SELF-REPORTED HYPOGLYCAEMIA IN PATIENTS TREATED WITH INSULIN: 
A LARGE SLOVENIAN RETROSPECTIVELY-PROSPECTIVE STUDY
Draženka PONGRAC BARLOVIČ1*, Andrej ZAVRATNIK2, Aleš SKVARČA1, Karmen JANŠA3, 
Bojana VUKELIČ4, Marjeta TOMAŽIČ1, Maja RAVNIK OBLAK1
1University Medical Centre Ljubljana, Clinical Department of Endocrinology, Diabetes and Metabolic Diseases, 
Zaloska 7, 1000 Ljubljana, Slovenia
2University Medical Centre Maribor, Ljubljanska 5,  2000 Maribor, Slovenia
3General Hospital Jesenice, Cesta marsala Tita 112, 4270 Jesenice, Slovenia
4General Hospital Novo Mesto, Smihelska cesta 1, 8000 Novo Mesto, Slovenia
Received: Feb 14, 2017
Accepted: Aug 10, 2017 
Original scientific article
Introduction. Hypoglycaemia is the major barrier for glycaemic target achievement in patients treated with 
insulin. The aim of the present study was to investigate real-world incidence and predictors of hypoglycaemia 
in insulin-treated patients.
Methods. More than 300 consecutive patients with type 1 or type 2 diabetes treated with insulin were 
enrolled during regular out-patient visits from 36 diabetes practices throughout the whole country. They 
completed a comprehensive questionnaire on hypoglycaemia knowledge, awareness, and incidence in the last 
month and last six months. In addition, in the prospective part, patients recorded incidence of hypoglycaemic 
events using a special diary prospectively on a daily basis, through 4 weeks.
Results. At least one hypoglycaemic event was self-reported in 84.1%, and 56.4% of patients with type 1 and 
type 2 diabetes, respectively, during the prospective period of 4 weeks. 43.4% and 26.2% of patients with 
type 1 and type 2 diabetes, respectively, experienced a nocturnal hypoglycaemic event. In the same time-
period, severe hypoglycaemia was experienced by 15.9% and 7.1% of patients with type 1 and type 2 diabetes, 
respectively. Lower glycated haemoglobin was not a significant predictor of hypoglycaemia.
Conclusions. Rates of self-reported hypoglycaemia in patients treated with insulin in the largest and 
most comprehensive study in Slovenia so far are higher than reported from randomised control trials, but 
comparable to data from observational studies. Hypoglycaemia incidence was high even with high glycated 
haemoglobin values.
Uvod. Hipoglikemije so glavni omejujoči dejavnik varnega doseganja glikemičnih ciljev pri bolnikih s 
sladkorno boleznijo, ki se zdravijo z insulinom. Namen te raziskave je bil raziskati pojavnost hipoglikemij in 
napovedne dejavnike hipoglikemij v vsakodnevnem življenju bolnikov s sladkorno boleznijo.
Metode. V raziskavo smo vključili več kot 300 zaporednih bolnikov s sladkorno boleznijo tipa 1 ali 2, 
zdravljenih z insulinom, iz 36 diabetoloških ambulant po državi. Bolniki so izpolnili natančen vprašalnik, ki 
je poizvedoval o znanju o hipoglikemijah, njihovemu zaznavanju in pojavnosti v zadnjem mesecu in v zadnjih 
šestih mesecih. V nadaljevalnem, prospektivnem delu raziskave, ki je trajal 1 mesec, so bolniki vsakodnevno 
beležili dnevnik hipoglikemij, kamor so sproti vpisovali, ali so doživeli hipoglikemijo.
Rezultati. V raziskavo je bilo vključenih 84 bolnikov s sladkorno boleznijo tipa 1 in 227 bolnikov s sladkorno 
boleznijo tipa 2. Med enomesečnim prospektivnim delom raziskave je 84,1% bolnikov s sladkorno boleznijo 
tipa 1 in 56,4% bolnikov s sladkorno boleznijo tipa 2 poročalo, da so doživeli vsaj eno hipoglikemijo. Nočno 
hipoglikemijo je doživelo 43,4% bolnikov s sladkorno boleznijo tipa 1 in 26,2% bolnikov s sladkorno boleznijo 
tipa 2. Hudo hipoglikemijo je doživelo 15,9 % bolnikov s sladkorno boleznijo tipa 1 in 7,1% bolnikov s 
sladkorno boleznijo tipa 2. Nižji glikiran hemoglobin ni bil napovedni dejavnik za pojav hipoglikemij.
Zaključki. Incidenca hipoglikemij, o katerih so poročali sami bolniki, zdravljeni z insulinom, je v doslej 
največji raziskavi o hipoglikemijah na Slovenskem višja kot v velikih randomiziranih prospektivnih raziskavah, 
a primerljiva kot v podobnih opazovalnih raziskavah iz vsakodnevnega življenja. Incidenca hipoglikemij je 
visoka tudi pri bolnikih z visokim glikiranim hemoglobinom.
ABSTRACT
Keywords: 
hypoglycaemia, 
type 1 diabetes, 
type 2 diabetes, 
insulin treatment, 
Slovenia
IZVLEČEK
Ključne besede: 
hipoglikemija, 
sladkorna bolezen tipa 1, 
sladkorna bolezen tipa 2, 
insulinsko zdravljenje, 
Slovenija
*Corresponding author: Tel: + 386 1 522 39 90; E-mail: drazenka.pongrac@gmail.com
10.1515/sjph-2017-0033 Zdr Varst 2017; 56(4): 244-250
HIPOGLIKEMIJE PRI BOLNIKIH, ZDRAVLJENIH Z INSULINOM: 
VELIKA SLOVENSKA RETROSPEKTIVNOPROSPEKTIVNA RAZISKAVA
Pongrac Barlovič D, Zavratnik A, Skvarča A, Janša K, Vukelič B, Tomažič M, Ravnik Oblak M. Self-reported hypoglycaemia in patients treated with insulin: a large 
Slovenian retrospectively-prospective study. Zdr Varst 2017; 56(4): 244-250.
244
© Nacionalni inštitut za javno zdravje, Slovenija. 
1 INTRODUCTION
Intensive hyperglycaemia treatment reduces the risk 
of development of chronic diabetes complications. 
However, the main obstacle to attain tight glycaemic 
goals is the risk of hypoglycaemia (1). In addition, 
experiencing hypoglycaemia, especially a nocturnal one, 
decreases quality of life substantially (2). Moreover, 
severe hypoglycaemia, requiring external assistance for 
recovery, was associated with increased cardiovascular 
and overall mortality (3).
Data on hypoglycaemia incidence are variable, mainly 
because of the lack of a single threshold plasma glucose 
concentration that defines hypoglycaemia in diabetes. 
Typically, it is believed that hypoglycaemia incidence 
is high in type 1 diabetes, but not in type 2 diabetes. 
Yet, incidence of hypoglycaemia increases with type 2 
diabetes duration (4, 5). Reported incidence of severe 
hypoglycaemia in retrospective observational studies in 
patients with longstanding type 1 diabetes was 320 cases 
per 100 patient-years (6). Of note, substantially lower 
incidence was established from a prospective randomised 
DCCT trial, with 62 cases per 100 patient-years (7). On 
the other hand, in patients with type 2 diabetes, severe 
hypoglycaemia incidence was 70 per 100 patient-years in 
observational studies (6), whereas it was only 3.1 per 100 
patient-years in a multicentre, prospective, randomised 
ACCORD study (8).
Hypoglycaemia incidence in patients treated with insulin 
in Slovenia was never systematically studied. Therefore, 
the aim of the present study was to assess hypoglycaemia 
incidence in insulin-treated patients with type 1 and type 
2 diabetes mellitus as patients report it, and to investigate 
factors, associated with hypoglycaemia risk.
2 METHODS
This was a multicentre, non-interventional study, designed 
to assess hypoglycaemia incidence in patients with type 
1 and type 2 diabetes, treated with insulin. The study 
protocol, with hypoglycaemia classification and statistical 
analyses was in detail described elsewhere (9).
During the routine, out-patient visits with diabetologists, 
from 474 consecutive patients from 36 clinical sites in 
Slovenia invited to participate, 311 were enrolled in 
the study. The sites were quite uniformly distributed 
throughout Slovenia. The biggest number of patients 
was recruited from the north-western Slovenia, the only 
region without any patients included was the Slovenj 
Gradec region. The average number of patients per site 
was 8.6, per region 39. Minimal number of patients per 
region was 10 (Murska Sobota), maximal 75 (Gorenjska). 
Patients included were more than 18 years old, had type 
1 or type 2 diabetes mellitus, with at least 12 months 
of insulin treatment experience, and had signed the 
informed consent. The exclusion criterion was the inability 
to complete a written questionnaire and a hypoglycaemia 
diary. Patients were not given any financial payment for 
the participation in the study.
Baseline characteristics of the patients analysed are 
presented in Table 1. More than two thirds of patients had 
type 2 diabetes mellitus.
10.1515/sjph-2017-0033 Zdr Varst 2017; 56(4): 244-250
245
Table 1. Baseline characteristics of patients included.
*Non-normally distributed variables are represented as median 
(25th, 75th percentile) 
Age (years)
Gender (male/female, %)
Diabetes duration (years)
Insulin therapy duration (years)
HbA1c (%)
Employed/unemployed/retired/other (%)
Diabetes treatment
 Short-acting insulin
 Long-acting insulin
 Pre-mixed insulin
Oral therapy
 Injectable non-insulin therapy
 Insulin pump
Self-measurement of blood glucose (%)
Continuous glucose measurement (%)
Hypoglycaemia experience (%)
49±13
57/43
21±11
19±12
9.2±2.7
65/5/28/12
85.7
60.7
1.2
4.8
3.6
32.1
98.8
34.2
98.8
64±10
62/38
16±9
6 (3, 10)*
9.3±2.8
15/8/75/2
48.9
63.1
35.1
24.9
10.2
4.9
99.6
38.4
89.2
DM type 1
N=84
DM type 2
N=227
The study was comprised of two parts: a retrospective 
6-month period and a prospective 4-week period. In 
the retrospective part, patients were asked to recall a 
6-month history of severe hypoglycaemia and a 4-week 
history of non-severe and severe hypoglycaemia. In the 
prospective period, they were asked to complete a special 
diary of hypoglycaemia on a daily basis. 
The primary endpoint of the study was the percentage 
of patients experiencing at least one hypoglycaemic 
event during the 4-week follow-up period. The majority 
of statistical analyses were prepared on data from the 
prospective part, in order to avoid a recall bias. 
The study was performed from March to September 2013. 
It was conducted in accordance with the Declaration of 
Helsinki and was also approved by the Slovenian Ethics 
Committee. 
 
2.1 Statistical Analyses
The majority of analyses were descriptive in nature. All 
statistical tests were two-sided. A p-value of less than 
10.1515/sjph-2017-0033 Zdr Varst 2017; 56(4): 244-250
246
0.05 was considered as statistically significant. Univariate 
binomial regression models were used to examine the 
relationship between hypoglycaemia and factors, including 
age, gender, HbA1c at baseline, diabetes duration, 
duration of insulin therapy, type of insulin therapy, 
frequency of blood glucose monitoring, knowledge of 
hypoglycaemia, hypoglycaemia unawareness, fear of 
hypoglycaemia, period, and diabetes type. Differences 
in retrospective versus prospective data reporting were 
assessed using a paired t-test. 
Definitions used: non-severe hypoglycaemia was defined 
as a hypoglycaemic event managed by the patient alone, 
whereas severe hypoglycaemia was defined as any 
hypoglycaemic event that requires external assistance 
for recovery. Nocturnal hypoglycaemia was defined as a 
hypoglycaemic event occurring between midnight and 6 
in the morning. Documented symptomatic hypoglycaemia 
was defined as any event reported by the patient as a 
symptomatic hypoglycaemia, regardless of the glucose 
level. Patients who answered the question ‘Do you have 
symptoms when you have a low blood sugar measurement?’ 
with ‘never’ or ‘occasionally,’ were said to have ‘severely 
impaired’ or ‘impaired’ hypoglycaemia awareness, 
respectively.
3 RESULTS
Ninety-nine % of patients with type 1 diabetes and 89% 
of patients with type 2 diabetes reported that they had 
experienced hypoglycaemia in their life. In addition, 30% 
of patients with type 1 diabetes and 27% of patients with 
type 2 diabetes reported impaired or severely impaired 
hypoglycaemia awareness. 
At least one hypoglycaemic event (with or without 
measured glucose value) was self-reported in 84.1% 
and 56.4% of patients with type 1 and type 2 diabetes, 
respectively, during the prospective period of 4 weeks. 
43.4% and 26.2% of patients with type 1 and type 2 diabetes, 
respectively, experienced a nocturnal hypoglycaemic 
event. In the same time-period severe hypoglycaemia was 
experienced by 15.9% and 7.1% of patients with type 1 
and type 2 diabetes, respectively. 
Estimated annual incidence rate of documented 
symptomatic hypoglycaemic events (with blood glucose 
3.9 mmol/l or less), calculated from patient diaries in the 
prospective follow-up was 48 events (95% CI 43 to 53) and 11 
events (95% CI 9 to 13) per patient-year in type 1 and type 
2 diabetes, respectively. Also, estimated annual incidence 
rate of severe hypoglycaemia was 6 events (95% CI 4 to 8) 
and 1 event (95% CI 1 to 2) per patient-year in type 1 and 
type 2 diabetes, respectively. There were altogether 62 
episodes of severe hypoglycaemia documented in 4 weeks 
period in 29 patients with type 1 and type 2 diabetes. 
Compared to type 2 diabetes, the percentage of patients 
experiencing severe hypoglycaemia was more than double 
in type 1 diabetes. Nocturnal hypoglycaemia was reported 
with an estimated annual rate 12 (95% CI 9 to 15) and 8 
(95% CI 5 to 8) patient-years in type 1 and type 2 diabetes, 
respectively.
When asked about their definition of hypoglycaemia, 
only 40% of type 1 and of type 2 diabetes patients 
define hypoglycaemia depending on both, blood glucose 
measurement and symptoms, whereas 33% of type 1 and 
37% of type 2 diabetes patients define hypoglycaemia only 
depending on the presence of symptoms. The mean blood 
glucose value below, which patients considered a glucose 
value to be a marker of hypoglycaemia, was 3.18 ±0.64 
mmol/l and 3.41±0.83 mmol/l in type 1 diabetes and type 
2 diabetes, respectively.
Differences on hypoglycaemia recall were noted when data 
on hypoglycaemia from the prospective and retrospective 
part of the study were compared, depending on diabetes 
type (Figure 1). Specifically, a large difference in recall 
was noted in the case of mild hypoglycaemia in type 1 
diabetes patients, with significantly less hypoglycaemias 
reported by the patients from the past 4 weeks compared 
to prospective 4 weeks (37 vs.77 cases, p<0.001). There was 
a much smaller, but still statistically significant difference 
seen in type 2 diabetes, and mild hypoglycaemia reporting, 
with lower reporting for the past 4 weeks, compared to 
the prospective reporting (18 vs. 24 cases, p=0.027). Of 
note, in type 2 diabetes, there was also a difference in 
nocturnal hypoglycaemia reporting, but in the opposite 
direction, reporting more nocturnal hypoglycaemia in a 
retrospective time period (12 vs.6 cases, p=0.007).
Figure 1. Hypoglycaemia incidence depending on the 
retrospective or prospective recall by patients.
R-retrospective, P-prospective
10.1515/sjph-2017-0033 Zdr Varst 2017; 56(4): 244-250
247
Figure 2.
Figure 3.
Hypoglycaemia incidence and HbA1c.
Actions resulting from hypoglycaemia in patients with 
Type 1 and Type 2 diabetes. (Statistically significant 
differences are marked with *).
Using a negative binomial model, adjusted for several 
factors, including duration of diabetes, age, hypoglycaemia 
awareness, and type of insulin therapy, we studied possible 
predictors of hypoglycaemia incidence. From all the 
variables studied, only fear of hypoglycaemia predicted 
severe hypoglycaemia incidence. Neither HbA1c, age, 
diabetes duration nor hypoglycaemia awareness were 
predictors of severe hypoglycaemia (Figure 2, Table 2). 
After experiencing hypoglycaemia in the prospective 4 
weeks of the study, patient actions differed substantially 
between Type 1 and Type 2 diabetes, as represented in 
Figure 3. 
Table 2. Predictors of severe hypoglycaemia in a fully adjusted 
negative binomial model.
NC-not calculable. Model adjusted for: age, gender, HbA1c at 
baseline, duration of diabetes, duration of insulin therapy, 
type of Insulin therapy, frequency of blood glucose monitoring, 
knowledge of hypoglycaemia, hypoglycaemia unawareness, 
fear of hypoglycaemia, period, diabetes type.
Age (years)
Female gender
HbA1c (%)
Diabetes duration (years) 
Type of insulin therapy 
   Short-acting (reference)
   Long-acting
   Long and short-acting
   Mixed
   Other
Blood glucose testing (per day)
Hypoglycaemia unawareness
Fear of hypoglycaemia
Diabetes type 2
0.99
0.80
1.01
1.02
 
 -
0.54
0.70
NC
0.36
1.08
1.00
1.20
0.72
0.556
0.585
0.441
0.594
 
 -
0.489
0.550
NC
0.175
0.555
0.996
0.009
0.627
0.96, 1.02 
0.36, 1.78
0.98, 1.04
0.94, 1.11
 
 -
0.10, 3.07
0.21, 2.28
NC
0.08, 1.57
0.84, 1.38
0.44, 2.24
1.05, 1.37
0.20, 2.67
HR P-
VALUE
95% C.I.VARIABLES
4 DISCUSSION
This is the first study that reports hypoglycaemia 
incidence in a large cohort of insulin-treated patients 
with type 1 and type 2 diabetes mellitus in Slovenia. The 
self-reported rates of hypoglycaemia in this study are 
substantially higher than previously observed in other 
studies, especially in randomised controlled trials. 
Hypoglycaemia is considered a major obstacle for optimal 
glycaemic control achievement in insulin-treated patients 
with diabetes. Moreover, a severe hypoglycaemia is 
strongly associated with a series of negative outcomes, 
including the increased risk of a major macrovascular 
event, as well as the increased risk of a cardiovascular or 
non-cardiovascular death (3,10). Therefore, prevention 
of severe hypoglycaemia is of central importance 
in delivering care to insulin-treated patients with 
diabetes. Interestingly, severe hypoglycaemia could 
not be predicted in our patients by any measured 
factor, including gender, diabetes duration, HbA1c, age, 
frequency of blood glucose measurement, or type of 
insulin therapy. The only factor that was significantly 
and independently associated with severe hypoglycaemia 
incidence in the fully adjusted multivariate model was 
greater fear of hypoglycaemia. Although from our model 
we cannot conclude that greater fear of hypoglycaemia 
was the direct consequence of severe hypoglycaemia 
experience in the past, it is the possible explanation, and 
in line with other studies (11, 12). Even more importantly, 
recognising fear of hypoglycaemia as a predictor of future 
severe hypoglycaemia gives us an important message – 
that addressing that fear by a tailored education we could 
potentially avoid severe hypoglycaemia. 
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248
The incidence of non-severe hypoglycaemia is not easily 
assessed in everyday life of insulin-treated patients, which 
is at least partly due to different levels of hypoglycaemia 
awareness. However, data on severe hypoglycaemia 
incidence is much more reliable (13). Nonetheless, in our 
study, severe hypoglycaemia incidence in type 2 diabetes 
was more than 20-times greater than, for example, in 
the ACCORD study (8), and more than 10-times greater 
than in the observational UK Hypoglycaemia study (6). In 
type 1 diabetes, on the other hand, difference in severe 
hypoglycaemia rate was smaller, but still 10-times higher 
in our study compared to the intensive arm of the DCCT 
trial (14), and almost 2-times higher compared to the 
UK Hypoglycaemia study (6). Not surprisingly, our data 
are very near to other real-world patient cohort studies 
(12, 15). Such a pronounced difference in hypoglycaemia 
incidence is likely due to the nature of the studies and 
study methodology. In other words,, results of our study 
reflect data on patients from the everyday practice, 
whereas patients with concomitant diseases, recurrent 
hypoglycaemia, or hypoglycaemia unawareness are 
usually excluded from randomised controlled trials. In 
addition, the incidence of severe hypoglycaemia was self- 
reported in our study, as experienced by the patients, 
and was not confirmed by means of patient medical 
files. Moreover, our patient population, especially with 
type 2 diabetes, was rather older and had, on average, 
diabetes for a substantially longer time period, compared 
to similar studies. The other important fact is also that 
the definitions of hypoglycaemia changed over the last 
years, even in the last few years (13, 16); however, the 
findings of our study go beyond the definitions and reveal 
what patients consider relevant for their everyday life 
with insulin. 
However, comparing results from the Slovenian cohort 
to the recently published results of the study analysing 
hypoglycaemia incidence in more than 27,000 patients 
globally (9), the incidence of severe hypoglycemia in 
Slovenian type 1 diabetes was higher (5.9 vs. 4.9 events-
patient-year) and in type 2 diabetes was lower (1.5 vs. 
2.5 events-patient-year). The incidence of nocturnal 
hypoglycaemia in type 1 diabetes was similar in Slovenia 
and globally, whereas in type 2 diabetes, it was almost 
twice as common as elsewhere (6.4 vs. 3.67 events-
patient-year) (9). Data on nocturnal hypoglycaemia is 
quite of a concern. Firstly, nocturnal hypoglycaemias can 
lead to sleep deprivation, lower quality of life, lower work 
performance, worse driving skills, etc. (17). Secondly, 
nocturnal hypoglycaemias are characterised by the 
lower intensity and recognizability of counterregulatory 
responses, thereby depriving individuals of the adequate 
stimulus to counteract hypoglycaemia. Therefore, 
nocturnal hypoglycaemias can pass by unrecognized and 
lead to lower hypoglycaemia awareness (18). Lastly, 
awakening response after nocturnal hypoglycaemia is 
lower and may affect the patient’s ability to intake 
adequate amount of carbohydrates, especially in elderly 
people with possibly pre-existing cognitive impairment 
(17). 
In type 1 diabetes, comparing prospective hypoglycaemia 
count with a retrospective recall, we detect a large 
discrepancy, especially in mild hypoglycaemia. Because 
it is a frequent event, patients probably consider it 
normal and devote less attention to it. However, the 
way the mild hypoglycaemia is perceived might be 
crucial to prevent hypoglycaemia desensitisation and 
even hypoglycaemia unawareness, often stemming 
from repetitive hypoglycaemia (19). A similar trend 
in mild hypoglycaemia was seen in our type 2 diabetes 
patients. However, in this group, reported past incidence 
of nocturnal hypoglycaemia was higher than in the 
prospective part of the study, possibly indicating that 
experience of nocturnal hypoglycaemia is more stressful 
than day hypoglycaemia, and leads to oversizing its 
appearance. Nocturnal hypoglycaemia, in particular, 
impacts one’s sense of well-being because of its impact on 
sleep quality and quantity (20). Fear of hypoglycaemia, 
especially nocturnal one, may be one of the important 
reasons patients rather choose higher glycaemic targets 
(21). 
From the DCCT trial, the association between lower HbA1c 
and higher hypoglycaemia incidence is well established 
(22). Yet, the results of our study underline that higher 
HbA1c values are not protective from experiencing 
hypoglycaemia, since hypoglycaemia was reported with 
similar frequency with low as well as with high levels 
of glycated haemoglobin. The association is easily 
understood with low levels of glycated haemoglobin, since 
frequent hypoglycaemias lower average glucose levels. 
On the other hand, it may be quite surprising to see that 
hypoglycaemias are no less frequent in patients with high 
glycated haemoglobin values. A possible explanation could 
be that patients experiencing hypoglycaemia deliberately 
lower insulin dose, as also reported in Figure 3 in our 
cohort of patients, or maybe even skip insulin application 
(23). 
In our study, a very high average glycated haemoglobin 
value was reported, even substantially higher from the 
global report of the same study (9). If this value holds 
true, it is very alarming for the diabetes patient care in 
Slovenia, and definitely deserves further assessments. 
However, due to the study design, where data were not 
captured by patient medical files, but rather by a patient 
recall, there is a possibility that patients reported values 
of average plasma glucose concentration rather than 
glycated haemoglobin percentages. Similarly, we explain 
a very high reported percentage of continuous glucose 
monitoring usage in type 2 diabetes with misunderstanding 
of the meaning of the question. Furthermore, in this 
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249
study, we did not collect data on education level, which 
is, together with low socioeconomic status, a very well 
recognised factor associated with higher hypoglycaemia 
risk in patients with diabetes (13, 24, 25). This patient 
population could also comprise a large part of the group of 
non-responders. Unfortunately, we do not have exact data 
on them, since they did not complete any questionnaire. 
We observed that the non-respondent population is of 
two categories. One is a working population, which 
did not decide to participate in the study due to lack 
of time. For this group, we expect it to be of younger 
age and not to have increased the number of overall 
hypoglycaemia incidence. The second group is a group of 
patients who could not be included because of illiteracy 
or other issues resulting in the inability to complete the 
written questionnaire, like vision impairment and the 
lack of language understanding. We expect this group of 
patients to be even more vulnerable to hypoglycaemia 
and, if included, would be expected to further increase 
hypoglycaemia incidence reported in the study. 
Despite some limitations of the design of the present 
study, this study design gives unique insights into the issue 
of hypoglycaemia through patient experience. In this way, 
new strategies can be employed that address this iatrogenic 
diabetes treatment complication more efficiently. Firstly, 
at the patient and the patient organisations level, the 
awareness of hypoglycaemia incidence should be raised, 
and instructions on the ways to decrease their occurrence 
should be given in a number of different formats, including 
visual and auditory message modes. In addition, fear of 
hypoglycaemia as a predictor of severe hypoglycaemia 
should be further addressed in the future studies as well 
as in routine clinical practice. Diabetes educators and 
medical doctors should become even more sensitised to 
the issue of high hypoglycaemia incidence, accurately 
assess it at every patient visit, and learn about the ways 
patients engage with them. Moreover, development of new 
treatment modules that include cognitive restructuring 
for addressing fear of hypoglycaemia should be welcomed. 
Furthermore, research with innovative methodological 
approach (26) and deep understanding of possibly 
preventable socioeconomic inequalities (27) could lead 
to a creation of patient-tailored, most probably region-
specific approaches to deliver the maximally efficient 
education on hypoglycaemia for its prevention. 
5 CONCLUSIONS
In conclusion, our study is the first comprehensive report 
on patient-reported hypoglycaemia incidence in Slovenian 
insulin-treated type 1 and type 2 diabetes patients that 
highlights several important aspects. Firstly, the incidence 
of hypoglycaemia, especially severe ones, is substantially 
higher than the ones reported from randomised controlled 
trials. Secondly, higher glycated haemoglobin values do not 
exclude high hypoglycaemia event rate. Thirdly, nocturnal 
hypoglycaemia needs special consideration in everyday 
management of insulin-treated patients, especially type 
2. Fourthly, since factors associated with hypoglycaemia 
remained largely unidentified, especially in the context 
of the socioeconomic status, such as education level, 
addressing hypoglycaemia efficiently in the future calls 
for a much broader mixed research method approach, 
including qualitative research. 
ACKNOWLEDGEMENTS
Acknowledgements to investigators, who participated in 
the study: Anja Babič, Kristina Cerk Porenta, Miro Čokolič, 
Kristina Groti Resman, Lidija Kaučevič Pohar, Renata 
Verboten Kopriva, Lučka Leskovšek, Mitja Krajnc, Stojan 
Kralj, Jana Kreč Šorli, Marjan Kristanc, Urša Kšela, Iris 
Marolt, Metka Mesec Staut, Maja Navodnik Preložnik, Ana 
Ogrič Lapajne, Tatjana Martinjak Perčič, Milivoj Piletič, 
Jana Plavc, Marta Simonič, Gorazd Staut, Borut Stravnik, 
Nika Šatej, Lucas Gaudencio Triep, Zorancho Trpkovski, 
Katarina Vukelič, Matej Završnik, Vanda Zorko Kostevc, 
Barbara Zupančič.
CONFLICTS OF INTEREST
The authors declare that no conflicts of interest exist.
FUNDING
The study was financed by NovoNordisk.
ETHICAL APPROVAL
The study was approved by the Slovenian Ethics 
Committee, reference number 116/02/13.
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