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Inicio Endocrinología, Diabetes y Nutrición (English ed.) Genetic Testing in Pituitary Adenomas: What, How, and In Whom?
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Vol. 66. Issue 2.
Pages 71-73 (February 2019)
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Vol. 66. Issue 2.
Pages 71-73 (February 2019)
Editorial
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Genetic Testing in Pituitary Adenomas: What, How, and In Whom?
Genética en adenomas hipofisarias: ¿qué, cómo y a quién?
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Adrian F. Daly
Corresponding author
adrian.daly@ulg.ac.be

Autor para correspondencia.
, Albert Beckers
Department of Endocrinology, Centre Hospitalier Universitaire de Liège, Liège University, Domaine Universitaire du Sart Tilman, 4000, Liège, Belgium
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Clinically diagnosed pituitary adenomas have a prevalence of approximately 1 per 1000 in the general population in Europe and are therefore encountered regularly by clinical endocrinologists in everyday practice1. Currently, it is believed that most pituitary adenomas arise from a clonal expansion derived from a somatic mutation in a single cell. For instance, a somatic mutation in GNAS is found in up to 40% of somatotropinomas in patients with acromegaly, while somatic USP8 mutations are now known to account for many cases of Cushing's disease2,3. Such pituitary level mutations are only discovered post hoc following tumor resection, cannot readily be predicted in advance and are not inheritable. Germline mutations in genes associated with pituitary adenomas are quite rare, and overall, pituitary adenomas occurring in an inheritable or familial setting account for about 5% of cases4. As they are rare, generalized screening of pituitary adenoma patient populations to identify genetic mutation carriers is not currently a scientifically or economically valid approach. Most of these genetic causes are associated with a clinical presentation that differs from other pituitary adenomas, and these characteristics can be used to refine screening significantly.

In general, when considering genetic analyses in pituitary adenoma patients a good first step is to determine if the tumor is isolated to the pituitary or forms part of a multi-organ tumor syndrome. Pituitary adenomas can form part of classical endocrine tumor syndromes, such as, multiple endocrine neoplasia types 1 (MEN1) and 4 (MEN4), Carney complex and McCune-Albright syndrome (MAS)5. The initial clinical investigation of the patient with a pituitary adenoma should include a detailed personal and family history about tumors and pathologies at other sites, particularly in endocrine tissues6,7. Similarly, the family history should specifically search for related individuals with pituitary adenomas.

The focus for genetic testing in pituitary adenomas should primarily be on three main groups: pediatric-adolescent patients, those with a family history of pituitary adenomas and patients with a personal/family history suggestive of an endocrine tumor syndrome.

Pediatric and adolescent patients are a particularly important population, as certain genetic abnormalities leading to pituitary adenomas present more often in the young. For example, in MEN1, pituitary adenomas can have an early age at presentation, and testing guidelines recommend surveillance beginning as early as 5 years of age8. In MEN1, pituitary adenomas are generally larger and more difficult to control hormonally than non-MEN1 cases. Pituitary gigantism, by definition a disease that begins at an early age, is a high priority for genetic testing as nearly 50% of cases have a known genetic cause, such as AIP mutations/deletions (29%), X-LAG syndrome (10%), McCune-Albright syndrome (5%), and MEN1 or Carney complex (1% each) 9.

Isolated pituitary adenomas can also occur in a hereditary setting as part of familial isolated pituitary adenomas (FIPA); FIPA is diagnosed in kindreds that have at least two pituitary adenomas in related individuals but in the absence of syndromic features in other organs, such as, MEN17. Mutations in the AIP gene explain about 15-25% of FIPA families. AIP mutations have quite a low penetrance and about 20% of mutation carriers will develop a clinically significant pituitary adenoma7. While AIP mutations can lead to all subtypes of pituitary adenomas, they usually cause growth hormone-secreting (GH) or mixed GH-prolactin secreting pituitary macroadenomas during childhood or adolescence. While they most often occur in the setting of FIPA, AIP mutation related pituitary adenomas also can occur in isolated patients with young onset, large macroadenomas. In acromegaly, AIP mutated patients can be difficult to control, due to high levels of hormonal secretion and poor hormonal and tumoral responses to first-generation somatostatin analogs7.

X-linked acrogigantism (X-LAG) syndrome is rare but has a very typical presentation as isolated GH-secreting pituitary adenoma and/or hyperplasia causing overgrowth that begins usually in the first 12 months of life10. It is due to a microduplication on chromosome Xq26.3 that encompasses the gene GPR101 and if untreated leads to very severe pituitary gigantism. Diagnosis is made using array comparative genome hybridisation (aCGH). X-LAG syndrome can occur in rare gigantism-only FIPA families11. Also, low-level somatic mosaicism is seen in male sporadic patients, which can be detected using specific ddPCR assays12.

Apart from MEN1 some other syndromic conditions include pituitary adenomas 4. MEN4 is due to CDKN1B mutations, and is a rare syndrome seen in MEN1 negative individuals and kindreds. As relatively few pituitary adenomas have been described in MEN4, there is no specific phenotype to direct genetic testing and CDKN1B mutations have not been reported in patients with isolated pituitary adenomas. Carney complex is due to germline PRKAR1A mutations and is a multiorgan syndrome involving the adrenals, skin, testes and many other sites. Pituitary adenomas (generally GH secreting) occur in 10% of patients with Carney complex, although many patients will have disorders of GH, insulin-like growth factor 1 (IGF1) or prolactin on hormonal testing in the absence of a pituitary adenoma. MEN1, CDKN1B and PRKAR1A mutations are not considered to be an important cause of isolated sporadic pituitary adenomas.

Mosaicism may also occur in patients with isolated and syndromic pituitary adenomas. In McCune-Albright syndrome, for instance, a post-zygotic, activating mutation in the GNAS gene can lead to variable proportions of mutated and wild-type cells across different tissues. Traditional sequencing of GNAS for mutations in McCune-Albright syndrome is often negative for technical reasons due to low levels of mutated allele in blood or tumor specimens. Recently, droplet digital PCR (ddPCR) and related techniques have been validated to diagnose very low levels of the mutant GNAS allele in blood and tissue DNA, thereby facilitating routine diagnosis13. Early genetic confirmation of MAS is important for disease surveillance in the affected individual (it is not currently believed to be hereditary). This is particularly true for somatotropinomas in MAS which can have an early onset, exacerbate co-existing craniofacial fibrous dysplasia and are challenging to treat.

One further syndromic situation of growing interest is the potential for a pituitary adenoma, pheochromocytoma/paraganglioma association (3PA)14. In individuals or kindreds presenting with 3PA, a number of mutated genes have been identified, including the succinate dehydrogenase subunit genes (SDHx); recently, mutations and intragenic deletions in MAX have also been implicated in 3PA15.

The increasing number of genes associated with pituitary adenomas has also been accompanied by an expansion in the methodologies needed to correctly identify pathological variations. Rather than Sanger sequencing of individual genes, most reference laboratories have migrated to Next Generation Sequencing (NGS) panels, which allow for parallel analyses of multiple potential genetic targets. Other methodologies need to be considered for specific conditions, such as aCGH for XLAG syndrome, or digital PCR, as mentioned above. Also, multiplex ligation dependent probe amplification (MLPA) kits are available to identify whole or partial gene deletions. MLPA has proven useful in identifying whole or intragenic deletions in genes such as MEN1, AIP, SDHx, and MAX, in patients and families with normal sequencing results.

Although rare, genetic causes of pituitary adenomas are important to be aware of, as their overall clinical course is often complicated by aggressive tumor characteristics and treatment is more difficult. Early diagnosis of genetic causes is important to allow for proper screening for syndromic disease and to counsel and identify at-risk mutation carriers. The increasing number of causative genes and emerging clinical syndromes means that clinical endocrinologists will increasingly act in partnership with clinical geneticists to optimise the management of patients with pituitary adenomas.

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