Miyazawa K. Incidence of endometriosis among Japanese women. Obstet Gynecol. 1976;48:407-9.
31. Simpson JL, Elias S, Malinak LR, Buttram VC. Heritable aspects of endometriosis. I. Genetic studies. Am J Obstet Gynecol. 1980;137:327-31.
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34. Treolar SA, O´Connor DT, O´Connor VM, Martin NG. Genetic influences on endometriosis in na Australian twin sample. Fertil Steril. 1999;71:701-10.
35. Sangi-Haghpeykar H, Poindexter AN. Epidemiology of endometriosis among parous women. Obstet Gynecol. 1995;85:983-92.
36. Cornillie FJ, Oosterlynck D, Lauweryns JM, Koninckx PR. Deeply infiltrating pelvic endometriosis: histology and clinical significance. Fertil Steril. 1990;53:978-83.
37. Remorgida V, Ferrero S, Fulcheri E, Ragni N, Martin DC. Bowel endometriosis: presentation, diagnosis, and treatment. Obstet Gynecol Surv. 2007;62:461-70.
38. Seracchioli R, Poggioli G, Pierangeli L, Surgical outcome and long-term follow up after laparoscopic rectosigmoid resection in women with deep infiltrating endometriosis. Br J Obstet Gynecol. 2007;114:889-95.
39. Abrão MS, Bassi MA, Podgaec S, Dias Júnior JA, Sobrado CW, D' Amico Filho N. Bowel endometriosis: a benign disease? Rev Assoc Med Bras. 2009;55:611-6.
40. Pérez-Utrilla Pérez M, Aguilera Bazán A, Alonso Dorrego JM, Hernández A, Francisco MG, Martín Hernández M, et al. Urinary tract endometriosis: clinical, diagnostic, and therapeutic aspects. Urology. 2009;73:47-51.
41. Abrao MS, Dias JA Jr, Bellelis P, Podgaec S, Bautzer CR, Gromatsky C. Endometriosis of the ureter and bladder are not associated diseases. Fertil Steril. 2009;91:1662-7.

*

Correspondência: R Dr. Homem de Mello, 1020 - Perdizes, São Paulo - SP - CEP: 05007-002 - Tel: 3673-3885/3868-1957

pbellelis@yahoo.com.br

Publication Dates

Publication in this collection
12 Nov 2010
Date of issue
2010

History

Received
29 Mar 2010
Accepted
09 May 2010

This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

[1] 1. Viganò, P., Parazzini, F., Somigliana, E., Vercellini, P. Endometriosis: epidemiology and aetiological factors. Best Pract Res Clin Obstet Gynecol. 2004;18:177-200.

[2] 2. Vinatier D, Orazi G, Cosson M, Dofour P. Theories of endometriosis. Eur J Obstet Gynecol Reprod Biol. 2001;96: 21-34.

[3] 3. Vercellini P, Fedele L, Aimi G, Pietropaolo G, Consonni D, Crosignani PG. Association between endometriosis stage, lesion type, patient characteristics and severity of pelvic pain symptoms: a multivariate analysis of over 1000 patients. Hum Reprod. 2007;22:266-71.

[4] 4. Gao X, Yeh YC, Outley J, Simon J, Botteman M, Spalding J. Health-related quality of life burden of women with endometriosis: a literature review. Curr Med Res Opin. 2006;22:1787-97.

[5] 5. Arruda MS, Petta CA, Abrão MS, Benetti-Pinto CL. Time elapsed from the onset of symptoms to diagnosis of endometriosis in a cohort study of Brazilian women. Hum Reprod. 2003;18:756-59.

[6] 6. Abrao MS, Podgaec S, Dias JA Jr, Averbach M, Garry R, Ferraz Silva LF, Carvalho FM. Deeply infiltrating endometriosis affecting the rectum and lymph nodes. Fertil Steril. 2006;86:543-7.

[7] 7. Podgaec S, Gonçalves MO, Klajner S, Abrão MS. Epigastric pain relating to menses can be a symptom of bowel endometriosis. São Paulo Med J. 2008;126:242-4.

[8] 8. Stefansson H, Geirsson RT, Steinthorsdottir V, Jonsson H, Manolescu A, Kong A, et al. Genetic factors contribute to the risk of developing endometriosis. Hum Reprod. 2002;17:555-9.

[9] 9. Hemmings R, Rivard M, Olive DL, Poliquin-Fleury J, Gagné D, Hugo P, et al. Evaluation of risk factors associated with endometriosis. Fertil Steril. 2004;81:1513-21.

[10] 10. Kashima K, Ishimaru T, Okamura H, Suginami H, Ikuma K, Muramaki T, et al. Familial risk among Japanese patients with endometriosis. Int J Gynecol Obstet. 2004;84:61-4.

[11] 11. Heilier JF, Donnez J, Nackers F, Rousseau R, Verougstraete V, Rosenkranz K, et al. Environmental and host-associated risk factors in endometriosis and deep endometriotic nodules: a matched case-control study. Environ Res. 2007;103:121-9.

[12] 12. Petta CA, Matos AM, Bahamondes L, Faúndes D. Current practice in the management of symptoms of endometriosis: a survey of Brazilian gynecologists. Rev Assoc Med Bras. 2007;53:525-9

[13] 13. Cramer DW, Wilson E, Stillman RJ, Berger MJ, Belisle S, Schiff I, et al. The relation of endometriosis to menstrual characteristics, smoking, and exercise. JAMA. 1986;255:1904-8.

[14] 14. Porpora MG, Koninckx PR, Piazze J. Correlation between endometriosis and pelvic pain. J Am Assoc Gynecol Laparosc. 1999;6:429.

[15] 15. Modesitt SC, Tortolero-Luna G, Robinson JB, et al. Ovarian and extraovarian endometriosis-associated cancer. Obstet Gynecol. 2002;100:788.

[16] 16. Parazzini F, Chiaffarino F, Surace M, Chatenoud L, Cipriani S, Chiantera V, et al. Selected food intake and risk of endometriosis. Hum Reprod. 2004;19:1755-9.

[17] 17. Lebovic DI, Mueller MD, Taylor, RN. Immunobiology of endometriosis. Fertil Steril. 2001;75:1.

[18] 18. Abrão MS, Podgaec S. Endometriose: aspectos atuais do diagnóstico e tratamento. Rev Assoc Med Bras. 2004;61:41-6.

[19] 19. Podgaec S, Abrão MS. Endometriose. In: Fonseca AM, Bagnoli VR, Pinotti JA, editores. Ginecologia endócrina. São Paulo: Atheneu; 2004. p.195-202.

[20] 20. Meyer R. Uber den staude der frage der adenomyosites adenomyoma in allgemeinen und adenomyonetitis sarcomatosa. Zentralbl Gynakol. 1919;36:745-59.

[21] 21. Sampson JA. Perforating hemorrhagic cysts of the ovary, their importance and especially their relation to pelvic adenomas of endometrial type. Arch Surg. 1921; 3:245-7.

[22] 22. Podgaec S, Abrão MS, Dias Jr JA, Rizzo LV, Oliveira RM, Baracat EC. Endometriosis: an inflammatory disease with a Th2 immune response component. Hum Reprod. 2007;22:1373-9.

[23] 23. Podgaec S, Abrão MS, Aldrighi JM. Aspectos hormonais da endometriose. In: Aldrighi JM, editor. Endocrinologia ginecológica - aspectos contemporâneos. São Paulo: Atheneu; 2005. p.221-8.

[24] 24. Podgaec S, Dias Junior JA, Chapron C, Oliveira RM, Baracat EC, Abrão MS. Th1 and Th2 immune responses related to pelvic endometriosis. Rev Assoc Med Bras. 2010;56:92-8.

[25] 25. Missmer SA, Cramer DW. The epidemiology of endometriosis. Obstet Gynecol Clin North Am. 2003;30:1-19.

[26] 26. Kuohung W, Jones GL, Vitonis AF. Characteristics of patients with endometriosis in the United States and the United Kingdom. Fertil Steril. 2002;78:767-72.

[27] 27. Makhlouf OC, Armenian HK, Azoury R. Endometriosis in Lebanon. A case-control study. Am J Epidemiol. 1986;124: 762-7.

[28] 28. Van Langendonckt, A, Casanas-Roux, F, Donnez, J. Oxidative stress and peritoneal endometriosis. Fertil Steril. 2002;77:861.

[29] 29. Schenken, R. Treatment of endometriosis. Up To Date. 2008 Oct [cited 2008 Nov 24].). Available from: http://www.uptodate.com/home/store/index.do

[30] 30. Miyazawa K. Incidence of endometriosis among Japanese women. Obstet Gynecol. 1976;48:407-9.

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Epidemiological and clinical aspects of pelvic endometriosis: series of cases

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