Pituitary Tumor Surgery - factors influencing outcome
Abstract
Background: Pituitary tumors represent 15–20% of intracranial tumors. The majority are
benign adenomas, of which 30 % are hormonally inactive, the non-functioning pituitary
adenomas (NFPAs). A possible neuronal damage during treatment of pituitary tumors with
endoscopic transsphenoidal surgery (ETSS) has not been previously investigated, and
postoperative sinonasal morbidity is frequently overlooked. Current markers predicting
postoperative tumor progression of NFPAs are insufficient.
Aims: To quantify a possible neuronal and astroglial damage during ETSS and to assess
sinonasal morbidity before and six months after surgery. To investigate novel
immunohistochemical and epigenetic markers as predictive factors for postoperative tumor
progression in NFPAs.
Methods: In paper I, sequential blood sampling of brain injury biomarkers GFAP, tau and NFL
was performed before and after ETSS. Correlations between their increase and perioperative
factors and fatigue outcome were investigated. In paper II, sinonasal and self-reported general
health was assessed preoperatively and 6 months postoperatively with the Sinonasal Outcome
Test 22 (SNOT-22) and EQ-5D. In paper III and IV, tumoral expression of minichromosome
maintenance protein 7 (MCM7) and DNA-methylation patterns were studied regarding their
association with postoperative tumor progression in NFPAs.
Results: GFAP, tau and NFL increased postoperatively, with peaks at different time points. The
increase of GFAP and tau correlated to preoperative suprasellar tumor extension. At 6 months
after surgery, self-reported general health was improved, but rhinologic symptoms had
worsened. Increased MCM7 expression and specific DNA methylation patterns were associated
with postoperative tumor progression.
Conclusions: GFAP and tau might be markers of neuronal and/or astroglial damage during
ETSS, but the clinical significance needs to be further investigated. ETSS is generally welltolerated,
but rhinologic symptoms should not be overlooked during follow-up. MCM7 might be
a valuable adjunct as a predictive marker for postoperative tumor progression in NFPAs.
Specific methylation patterns might be used as epigenetic signatures predictive of tumor
progression in NFPAs.
Parts of work
I. Hallén T, Olsson D.S, Hammarstrand C, Farahmand D, Olofsson A-C, Jakobsson Ung E,
Jakobsson S, Bergquist H, Blennow K, Zetterberg H, Johannsson G, Skoglund T.
Circulating brain injury biomarkers increase after endoscopic surgery for pituitary
tumors. Submitted II. Hallén T, Olsson D.S, Farahmand D, Esposito D, Olofsson A-C, Jakobsson S, Jakobsson
Ung E, Sahlstrand-Johnson P, Johannsson G, Skoglund T, Bergquist H.
Sinonasal symptoms and self-reported health before and after endoscopic pituitary
surgery – a prospective study
J Neurol Surg B. 2021 Feb 18. ::doi::10.1055/s-0041-1722929 III. Hallén T, Olsson D.S, Hammarstrand C, Örndal C, Engvall A, Ragnarsson O, Skoglund T,
Johannsson G.
MCM7 as a marker of postsurgical progression in non-functioning pituitary
adenomas
Eur J Endocrinol. 2021;184(4):521-535. ::doi::10.1530/EJE-20-1086 IV. Hallén T, Johannsson G, Dahlén R, Glad, C, Örndal C, Engvall A, Carén H, Skoglund T,
Olsson D.S.
Genome-wide DNA methylation differences in non-functioning pituitary adenomas
with or without postsurgical tumor progression.
Manuscript
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Neuroscience and Physiology. Department of Clinical Neuroscience
Disputation
Fredagen den 28 maj 2021, kl 9.00, lokal 2119 Hälsovetarbacken, Medicinareberget, Göteborg. https://gu-se.zoom.us/j/63817014048?pwd=aTQyd0l4emQvaVVpWmozcE4ySEQ5dz09
Date of defence
2021-05-28
tobias.hallen@vgregion.se
Date
2021-05-05Author
Hallén, Tobias
Keywords
Endoscopic transsphenoidal surgery
biomarkers
glial fibrillary acidic protein
neurofilaments
tau protein
pituitary tumors
sinonasal health
tumor progression
predictive markers
MCM7
methylation patterns
NFPA
Publication type
Doctoral thesis
ISBN
978-91-8009-288-3 (PRINT)
978-91-8009-289-0 (PDF)
Language
eng