TY - JOUR
T1 - Copeptin adaptive response to SGLT2 inhibitors in patients with type 2 diabetes mellitus: The GliRACo study
AU - AM, Berton
AU - Parasiliti-Caprino, M
AU - Prencipe, N
AU - Bioletto, F
AU - Lopez, C
AU - Bona, C
AU - CAPUTO, Marina
AU - Rumbolo, F
AU - Ponzetto, F
AU - Settanni, F
AU - Gasco, V
AU - Mengozzi, G
AU - Ghigo, E
AU - Grottoli, S
AU - Maccario, M
AU - AS, Benso
PY - 2023
Y1 - 2023
N2 - Introduction: In type 2 diabetes mellitus (T2DM), the antidiuretic system
participates in the adaptation to osmotic diuresis further increasing urinary
osmolality by reducing the electrolyte-free water clearance. Sodium glucose
co-transporter type 2 inhibitors (SGLT2i) emphasize this mechanism, promoting
persistent glycosuria and natriuresis, but also induce a greater reduction
of interstitial fluids than traditional diuretics. The preservation of osmotic
homeostasis is the main task of the antidiuretic system and, in turn, intracellular
dehydration the main drive to vasopressin (AVP) secretion. Copeptin is a stable
fragment of the AVP precursor co-secreted with AVP in an equimolar amount.
Aim: To investigate the copeptin adaptive response to SGLT2i, as well as the
induced changes in body fluid distribution in T2DM patients.
Methods: The GliRACo study was a prospective, multicenter, observational
research. Twenty-six consecutive adult patients with T2DM were recruited and
randomly assigned to empagliflozin or dapagliflozin treatment. Copeptin, plasma
renin activity, aldosterone and natriuretic peptides were evaluated at baseline
(T0) and then 30 (T30) and 90 days (T90) after SGLT2i starting. Bioelectrical
impedance vector analysis (BIVA) and ambulatory blood pressure monitoring
were performed at T0 and T90.
Results: Among endocrine biomarkers, only copeptin increased at T30, showing
subsequent stability (7.5 pmol/L at T0, 9.8 pmol/L at T30, 9.5 pmol/L at T90;
p = 0.001). BIVA recorded an overall tendency to dehydration at T90 with a stable
proportion between extra- and intracellular fluid volumes. Twelve patients (46.1%)
had a BIVA overhydration pattern at baseline and 7 of them (58.3%) resolved this
condition at T90. Total body water content, extra and intracellular fluid changes
were significantly affected by the underlying overhydration condition (p < 0.001),
while copeptin did not.
Conclusion: In patients with T2DM, SGLT2i promote the release of AVP, thus
compensating for persistent osmotic diuresis. This mainly occurs because of
a proportional dehydration process between intra and extracellular fluid (i.e.,
intracellular dehydration rather than extracellular dehydration). The extent of fluid
reduction, but not the copeptin response, is affected by the patient’s baseline
volume conditions
AB - Introduction: In type 2 diabetes mellitus (T2DM), the antidiuretic system
participates in the adaptation to osmotic diuresis further increasing urinary
osmolality by reducing the electrolyte-free water clearance. Sodium glucose
co-transporter type 2 inhibitors (SGLT2i) emphasize this mechanism, promoting
persistent glycosuria and natriuresis, but also induce a greater reduction
of interstitial fluids than traditional diuretics. The preservation of osmotic
homeostasis is the main task of the antidiuretic system and, in turn, intracellular
dehydration the main drive to vasopressin (AVP) secretion. Copeptin is a stable
fragment of the AVP precursor co-secreted with AVP in an equimolar amount.
Aim: To investigate the copeptin adaptive response to SGLT2i, as well as the
induced changes in body fluid distribution in T2DM patients.
Methods: The GliRACo study was a prospective, multicenter, observational
research. Twenty-six consecutive adult patients with T2DM were recruited and
randomly assigned to empagliflozin or dapagliflozin treatment. Copeptin, plasma
renin activity, aldosterone and natriuretic peptides were evaluated at baseline
(T0) and then 30 (T30) and 90 days (T90) after SGLT2i starting. Bioelectrical
impedance vector analysis (BIVA) and ambulatory blood pressure monitoring
were performed at T0 and T90.
Results: Among endocrine biomarkers, only copeptin increased at T30, showing
subsequent stability (7.5 pmol/L at T0, 9.8 pmol/L at T30, 9.5 pmol/L at T90;
p = 0.001). BIVA recorded an overall tendency to dehydration at T90 with a stable
proportion between extra- and intracellular fluid volumes. Twelve patients (46.1%)
had a BIVA overhydration pattern at baseline and 7 of them (58.3%) resolved this
condition at T90. Total body water content, extra and intracellular fluid changes
were significantly affected by the underlying overhydration condition (p < 0.001),
while copeptin did not.
Conclusion: In patients with T2DM, SGLT2i promote the release of AVP, thus
compensating for persistent osmotic diuresis. This mainly occurs because of
a proportional dehydration process between intra and extracellular fluid (i.e.,
intracellular dehydration rather than extracellular dehydration). The extent of fluid
reduction, but not the copeptin response, is affected by the patient’s baseline
volume conditions
KW - arginine-vasopressin
KW - sodium glucose co-transporter type 2 inhibitors
KW - osmotic
homeostasis
KW - extracellular fluid
KW - bioelectrical impedance vector analysis
KW - reninangiotensin-aldosterone system
KW - arginine-vasopressin
KW - sodium glucose co-transporter type 2 inhibitors
KW - osmotic
homeostasis
KW - extracellular fluid
KW - bioelectrical impedance vector analysis
KW - reninangiotensin-aldosterone system
UR - https://iris.uniupo.it/handle/11579/169003
M3 - Article
SN - 1662-4548
JO - Frontiers in Neuroscience
JF - Frontiers in Neuroscience
ER -
