Introduction
Primary aldosteronism (PA) is the most common cause of secondary hypertension (HT),
accounting for up to 29% of cases of resistant HT and 14% in general practice. Familial
hyperaldosteronism (FH) is a rare cause of PA. The most common presentation of PA is
HT with normal potassium levels. PA is widely underdiagnosed, and diagnostic delay
reduces treatment efficacy. Early detection and specialized treatment are crucial as PA
carries significantly higher cardiovascular risk than essential HT. Adrenal venous
sampling (AVS) is the gold standard method to differentiate between unilateral and
bilateral PA. Adrenalectomy is potentially curative for the unilateral group, while
bilateral disease is managed with mineralocorticoid receptor antagonists (MRA).
Immunohistochemistry (IHC) has advanced the histopathological diagnosis of unilateral
PA and shown potential in predicting outcomes. Standardized methods for outcome
evaluation were introduced recently.
The aims of this thesis were to investigate the incidence of PA in Iceland during the
study period and assess whether it is underdiagnosed. Additionally, to compare results
from screening and confirmatory tests between AVS subgroups and evaluate treatment
outcomes. Another objective was to assess long-term outcomes and follow-up needs by
classifying patients based on IHC. Finally, we aimed to explore the role of the posture
test (PT) and screen the appropriate patients for FH.
Methods
In 2007, an evidence-based PA work-up protocol was introduced in Landspítali
National University Hospital of Iceland. The study cohort consisted of all adults
diagnosed with PA during the 10-year period 2007–2016. Screening was performed
by measuring morning serum aldosterone, direct renin concentration and 24-hour
urinary excretion of aldosterone (UEA). PA was confirmed through the recumbent saline
infusion test. All patients underwent adrenal computed tomography (CT) and a 4-hour
PT. AVS was used for subtyping. Unilateral PA was treated with laparoscopic
adrenalectomy and bilateral PA was managed with MRA. During follow-up visits, blood
pressure (BP) was measured, need for potassium supplementation evaluated, and
antihypertensive treatment assessed.
Outcomes were evaluated based on the alterations in BP, count of antihypertensives,
and need for potassium supplementation. Clinical outcomes were further assessed
using the Primary Aldosterone Surgical Outcome criteria and the Primary
Aldosteronism Medical Outcome criteria. IHC was performed to reevaluate routinely
stained tissue samples and histopathological diagnoses using The International
Histopathology Consensus for Unilateral Primary Aldosteronism (HISTALDO). Outcomes
v
were compared between HISTALDO subgroups and the need for follow-up was
evaluated. First-degree relatives within the study cohort were screened for FH.
Results
Between 2007 and 2016, the incidence of confirmed PA in Iceland was 58 cases, 47%
(n = 27) had unilateral disease and 53% (n = 31) bilateral. All patients had
hypokalaemia at case detection or during work-up. Compared to the bilateral group,
the unilateral group had a significantly higher UEA (33,9 vs. 24,6 μg, p < 0,001), post-
infusion aldosterone levels (385 vs. 251 pmol/l, p = 0,01), and a higher frequency of
adrenal nodules (19/27 vs. 10/31, p = 0,008). The bilateral group was significantly
more responsive to posture (206% vs. 56%, p = 0,002). The PT had 81% sensitivity
and 45% specificity for detecting bilateral PA. The combination of CT and PT was 96%
specific and 32% sensitive for detecting unilateral PA. The AVS success rate was 86%
(57/66), with 7/9 failed AVS performed on women (p = 0,08). Following IHC,
classical histopathology was identified in 85% (22/26) of the unilateral group, with
23% (6/26) alteration of histopathological diagnoses. During follow-up, both the
unilateral and bilateral group experienced significant reductions in systolic BP (p <
0,001, both groups), antihypertensive use (p = 0,002, p = 0,04, respectively), and
potassium supplementation needs (p < 0,001, both groups). All patients with classical
histopathology who achieved complete clinical success at 12 months (n = 5) remained
normotensive without antihypertensives throughout the follow-up period (4–10 years).
FH screening among brothers (n = 2) within the cohort yielded negative results.
Conclusions
This study highlights the underdiagnosis of PA in Iceland as the incidence was low and
all patients in the cohort had hypokalaemia. Most cases presented with severe PA,
emphasizing the need for increased awareness and broader screening indications at
earlier stages of the disease. Unilateral PA was associated with more severe disease at
presentation and a more significant reduction in antihypertensive use during follow-up,
indicating better treatment response. The combination of PT and CT was highly specific
for detecting unilateral PA. IHC improved histopathological diagnosis and was essential
for accurate diagnosis. Additionally, follow-up could be individualized based on IHC
results, though further research is needed to confirm this. Overall, our study underlines
the need for improved screening, a simpler work-up, and personalized treatment and
follow-up strategies to optimize PA care.
Frumkomið aldósterónheilkenni (FA) er algengasta orsök afleidds háþrýstings. Allt að
29% lyfjaþolins háþrýstings og 14% háþrýstings í heilsugæsluþýði orsakast af
sjúkdómnum. Arfgeng form FA eru sjaldgæf. Algengasta birtingarmynd sjúkdómsins er
háþrýstingur með eðlilegu blóðkalíumgildi. FA er víða vangreint og greiningartöf
dregur úr meðferðarárangri. Snemmgreining og sérhæfð meðferð skipta sköpum því
sjúkdómnum fylgir aukin hættu á hjarta- og æðaáföllum samanborið við frumkominn
háþrýsting. Nýrnahettubláæðaþræðing (NHBÞ) er áreiðanlegasta aðferðin til mats á því
hvort FA er í annarri eða báðum nýrnahettum (einhliða eða tvíhliða).
Nýrnahettubrottnám getur veitt lækningu ef einhliða en tvíhliða sjúkdómur er
meðhöndlaður með aldósterón-viðtakahindrum. Sértæk mótefni hafa bætt
vefjagreiningu í einhliða FA. Staðlaðar aðferðir við mat á meðferðarárangri komu fram
nýlega.
Markmið rannsóknarinnar voru að kanna nýgengi FA á rannsóknartímabilinu og meta
hvort sjúkdómurinn sé vangreindur á Íslandi. Ennfremur að gera samanburð á
niðurstöðum úr skimun og frekari uppvinnslu á milli undirhópa og meta
meðferðarsvörun. Einnig að meta áreiðanleika stöðuprófs og vægi sértækrar
mótefnalitunar með tilliti til áreiðanleika greiningar og þarfar á eftirfylgd. Loks var
kannað hvort arfgeng form FA fyndust innan þýðisins.
Locked until 2027-01-01