Is it time to consider the expression of specific-pituitary hormone genes when typifying pituitary tumours?

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Abstract

The aim of the present study is to check whether we can replicate, in an independent series, previous results showing that the molecular study of pituitary-specific gene expression complements the inmunohistochemical identification of pituitary neuroendocrine tumours. We selected 112 patients (51 (46.4%) women; mean age 51.4±16 years; 102 macroadenomas (91.9%), 9 microadenomas (8.1%)) with complete clinical, radiological, immunohistochemical and molecular data from our data set of pituitary neuroendocrine tumours. Patients were different from those previously studied. We measured the expression of the pituitary-specific hormone genes and type 1 corticotrophin-releasing hormone and arginine vasopressin 1b receptors, by quantitative real-time polymerase chain reaction using TaqMan probes. Afterwards, we identified the different pituitary neuroendocrine tumour subtypes following the 2017 World Health Organization classification of pituitary tumours, calculating the concordance between their molecular and immuhistochemical identification. The concordance between molecular and immunohistochemical identification of functioning pituitary neuroendocrine tumours with the clinical diagnosis was globally similar to the previous series, where the SYBR Green technique was used instead of TaqMan probes. Our results also corroborated the poor correlation between molecular and immunohistochemical detection of the silent pituitary neuroendocrine tumour variants. This discrepancy was more remarkable in lactotroph, null-cell and plurihormonal pituitary neuroendocrine tumours. In conclusion, this study validates the results previously published by our group, highlighting a complementary role for the molecular study of the pituitary-specific hormone genes in the typification of pituitary neuroendocrine tumours subtypes.

Figures

  • Table 1. PitNET subtypes identified by the immunohistochemical and molecular studies in the present series.
  • Table 2. Classification and prevalence of the different PitNET subtypes according to their clinical (functioning and silent), molecular and IHC identification.
  • Table 3. Concordance between IHC and molecular identification of subtypes of functioning PitNET with clinical diagnosis.
  • Fig 1. Linear regression between PRL gene expression in seven functioning lactotropinomas and the dose of cabergoline administered prior to surgery.
  • Table 4. Concordance between molecular and IHC identification in functioning and silent variants of PitNET.
  • Table 5. Concordance between molecular and IHC identification of functioning PitNET subtypes with clinical diagnosis in the present series and in the previous one.
  • Table 6. Concordance between molecular and IHC identification in silent functioning PitNET subtypes in the present series and in the previous one.

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CITATION STYLE

APA

García-Martínez, A., Sottile, J., Fajardo, C., Riesgo, P., Cámara, R., Simal, J. A., … Pico, A. (2018). Is it time to consider the expression of specific-pituitary hormone genes when typifying pituitary tumours? PLoS ONE, 13(7). https://doi.org/10.1371/journal.pone.0198877

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