Molecular diagnosis of pituitary adenoma predisposition caused by aryl hydrocarbon receptor-interacting protein gene mutations

Georgitsi, Marianthi; Raitila, Anniina; Karhu, Auli; Tuppurainen, Karoliina; Mäkinen, Markus J.; Vierimaa, Outi; Paschke, Ralf; Saeger, Wolfgang; Luijt, Rob B. van der; Sane, Timo; Robledo, Mercedes; Menis, Ernesto De; Weil, Robert J.; Wasik, A.; Zieliński, Grzegorz; Lucewicz, Olga; Lubiński, Jan; Launonen, Virpi; Vahteristo, Pia; Aaltonen, Lauri A.

doi:10.1073/pnas.0700004104

Cited by 170 publications

(179 citation statements)

References 38 publications

(36 reference statements)

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“…Bold represents the more likely at-risk haplotype shared by at least two subjects. near 7% (7,8). This prevalence reaches 14.3% in patients with GH-secreting tumors diagnosed before 25 years old (28).…”

Section: Discussionmentioning

confidence: 90%

“…In 2006, Vierimaa et al (4) identified mutations in the aryl hydrocarbon receptor interacting protein (AIP) gene in the familial setting of PA. In FIPA kindreds, AIP mutations occur in 15-20% of cases (5), whereas they occur at a very low frequency in sporadic cases, between 0 and 4% (6,7,8,9). Because patients mutated for AIP (AIPmut) have typically early onset disease and larger PA compared with controls (10), Tichomirowa et al (11) performed AIP screening in young patients with isolated sporadic macroadenomas and identified that nearly 12% of patients had germline AIP mutations.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Genetic analysis in young patients with sporadic pituitary macroadenomas: besides AIP don't forget MEN1 genetic analysis

Cuny

Pertuit

Sahnoun-Fathallah

et al. 2013

European Journal of Endocrinology

144

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Context: Germline mutations in the aryl hydrocarbon receptor interacting protein gene (AIP) have been identified in young patients (age %30 years old) with sporadic pituitary macroadenomas. Otherwise, there are few data concerning the prevalence of multiple endocrine neoplasia type 1 (MEN1) mutations in such a population. Objective: We assessed the prevalence of both AIP and MEN1 genetic abnormalities (mutations and large gene deletions) in young patients (age %30 years old) diagnosed with sporadic and isolated macroadenoma, without hypercalcemia and/or MEN1-associated lesions. Design: The entire coding sequences of AIP and MEN1 were screened for mutations. In cases of negative sequencing screening, multiplex ligation-dependent probe amplification was performed for the detection of large genetic deletions. Patients and settings: One hundred and seventy-four patients from endocrinology departments of 15 French University Hospital Centers were eligible for this study. Results: Twenty-one out of 174 (12%) patients had AIP (nZ15, 8.6%) or MEN1 (nZ6, 3.4%) mutations. In pediatric patients (age %18 years old), AIP/MEN1 mutation frequency reached nearly 22% (nZ10/46). AIPmut and MEN1mut were identified in 8/79 (10.1%) and 1/79 (1.2%) somatotropinoma patients respectively; they each accounted for 4/74 (5.4%) prolactinoma (PRL) patients with mutations. Half of those patients (nZ3/6) with gigantism displayed mutations in AIP. Interestingly, 4/12 (33%) patients with non-secreting adenomas bore either AIP or MEN1 mutations, whereas none of the eight corticotroph adenomas or the single thyrotropinoma case had mutations. No large gene deletions were observed in sequencing-negative patients. Conclusion: Mutations in MEN1 can be of significance in young patients with sporadic isolated pituitary macroadenomas, particularly PRL, and together with AIP, we suggest genetic analysis of MEN1 in such a population.

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Section: Discussionmentioning

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Genetic analysis in young patients with sporadic pituitary macroadenomas: besides AIP don't forget MEN1 genetic analysis

Cuny

Pertuit

Sahnoun-Fathallah

et al. 2013

European Journal of Endocrinology

144

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“…From a cohort of 74 pediatric patients with isolated CD, one presented with AIP and two with MEN1 mutations (14). Altogether, mutations in MEN1, AIP, CDKN1B or CDKN2C (encoding p18/INK4C) are rarely found in patients with CD (14,15,19,20). These features point to evidence against inheritance caused by germline mutations and suggest an acquired genetic basis of CD.…”

Section: Genetic Events In CDmentioning

confidence: 96%

Decoding the genetic basis of Cushing's disease: USP8 in the spotlight

Theodoropoulou

Reincke

Faßnacht

et al. 2015

European Journal of Endocrinology

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Cushing's disease (CD) arises from pituitary-dependent glucocorticoid excess due to an ACTH-secreting corticotroph tumor. Genetic hits in oncogenes and tumor suppressor genes that afflict other pituitary tumor subtypes are not found in corticotrophinomas. Recently, a somatic mutational hotspot was found in up to half of corticotrophinomas in the USP8 gene that encodes a protein that impairs the downregulation of the epidermal growth factor receptor (EGFR) and enables its constitutive signaling. EGF is an important regulator of corticotroph function and its receptor is highly expressed in Cushing's pituitary tumors, where it leads to increased ACTH synthesis in vitro and in vivo. The mutational hotspot found in corticotrophinomas hyper-activates USP8, enabling it to rescue EGFR from lysosomal degradation and ensure its stimulatory signaling. This review presents new developments in the study of the genetics of CD and focuses on the USP8-EGFR system as trigger and target of corticotroph tumorigenesis.

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“…This suggests that amino acid substitutions, such as R16H for instance, could be expected to have functional significance. Indeed, since we reported germline R16H changes in a FIPA family, others have noted similar mutations in four sporadic pituitary adenoma patients and also in the germline and tumors of two patients with colorectal carcinoma (and family histories of colorectal, carcinoid, and other tumors) (47,48). A full appreciation of the effect of R16H on AIP expression and/or function will be required to determine whether this is Familial isolated pituitary adenomas truly a pathogenic mutation.…”

Section: The Genetics Of Fipamentioning

confidence: 99%

“…With the identification of AIP mutations as being involved in the etiology of familial pituitary tumors, the issue of screening has been raised (47). In particular, it has been suggested that immunohistochemistry for AIP in pituitary tumor tissue be used to screen operated patients for mutations.…”

Section: Perspectivesmentioning

confidence: 99%

The clinical, pathological, and genetic features of familial isolated pituitary adenomas

Beckers¹,

Daly²

2007

eur j endocrinol

153

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Pituitary adenomas occur in a familial setting in multiple endocrine neoplasia type 1 (MEN1) and Carney's complex (CNC), which occur due to mutations in the genes MEN1 and PRKAR1A respectively. Isolated familial somatotropinoma (IFS) is also a well-described clinical syndrome related only to patients with acrogigantism. Pituitary adenomas of all types -not limited to IFS -can occur in a familial setting in the absence of MEN1 and CNC; this phenotype is termed familial isolated pituitary adenomas (FIPA). Over the past 7 years, we have described over 90 FIPA kindreds. In FIPA, both homogeneous and heterogeneous pituitary adenoma phenotypes can occur within families; virtually all FIPA kindreds contain at least one prolactinoma or somatotropinoma. FIPA differs from MEN1 in terms of a lower proportion of prolactinomas and more frequent somatotropinomas in the FIPA cohort. Patients with FIPA are significantly younger at diagnosis and have significantly larger pituitary adenomas than matched sporadic pituitary adenoma counterparts. A minority of FIPA families overall (15%) exhibit mutations in the aryl hydrocarbon receptor-interacting protein (AIP) gene; AIP mutations are present in only half of IFS kindreds occurring as part of the FIPA cohort. In families with AIP mutations, pituitary adenomas have a penetrance of over 50%. AIP mutations are extremely rare in patients with sporadic pituitary adenomas. This review deals with pituitary adenomas that occur in a familial setting, describes in detail the clinical, pathological, and genetic features of FIPA, and addresses aspects of the clinical approach to FIPA families with and without AIP mutations.

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Molecular diagnosis of pituitary adenoma predisposition caused by aryl hydrocarbon receptor-interacting protein gene mutations

Cited by 170 publications

References 38 publications

Genetic analysis in young patients with sporadic pituitary macroadenomas: besides AIP don't forget MEN1 genetic analysis

Genetic analysis in young patients with sporadic pituitary macroadenomas: besides AIP don't forget MEN1 genetic analysis

Decoding the genetic basis of Cushing's disease: USP8 in the spotlight

The clinical, pathological, and genetic features of familial isolated pituitary adenomas

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