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Peutz–Jeghers syndrome: a systematic review and recommendations for management
  1. A D Beggs1,
  2. A R Latchford2,
  3. H F A Vasen3,
  4. G Moslein4,
  5. A Alonso5,
  6. S Aretz6,
  7. L Bertario7,
  8. I Blanco8,
  9. S Bülow9,
  10. J Burn10,
  11. G Capella11,
  12. C Colas12,
  13. W Friedl6,
  14. P Møller13,
  15. F J Hes14,
  16. H Järvinen15,
  17. J-P Mecklin16,
  18. F M Nagengast17,
  19. Y Parc18,
  20. R K S Phillips19,
  21. W Hyer19,
  22. M Ponz de Leon20,
  23. L Renkonen-Sinisalo15,
  24. J R Sampson21,
  25. A Stormorken22,
  26. S Tejpar23,
  27. H J W Thomas24,
  28. J T Wijnen14,
  29. S K Clark19,
  30. S V Hodgson1
  1. 1Department of Clinical Genetics, St George's Hospital, London, UK
  2. 2Department of Gastroenterology, Derriford Hospital, University of Plymouth, Devon, UK
  3. 3Department of Gastroenterology and Hepatology, Leiden University Medical Centre, Leiden, The Netherlands
  4. 4Department of Surgery, St Josefs Hospital Bochum-Linden (Helios), Bochum, Germany
  5. 5Department of Medical Genetics, Hospital Virgen del Camino, Pamplona, Spain
  6. 6Institute of Human Genetics, University of Bonn, Germany
  7. 7Department of Surgery, Hospital Tumori, Milan, Italy
  8. 8Genetic Counselling Unit, Prevention and Cancer Control Department, Catalan Institute of Oncology, Barcelona, Spain
  9. 9Danish Polyposis Registry, Department of Surgery, Hvidovre University Hospital, Hvidovre, Denmark
  10. 10Institute of Human Genetics, Newcastle-upon-Tyne, UK
  11. 11Institute Catala D'Oncologia, Barcelona, Spain
  12. 12Laboratoire d'Oncogenetique, Groupe Hospitalier Pitié-Salpêtre, Paris
  13. 13Section of Inherited Cancer, Department of Medical Genetics, Rikshospitalet-Radium Hospitalet Medical Centre, Oslo, Norway
  14. 14Departments of Human & Clinical Genetics, Leiden University Medical Centre, The Netherlands
  15. 15Department of Surgery, Helsinki University Central Hospital, Helsinki, Finland
  16. 16Department of Surgery, Jyvaskyla Central Hospital, Jyvaskyla, Finland
  17. 17Department of Gastroenterology and Hepatology, Radboud University Medical Centre, Nijmegen, The Netherlands
  18. 18Department of Digestive Surgery, Hospital Saint-Antoine, University Pierre et Marie, Paris, France
  19. 19The Polyposis Registry, St Mark's Hospital, Harrow, Middlesex, UK
  20. 20Department of Internal Medicine, University Hospital, Modena, Italy
  21. 21Institute of Medical Genetics, School of Medicine, Cardiff University, UK
  22. 22Department of Medical Genetics, Ullevål University Hospital, Oslo, Norway
  23. 23Digestive Oncology Unit, Department of Internal Medicine, University Hospital Gasthuisberg, Leuven, Belgium
  24. 24CRUK, Family Cancer Group, St Mark's Hospital, Harrow, Middlesex, UK
  1. Correspondence to Professor Shirley Hodgson, Department of Clinical Genetics, St Georges, University of London, Cranmer Terrace, London SW17 ORE, UK; shodgson{at}sgul.ac.uk

Abstract

Peutz–Jeghers syndrome (PJS, MIM175200) is an autosomal dominant condition defined by the development of characteristic polyps throughout the gastrointestinal tract and mucocutaneous pigmentation. The majority of patients that meet the clinical diagnostic criteria have a causative mutation in the STK11 gene, which is located at 19p13.3. The cancer risks in this condition are substantial, particularly for breast and gastrointestinal cancer, although ascertainment and publication bias may have led to overestimates in some publications. Current surveillance protocols are controversial and not evidence-based, due to the relative rarity of the condition. Initially, endoscopies are more likely to be done to detect polyps that may be a risk for future intussusception or obstruction rather than cancers, but surveillance for the various cancers for which these patients are susceptible is an important part of their later management.

This review assesses the current literature on the clinical features and management of the condition, genotype–phenotype studies, and suggested guidelines for surveillance and management of individuals with PJS. The proposed guidelines contained in this article have been produced as a consensus statement on behalf of a group of European experts who met in Mallorca in 2007 and who have produced guidelines on the clinical management of Lynch syndrome and familial adenomatous polyposis.

  • Peutz–Jegher syndrome
  • hamartoma
  • polyp
  • screening
  • colonic polyps
  • polyposis
  • screening

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Introduction

Peutz-Jeghers syndrome (PJS) is an inherited polyposis syndrome in which multiple characteristic polyps occur in the gastrointestinal tract, associated with mucocutaneous pigmentation, especially of the vermilion border of the lips. It is inherited in an autosomal dominant manner and is caused by a germline mutation in the STK11 (LKB1) gene. The proposed guidelines contained in this article have been produced as a consensus statement on behalf of a group of European experts who met in Mallorca in 2007 and who have produced guidelines on the clinical management of Lynch syndrome1 and familial adenomatous polyposis.2

PJS was initially documented by an English physician3 who described twin sisters with oral pigmentation, who were subsequently illustrated by the surgeon J Hutchinson.4 One of the twins died of an intussusception at age 20 years, and the other of breast cancer at 52 years.

The eponym Peutz–Jeghers syndrome was originally put forward in 1954 by Bruwer et al5 who based the name on the work of Peutz,6 who described a family with autosomal dominant inheritance of gastrointestinal polyposis and pigmented mucous membranes, and Jeghers7 8 who defined the coexistence of mucocutaneous pigmentation and gastrointestinal polyposis as a distinct clinical entity.

The incidence of this condition is estimated to be between 1 in 50 000 to 1 in 200 000 live births.9

Clinical features

Mucocutaneous pigmented lesions are seen in around 95% of patients and may be the first clue to an individual having PJS. Lesions tend to arise in infancy, occurring around the mouth, nostrils, perianal area, fingers and toes, and the dorsal and volar aspects of hands and feet. They may fade after puberty but tend to persist in the buccal mucosa. The histology of the pigmented macules is increased melanin in basal cells, possibly due to an inflammatory block to melanin migration from melanocyte to keratinocyte. Lip freckling is not unique to PJS and the differential diagnosis includes Carney complex, a syndrome characterised by spotty skin pigmentation and lentigines, most commonly on the face, especially on the lips, eyelids, conjunctiva and oral mucosa.10

The polyps seen in PJS have characteristic histological features, with a frond-like elongated epithelial component and cystic gland dilatation extending into the sub-mucosa or muscularis propria, and arborising smooth muscle extending into polyp fronds (in contrast to juvenile polyps, which have a lamina propria lacking smooth muscle11). These polyps are usually referred to as hamartomas, but controversy surrounds their origin. It has been suggested that the process underlying their development may be mechanical, or that they may be a result of stromal neoplasia.12 Small bowel polyps may display the phenomenon of ‘pseudoinvasion’, which may be mistaken for invasive carcinoma.13 The lack of cytological atypia among other features can distinguish between true and pseudo invasion.

Polyps are found throughout the gastrointestinal tract but most are in the small bowel (60–90%)14 and colon (50–64%). They may also be found at extra-intestinal sites such as the gallbladder, bronchi, bladder and ureter.15 Gastrointestinal polyps may cause gastrointestinal bleeding, anaemia and abdominal pain due to intussusception, obstruction or infarction. Polyp-related symptoms usually arise in childhood and are seen by the age of 10 years in 33% and by 20 years in 50%.

In a single individual, a clinical diagnosis of PJS may be made when any ONE of the following is present16 17:

  1. Two or more histologically confirmed PJ polyps

  2. Any number of PJ polyps detected in one individual who has a family history of PJS in close relative(s)

  3. Characteristic mucocutaneous pigmentation in an individual who has a family history of PJS in close relative(s)

  4. Any number of PJ polyps in an individual who also has characteristic mucocutaneous pigmentation.

A study by Aretz et al17 correlated the diagnostic criteria for PJS with STK11 mutation detection rates. Of the patients who met the criteria for PJS, over 94% had a mutation detected (64% point mutation, 30% deletions).

Molecular genetics of PJS

Initial linkage analysis localised the affected gene to chromosome 19p13.3.18 19 Further studies identified a gene encoding a serine–threonine kinase, STK11 (LKB1).20 21 Hemminki et al20 cloned the gene and demonstrated mutations in the STK11 gene in 11/12 (90%) PJS cases using direct sequencing of DNA and mRNA. Recent studies which have searched for germline mutations by both direct sequencing and also multiplex ligation dependent probe amplification (MLPA) demonstrate a detection rate of germline mutations between 80% and 94%.17 22 23

Loss of heterozygosity at 19p13.3 seen in PJS polyps and malignancy suggests that STK11 acts as a tumour suppressor gene. The gene is more than 23 kb in length, and extends over nine exons, encoding a 433 amino acid protein.

The function of STK11 is complex and still being clarified.24 This serine–threonine kinase is expressed ubiquitously in adult and fetal tissue. In brief, STK11 has been found to regulate cellular proliferation via G1 cell-cycle arrest, WAF1 (a cyclin-dependent kinase inhibitor) signalling25 26 and p53 mediated apoptosis.27 It has an important role in cell polarity28 and regulates the Wnt signalling pathway.29 It is also involved in cell metabolism and energy homeostasis.30 It is an upstream regulator of AMP activated protein kinase (AMPK), thereby regulating the TSC pathway and acting as a negative regulator of the mammalian target of rapamycin (mTOR) pathway.31 The mTOR pathway is particularly important as it is a final common pathway that is also dysregulated by other hamartomatous polyposis syndromes caused by germline PTEN, BMPR1A and SMAD4 mutations.

Over-expression of COX-2 has been noted in PJS polyps and cancers,32 and may present a therapeutic target for modulation of polyp development.

A single family has shown linkage to 19q13.419 and some evidence of linkage to 6p11-cen has also been demonstrated.33 In addition, linkage studies of PJS families looking for a second PJS locus34 35 suggested that in some the 19p13.3 locus was not involved in PJS. This has raised the possibility of genetic heterogeneity. A recent study36 examined the role of mutations in the MYH11 gene in 25 STK11 mutation negative patients with the PJS phenotype. One patient had a mutation (c.5798_5799insC) in the MYH11 gene, although this mutation was also found in apparently unaffected relative. Although genetic heterogeneity has been questioned, no clear second causative gene has been found for PJS cases without detectable STK11 mutation. It is likely that with continued improvements in genetic testing that mutation detection rates will improve further, making genetic heterogeneity even less likely.

Genotype–phenotype correlation

A genotype–phenotype correlation has been sought in PJS. Amos et al37 suggested individuals with missense mutations had a later onset of symptoms than individuals with other mutations in STK11. Schumacher et al38 suggested that in-frame mutations in domains encoding protein and ATP binding and catalysis (I–VIA) were rarely associated with cancer, missense mutations in the C terminus and in the part of the gene encoding protein domains for substrate recognition (VIB–VIII) were more associated with malignancies, and patients with breast carcinomas had predominantly truncating mutations. Mehenni et al39 studied 49 PJS families with defined mutations, and found 32 cancers. They suggested that there was a higher risk of cancer in cases with mutations in exon 6 of the STK11 gene. These studies, however, are small and it is difficult to draw firm conclusions from them. Most studies have been carried out on western European populations but a study of Latin-American PJS patients40 demonstrated mutations in exon 2 (c.350_351insT) and exon 6 (c.811_813delAG) of the STK11 gene.

In a larger series 240 PJS patients with STK11 mutations were analysed. No difference was seen between individuals with missense and truncating mutations, nor between familial and sporadic cases although it was suggested that there was a higher risk of cancer in individuals with mutations in exon 3 of the gene. Hearle et al41 continued this study, analysing a total of 419 PJS patients, 297 with documented mutations. They found that the type and site of mutation did not influence cancer risk.

In conclusion, no clear genotype–phenotype correlation has been demonstrated in PJS, and no clear differences found between cases with STK11 mutation and in those in whom no mutation has been detected.

Cancer risk

How cancer arises in PJS and the role of the PJS polyp in cancer development remain controversial. It has been proposed that a unique hamartoma–adenoma–carcinoma pathway42 exists. This hypothesis is supported by the finding of adenomatous foci within PJS polyps and also by the description of cancer arising within PJS polyps.43 Others have proposed that the PJS polyps have no malignant potential. Malignant transformation within a PJS polyp is only seen as a rare event supporting this hypothesis.44 In addition PJS polyps have been shown to be polyclonal (and therefore unlikely to have malignant potential) and it is suggested that the ‘PJS polyp’ may actually represent a form of abnormal mucosal prolapse,44 caused by changes in cellular polarity induced by mutation in the STK11 gene, rather than a true hamartoma. If PJS polyps have no malignant potential it would imply that cancer arises on a background of mucosal instability, presumably through conventional neoplastic pathways. Whether this pathway is accelerated is an intriguing question which has yet to be answered. Certainly the fact that only one of the 17 colorectal cancers seen in the largest series41 was detected at surveillance raises the possibility of an accelerated pathway (provided that patients were under surveillance and compliance was adequate). Further research in this area is required to clarify these issues.

Based on epidemiological and molecular genetic studies,45 it is now widely accepted that there is an increased risk of many cancers in PJS. Multiple single cohort studies have been carried out by individual groups14 38 46–52 which make up the bulk of the literature. It is difficult to come to any firm conclusions from these relatively small studies, which are likely to be subject to both ascertainment and publication bias, thereby potentially inflating the cancer risk in PJS. A meta-analysis has been performed by Giardiello et al, assessing 210 patients from six studies.53 A study by Lim et al54 was subsequently continued by Hearle et al41 to produce a cohort of 419 patients with PJS. These studies by Giardiello and Hearle offer the most comprehensive data for cancer risk and their main findings are summarised in tables 1 and 2.

Table 1

Cumulative cancer risk by site and age in Peutz–Jeghers syndrome patients (from Hearle et al41)

Table 2

Risk ratios, frequencies and ages of onset of Peutz–Jeghers syndrome cancers by site (from Giardiello et al53

Hearle et al41 examined the incidence of cancer in 419 individuals with Peutz–Jeghers syndrome, 297 of which had documented STK11 mutations. Ninety-six (23%) developed cancer, the risks of which stratified by age are shown in table 1. Giardiello et al53 reviewed 210 PJS cases from six publications: the relative risks of cancer of different sites are shown in table 2. From these studies it can be seen that luminal gastrointestinal cancers and breast cancer are the most common cancers, followed by pancreatic cancer. It is striking in the Hearle study how risk increases rapidly after the age of 50 for all cancers, a fact not taken into consideration in most current surveillance protocols.

Mehenni et al55 recently examined the survival of 149 patients (76 male, 73 female) all of whom had a documented STK11 mutation (table 3). This study differs from those above in that only one case of breast cancer was observed. The reason for this discrepancy is not clear. Otherwise the predominance of luminal gastrointestinal cancer (especially colorectal) and the rapid increase in cancer risk after the age of 50 years are confirmed.

Table 3

Frequency of cancer in Peutz–Jeghers syndrome (Mehenni et al55)

The observation of a rare sex cord tumour in PJS is important. Young et al56 carried out a review of 74 sex cord ovarian tumours with annular tubules (SCTAT), of stromal origin. Of these, 27 were in individuals with PJS, and all were multifocal, bilateral, very small, benign and calcified. They could develop in young children, the youngest diagnosed at 4 years of age. Twelve affected individuals had hyper-oestrogen syndrome; four had adenoma malignum of the cervix of which two were fatal, diagnosed at 23 years and 36 years of age.

Song et al57 described the case of a 41-year-old woman with PJS who had multiple genital tract tumours and breast cancer; their literature review found that 36% patients with SCTAT have PJS, and SCTAT is usually benign and multifocal. Bilateral malignant ovarian sex cord tumour was described in a 47-year-old woman with PJS presenting with an abnormal cervical smear58 and it was suggested that the hyper-oestrogenism caused by sex cord tumours could induce cervical adenoma malignum. This has a poor prognosis in general; of 10 cases reviewed by Srivatsa et al,59 eight died, only one survived longer than 5 years. One case of gonadoblastoma was described in a 34-year-old PJS patient.60 Large-cell calcifying Sertoli cell tumours of the testis can also develop, usually in pre-pubescent boys, leading to gynaecomastia because of hormonal imbalance caused by the neoplasm.61

Dozois et al62 reviewed 115 reported cases of PJS in females from the literature. Of these 16/115 had ovarian tumours diagnosed at ages 4.5 to 60 years. There were five granulosa cell tumours, five cystadenomas, four non-neoplastic cysts, one Brenner tumour, one dysgerminoma, and two with undetermined diagnoses.

Von Herbay63 reported a case of bronchoalveolar cancer of mucinous type in a 22-year-old male with PJS, hypothesising that it may represent a PJS associated cancer.

Clinical management

Surveillance

Surveillance protocols in PJS have two main purposes. One is to detect sizeable gastroenterological polyps which could cause intussusception/obstruction or bleeding/anaemia. The other is the detection of cancer at an early stage. The indication for screening is therefore age dependent: polyp-related complications may arise in childhood, whereas the cancer risk largely pertains to the adult population.

Although most authorities agree that surveillance of some sort is warranted in patients with PJS, there is no consensus as to what organs should be monitored, with what frequency and when to start.

In order to carry out a comprehensive review of the literature a systematic review of the screening evidence was carried out.

Systematic review

Method

A systematic review of the available literature was carried out using the Ovid Medline 1950 to current; the Ovid EMBASE 1980 to current; Ovid OLDMEDLINE; Cochrane Database of Systematic Reviews and Pubmed.

Seperate search strategies were carried out with the MESH search term ‘Peutz–Jeghers Syndrome’ and ‘screening’. Searches were combined with the AND operator.

All papers identified had their bibliography searched manually to identify further papers of interest. A separate literature search was carried out for therapeutic modalities using the MESH search terms ‘Peutz–Jeghers Syndrome’ and ‘therapy’.

The strength of evidence was classified according to the north of England evidence-based guidelines development project64 (see table 4).

Table 4

Categories of evidence and grading of recommendations

Inclusion and exclusion criteria

All articles discussing Peutz–Jeghers syndrome mentioning screening or surveillance were retrieved. For the therapy search, all articles discussing PJS mentioning any therapeutic aspect were retrieved. Acceptable article types retrieved were retrospective cohort studies, case reports, randomised controlled trials and case–control studies up to May 2009. Only English language articles were retrieved and all articles were reviewed independently for suitability (see figure 1).

Figure 1

QUORUM diagram for screening evidence review.

Results

Screening

A total of 1254 papers were identified (Medline=73, Embase=152, Cochrane=0, OLDMedline=0, Pubmed=1029), of which 12 met the criteria. Manual examination of the bibliography of each paper found three additional papers that met the criteria, giving a total of 15. Figure 1 shows the QUORUM flowchart for this search. Table 5 summarises the key recommendations of each of the papers retrieved.

Table 5

Systematic review of surveillance evidence

Therapy

A total of 286 papers were identified (Medline=26, Embase=9, Cochrane=0, OLDMedline=0, Pubmed=251). All 286 met the criteria and were carried forward. Because of space constraints, these papers are not listed in this review.

Surveillance recommendations

Question: What is the role of surveillance endoscopic examination of the gastrointestinal tract?

One role for surveillance endoscopy is the detection of cancer. Giardiello et al53 found a range of age from 27 to 71 years for colorectal cancer diagnosis in PJS, with an overall risk of 39%, the majority of which were in males. Hearle et al41 found that colorectal cancer was the most common luminal gastrointestinal cancer (17/40). The risk of colorectal cancer was 3%, 5%, 15% and 39% at ages 40, 50, 60 and 70 years, respectively. Although there was a male preponderance, this was not statistically significant. In this large series only one case of sigmoid cancer was detected during surveillance.

Upper gastrointestinal (GI) cancers are less common. Gastric cancer is far more common than oesophageal53 and the average age of stomach cancer diagnosis was 30 years. Although very rare, upper GI cancer has been reported during the first and second decades of life.53

The other indication for surveillance is the detection of large polyps allowing early therapy and the prevention of polyp related symptoms. There are sparse data regarding this. In a study from a single institution reporting outcomes from gastrointestinal surveillance, of 28 patients who had undergone one or more surveillance endoscopies by the age of 18 years, 17 were found to have developed significant gastroduodenal or colonic polyps.79 Thirty-nine colonic polyps and 20 gastroduodenal polyps larger than 1 cm were detected in these patients; the largest lesions were a 6 cm colonic polyp and an 8 cm gastric polyp.

The same series79 demonstrated that colonoscopic and upper GI tract surveillance is safe. During 786 surveillance examinations and over 1500 polypectomies, there were only two cases of perforation (both following resection of polyps larger than 2 cm) and no post-polypectomy bleeding was observed.

Dunlop et al68 recommended screening intervals of every 3 years for upper and lower GI endoscopy, beginning at age 18. Hemminki et al65 recommended screening start at age 18, with upper and lower GI endoscopy being performed at 2–5 year intervals. Giardiello et al9 recommended a baseline upper GI endoscopy at the age of 8 years and every 2–3 years thereafter if polyps were detected. If no polyps are detected they recommend further surveillance upper GI endoscopy from the age of 18 years, with colonoscopic surveillance also starting at this age.

Some authors advocate not starting screening at all until age 18. We suggest starting at 8 years to pick up those with polyps at that stage to prevent problems in late childhood/early adolescence, which is when most obstructions occur. Data is lacking on the rate of polyp progression, but those with no polyps aged 8 years will still have follow-up, and be investigated if symptomatic/anaemic. There is a paucity of evidence to support recommendations here; however, we feel that this strikes a balance between preventing polyp complications and over-investigating children.

Conclusion: A baseline colonoscopy and upper GI endoscopy (OGD) is indicated at age 8years. In those in whom significant polyps are detected these should be repeated every 3years. In those in whom there are no significant polyps at baseline endoscopy, routine surveillance is repeated at age 18, or sooner should symptoms arise, and then three yearly. We recommend that after the age of 50years the frequency is increased to every 1–2years due to the rapid increase in cancer risk at this age. There is, however, no evidence of benefit (Level of evidence: III, Grade of recommendation: C)

Question How and when should small bowel surveillance be performed in PJS?

Small bowel surveillance for polyps allows polypectomy before symptoms develop or obstruction occurs. A variety of investigations can be used.

Several studies80 81 have compared barium follow-through and capsule endoscopy. Two studies in adult patients found that video capsule endoscopy (VCE) has a greater sensitivity in detecting small bowel polyps. The study size was small in both studies. A prospective study has been performed comparing barium follow-through (BaFT) and VCE in paediatric patients with PJS.82 No significant difference was found in detection rates of polyps >1 cm but VCE detected more polyps<1 cm and also was much better tolerated. Many centres now use VCE, since it appears at least as accurate as barium follow through, is preferred by patients and reduces radiation exposure.

There are some early data on the use of magnetic resonance enterography (MRE) assessment of the small bowel in patients with PJS. Kurugoglu et al83 compared barium follow-through with ultrasound and MRE. They found that polyps were detected equally with contrast studies and MRE. Caspari et al84 compared VCE with MRE and observed that VCE was superior at detecting small polyps. Polyps of 15 mm and above were detected equally with both modalities and location of polyps and determination of their exact sizes was more accurate with MRE. Further studies to assess the utility of MRE are required.

There are no data to support the use of double-balloon enteroscopy as a method of small bowel surveillance in PJS. It is a prolonged, very invasive procedure and does not guarantee visualisation of the entire small bowel, especially in those who have undergone previous abdominal surgery. Although there are some reports of its use in PJS these are in the setting of therapy in patients with intussusception or prophylactically in patients who have had polyps detected by other means.79

The main indication for surveillance of the small bowel is the prevention of intussusception and the need for emergency laparotomy. There are limited data to guide when to start surveillance of the small bowel. A survey of adults with PJS70 found that by the age of 18 years, 23/34 (68%) of adults had undergone laparotomy, 70% of which were performed as an emergency. By the age of 10 years, 30% had required a laparotomy. In order to reduce the likelihood of developing intestinal obstruction, the study recommended that asymptomatic children start small bowel screening at the age of 8 years. A recent review of gastrointestinal surveillance from a single institution found that no patients enrolled on the programme required emergency surgery for obstruction or intussusception during 683 patient years follow-up.79

Conclusion: Small bowel screening using video capsule endoscopy (VCE) should be performed every 3years if polyps are found at the initial examination, from age 8years, or earlier if the patient is symptomatic. If few or no polyps are found at the initial examination, screening should commence again at the age of 18. Magnetic resonance enterography (MRE) and barium follow-through (BaFT) are reasonable alternatives in adult patients but BaFT is not favoured in children due to radiation exposure. (Level of evidence: III, Grade of recommendation: B)

Question: What is the best method of breast cancer surveillance in PJS?

The earliest documented case of breast cancer in PJS is 19 years, and clearly the breast cancer risk (cumulative risk 31–54% at age 60 years,41 53 usually ductal, sometimes lobular with a mean age at diagnosis of 37 years (19–48), is significant.

Breast cancer screening can be carried out via a variety of methods including digital x-ray mammography, MR mammography, ultrasound and self-examination. Radiological techniques confer greater sensitivity than self-examination but the radiation burden of repeated x-ray mammography is significant. In addition, the sensitivity of mammography in younger patients with dense breast tissue is reduced. In diagnostic use, ultrasound and MR mammography both increase diagnostic accuracy in a younger patient group with dense breast tissue compared to x-ray mammography.85 However, MRI mammography is significantly superior to ultrasound in screening. A model developed to assess cost effectiveness of breast cancer screening with contrast-enhanced MRI in patients with germline BRCA1 and 2 mutations demonstrated that screening with MRI, alone or in combination with x-ray mammography, is cost effective by current standards compared with x-ray mammography alone.86

Although no breast screening techniques have been evaluated specifically in patients with PJS, due to the fact that the risk is approaching that of patients with BRCA mutations, it would seem logical that the breast surveillance programme recommended for BRCA mutation and other high risk patients be utilised in PJS 87; namely annual MRI from age 25 years. These guidelines recommend mammography in addition, because of the high incidence of ductal carcinoma in situ (DCIS) associated with BRCA mutations. There is currently no evidence of increased incidence of DCIS in PJS.

MR mammography may not currently be widely available. It is also more expensive than mammography and may not be tolerated by some individuals. In this setting it may be reasonable to offer supplemental ultrasound, especially in those with dense breast tissue, although it is not recommended as a screening modality.

Conclusion: Annual MRI/US should start at age 25–30years, with x-ray mammography being substituted after the age of 50. (Level of evidence: IV, Grade of recommendation: C)

Question: Is pancreatic cancer surveillance useful in PJS?

The degree to which pancreatic cancer risk is elevated is unclear. Hearle et al41 observed a cumulative risk of 7% at age 60, which is at markedly less than 36% by 64 years observed by Giardiello et al.53

Screening for pancreatic cancer is particularly difficult and to date there are no firm data that demonstrate clear benefit even in the setting of a higher risk of development of pancreatic cancer (eg, hereditary pancreatitis). The sequence of the development of pancreatic cancer is thought to be similar to that of the adenoma–carcinoma sequence in colorectal cancer. Initially, a pancreatic intraepithelial neoplasia (PanIN) lesion (elongated mucin-producing cells with little neoplasia) develops, leading through to PanIN-lll lesions (carcinoma in situ). Although this model of progression is widely accepted it has not been fully validated and the natural history of PanIN, in terms of time to progression to cancer, has not been established. In addition early lesions are not radiologically detectable until the development of associated secondary changes such as fibrosis and retention cysts.72

Suggested screening regimes have included endoluminal ultrasonography (sensitive), CT (not sensitive for detecting small lesions especially PanIN) and endoscopic cholangiopancreatography (ERCP), with molecular analysis of pancreatic secretions,88 specifically for k-RAS mutations (not specific for cancer); p16/INK4A and p53 mutations (more specific) and methylation analysis of the p16/INK4A promoter (60% sensitivity, 90% specificity). However, in order to harvest these pancreatic secretions, ERCP must be used. The complications of ERCP are pancreatitis (6.7% incidence), which is severe in 0.3%, and a mortality rate of 0.03% post-procedure. Magnetic resonance cholangiopancreatography (MCRP) is a possible alternative to the other modalities, but there is no evidence for its routine use. It has been estimated that implementing a surveillance programme in PJS would cost in excess of US$ 350 000 per life saved, assuming that all cases of pancreatic cancer diagnosed during the programme survived.72

Conclusion: Routine surveillance for pancreatic cancer in PJS using current methods is not proven to be of benefit and is not cost effective. It should only be performed in the setting of a clinical research study. (Evidence level: III, Grade of recommendation: B)

Question: Should surveillance for genital tract malignancies be performed in PJS?

The increase in ovarian tumour risk is mainly not for epithelial ovarian cancer but for SCTAT, which can occur in very young children (2 and 4 years of age reported in the study by Lim et al54) although the main risk appears to be in the fourth and fifth decades of life. Giardiello et al53 reported a 21% lifetime risk of ovarian tumours, a risk of cervical cancer of 9% by 64 years (mean age at diagnosis 34 years) and 10% of uterine cancer. The risks observed by Hearle and colleagues are lower.41 They observed nine gynaecological cancers (two uterine, two ovarian and five cervical), with a risk of 1% at age 30 years, rising to 18% at age 60 years.

Ovarian cancer screening is based on CA-125 levels and trans-vaginal ultrasound scanning, and has been suggested at 6–12 monthly intervals in patients with PJS.77 However, as epithelial ovarian cancer is not a specific risk, and there are no data on this type of surveillance in PJS, this recommendation is not supported by evidence. Furthermore, initial findings from the UKCTOCS have recently been reported, assessing multimodal screening (ultrasound and Ca-125) for ovarian cancer in a postmenopausal cohort.89 The positive predictive value (PPV) was poor: 43% for multimodal screening and only 5% for ultrasound. In addition an effect on survival using multimodal screening has not yet been demonstrated. The poor PPV observed reflects the high prevalence of benign adnexal abnormalities. In PJS, the ovarian tumours are SCTAT, and there is no clear evidence about the effectiveness of any screening modality for this type of tumour. In a younger cohort of PJS patients, it would be a concern that there would be a higher prevalence of benign pathology detected by screening and unnecessary surgical intervention might be performed as a result.

Surveillance for endometrial cancer could be similar to that of Lynch syndrome patients, with a 12-month interval being recommended, from 35 years of age. Endometrial pipelle biopsy sampling and trans-vaginal ultrasound are the recommended screening modalities.90 However, the value of surveillance for endometrial cancer in Lynch syndrome is unknown.1 Given that most cases of sporadic endometrial cancer are detected at an early stage and the risk of endometrial cancer in PJS is much lower than in Lynch syndrome, it would be reasonable to argue that endometrial surveillance is unnecessary and certainly has no evidence to support its use.

Population cervical screening is widely practised and has been shown to be effective in the reduction of cervical cancer and associated mortality91 92 There are no studies that have specifically addressed any means of surveillance for cervical cancer in patients with PJS. It has been recommended on expert opinion that patients with PJS undergo cervical smears as per population screening programme but with a high index of suspicion for adenoma malignum. This would mean a smear every 2–3 years using the new technique of liquid-based cytology (LBC)91 from age 21 to 25 years.

Testicular cancer surveillance is recommended on the basis of expert opinion only. In a literature review all cancers detected were Sertoli cell tumours and occurred at an average age of 9 years.53 Annual testicular examination47 93 is recommended with ultrasound scanning reserved for patients where an abnormality is found or precocious puberty develops.

Conclusion: There is no evidence to support routine screening for genital tract malignancies in PJS. However, expert opinion advocates regular screening consisting of 2–3 yearly cervical smears using liquid-based cytology (LBC) from age 25years, testicular examination and testicular ultrasound in patients where an abnormality is detected at examination. Routine surveillance for endometrial and ovarian cancers is not recommended. (Evidence level: IV, Grade of recommendation: C)

Question: Are there any other malignant tumours that should be part of a PJS surveillance programme?

Thyroid cancer may be slightly increased in PJS, and has been reported at a young age (30 years)48 but screening for thyroid cancer is not validated although clinical thyroid examination could be included in regular clinical examinations of PJS patients. Lung cancer is also increased, with a young age at diagnosis (mean age at diagnosis 49 years),48 but screening for this has not been advocated.

Conclusion: There is no evidence for screening of other malignancies in PJS (Evidence level: IV, Grade of recommendation: C)

Therapy

Few options exist for the therapeutic management of PJS. Surgical strategies are common with dealing with the sequelae of PJS such as small bowel intussusception due to hamartomatous polyps or resection of neoplastic lesions.

Question: Is endoscopic polypectomy of benefit?

Endoscopic polypectomy is recommended at upper GI endoscopy and colonoscopy to reduce cancer risk9 93 94 based on data obtained from patients with a sporadic adenomatous polyp. As the malignant potential of polyps in PJS is unknown, it is not clear if endoscopic polypectomy alters cancers risk. Latchford et al79 found only six cases of atypia or dysplasia in over 1000 PJS polyps; there were no polyps with adenomatous foci or malignant change.79 The rarity of dysplasia and neoplasia argues against a hamartoma–adenoma–carcinoma pathway and therefore it is likely that polypectomy does not influence cancer risk.

The recent development of the double balloon enteroscope95 and the capsule endoscopy device95 have allowed direct visualisation of the small bowel, and in the case of the double balloon enteroscope, resection of polyps via a standard snare polypectomy.

Intra-operative enteroscopy (IOE) has been also recommended67 96 in any patient with PJS undergoing laparotomy, as careful endoscopy via an enterotomy in the small bowel allows identification and removal of polyps found in the small bowel, thus avoiding multiple enterotomies and the risk of short bowel syndrome associated with resection. This technique allows greater sensitivity in polyp detection than palpation and transillumination (38% of polyps identified at IOE were not detected by these methods,97 and removal of all detected polyps (‘clean sweep’) reduced the re-laparotomy rate significantly.98

It is likely that the main benefit of polypectomy is to prevent polyp-related complications rather than reduce cancer risk. Prevention of anaemia and bleeding is difficult to quantify but certainly IOE has been shown to reduce the risk of further operative polypectomy in the future.99

Conclusion: Endoscopic polypectomy reduces polyp-related complications and risk of future operative polypectomy. If a laparotomy is performed on a patient with PJS, either as an emergency for obstruction/intussusception, or electively for the removal of large or symptomatic polyps which cannot be removed endoscopically, IOE and ‘clean sweep’ polypectomy should be undertaken (Evidence level: IIb, Grade of recommendation: B)

Question: Does pharmacological prophylaxis exist for PJS patients?

Lack of LKB1 kinase in PJS and many sporadic cancers drives cell growth and proliferation by inappropriate activation of mTOR protein kinase cascade. Recent animal-based studies have focused upon inhibitors of the mTOR pathway, specifically rapamycin.100 Lkb1± mice were treated with rapamycin 2 mg/kg/day and killed mice were examined for polyp burden. It was found that tumour burden decreased significantly in the treatment group, suggesting that rapamycin may have potential as a therapeutic agent in patients with STK11 mutations. There is a clinical trial (NCT00811590) under way in PJS patients of everolimus (RAD001), which inhibits one of the complexes of mTOR, mTORC1 but does not inhibit mTORC2. Some companies also are trialling PI3-kinase, AKT and PDK1 inhibitors, upstream regulators of mTOR.

The role of the pro-inflammatory cyclooxygenase pathway in the pathogenesis of PJS polyps has been studied in a mouse model by Udd et al.101 LKB1± mice were treated with 1500 ppm of celecoxib, a selective COX2 inhibitor. These mice were found to have a 54% reduction in polyp burden. A very small clinical trial within this study was carried out in six patients with documented STK11 mutations who were treated with 400 mg of celecoxib daily for 6 months. In two patients gastric polyp burden was reduced after treatment with celecoxib.

Metformin has been identified as a potential agent that could slow the development of neoplasia in PJS. Using a PTEN-deficient mouse model, Huang et al102 demonstrated that activation of the LKB1-AMPK pathway by metformin, phenformin or A-769662 significantly slowed tumour onset and identified the potential of metformin in polyposis syndromes associated with the dysregulation of LKB1 and PTEN.

Large cell calcified Sertoli cell tumours (LCST) can lead to gynaecomastia, which has been hypothesised to be due to an alteration in inhibin regulation. A small study examined the use of anastrozole, an aromatase inhibitor used for the treatment of breast carcinoma61 to inhibit the clinical features of LCST and found that oestradiol and inhibin levels decreased, suggesting that it may have a role in this condition. However, as these tumours have a malignant potential, bilateral orchidectomy is still recommended as a curative procedure.67

Conclusion: There are a number of potentially promising agents for reduction of polyp burden in PJS; however, none of these are in routine clinical use (Evidence level: IIb, Grade of recommendation: B)

Question: Is there any treatment to ameliorate the mucocutaneous pigmentation seen in PJS?

Although the mucocutaneous pigmentation seen in PJS may fade with age, it can be disfiguring and cause psychological stress. The use of filtered intense pulse light (IPL) with a 590 nm cut-off filter was reported in a single case whereby it led to a rapid improvement in the cosmetic appearance of the lesions.103 Similar improvements have also been described with Q-switched ruby laser104 105 and CO2-based lasers.106

Conclusion: Although there have been reports of success with intense pulsed light and laser therapy, their use cannot be supported in routine clinical practice. Its use should be reserved for cases with significant psychological morbidity related to pigmentation (Evidence level: IV, Grade of recommendation: C)

Discussion and conclusions

Peutz–Jeghers syndrome is a clinically diverse disease entity, with multiple neoplastic manifestations and a very high lifetime risk of developing malignancy. The current evidence for surveillance guidelines is weak due to the relative rarity of PJS and the lack of data addressing effectiveness and outcomes from surveillance in PJS.

Current surveillance guidelines are highly intensive. Several of the surveillance modalities presented here are invasive and the frequency at which they are carried out presents a significant burden for the PJS patient. Surveillance has two purposes in PJS patients: first, to reduce the polyp burden and the likelihood of polyp related complications, particularly intussusception, in the young PJS patient; and, second, cancer surveillance in the older PJS patient. We have attempted to reflect this in our guidelines. The main aim of surveillance in childhood should be reducing the risk of intussusception. As such we have recommended that endoscopic examination is less frequent in this age group compared to adult patients, where the main aim is detecting cancer at an early stage. Recommendations on surveillance, therapy and clinical management are summarised in boxes 1 and 2.

Box 1 Summary of recommendations for surveillance and follow-up

General

  • Annual full blood count (FBC), Liver function testing (LFT)

  • Annual clinical examination

Genital tract

  • Annual examination and testicular examination from birth until 12 years

  • Testicular ultrasound if abnormalities detected at examination

  • Cervical smear with LBC three yearly from age 25 years

Gastrointestinal

  • Baseline OGD/colonoscopy age 8

    • Polyps detected, continue three yearly until 50 years

    • No polyps detected, repeat age 18 years, then three yearly until 50 years

  • Colonoscopy 1–2 yearly after age 50 years

  • VCE every 3 years from age 8 years

Breast

  • Monthly self examination from age 18 years

  • Annual breast MRI from age 25–50, thereafter annual mammography

  • LBC, liquid-based cytology; MRI, magnetic resonance imaging; OGD, baseline colonoscopy and upper gastrointestinal endoscopy; VCE, video capsule endoscopy.

Box 2 Summary of guidelines and grading of recommendation

  1. Gastrointestinal surveillance using colonoscopy, upper GI endoscopy and video capsule endoscopy should be performed….GRADE C

  2. Magnetic resonance imaging mammography is recommended….GRADE C

  3. Pancreatic surveillance is not recommended….GRADE B

  4. Testicular examination and ultrasound is recommended….GRADE C

  5. Cervical smears are recommended….GRADE C

  6. Ovarian and uterine surveillance are not recommended….GRADE C

  7. An intraoperative enteroscopy should be performed on patients with Peutz–Jeghers syndrome who are undergoing laparotomy….GRADE B

  8. No pharmacological prophylaxis can be recommended for routine use….GRADE B

  9. Intense pulsed light and laser therapy, should be reserved for cases with significant psychological morbidity related to pigmentation….GRADE C

The lack of understanding regarding cancer development in PJS makes the generation of surveillance guidelines problematic, when one of the main aims is cancer detection/prevention. Studies to clarify cancer development and the malignant potential of PJS polyps are required and may have a significant impact on our current recommendations.

There is little research currently about potential biomarkers for the identification of early neoplasia, with the exception of colorectal (faecal occult blood, faecal k-RAS) and pancreatic lesions (k-RAS in pancreatic secretions), but these methods lack sensitivity and specificity and have only been applied previously to sporadic cancer. Radiological screening shows promise in certain tumour types; however, tumours such as ovarian carcinoma are difficult to diagnose effectively by conventional radiological methods until they have progressed beyond an early, pre-invasive stage.

Endoscopic polypectomy via upper GI endoscopy, colonoscopy and double-balloon enteroscopy has demonstrated its utility in reducing the need for future operative polypectomy from the small bowel. Double-balloon enteroscopy, however, can be a traumatic procedure and its use currently is limited to therapy rather than diagnosis. The development of capsule endoscopy has enhanced the diagnostic armamentarium available to the clinician and allows more thorough and regular surveillance of the small bowel for polyposis.

The mTOR pathway shows significant promise for modulation or limitation of progression of PJS polyps; however, clinical trials in this area are at a very early stage and involve some agents, such as everolimus/sirolimus that carry a risk of significant systemic toxicity. Intervention in the COX2 pathway also shows promise, although a very limited study has examined the role of celecoxib which has now been associated with increases in cardiovascular disease risk and therefore its long term use may not be suitable in this group.

In conclusion, guidelines for PJS are largely formed via consensus rather than a robust evidence base. Therapeutic interventions and surveillance modalities are expanding, but assessment of these is challenging given the rarity of the condition.

References

View Abstract

Footnotes

  • Competing interests None.

  • Provenance and peer review Not commissioned; externally peer reviewed.