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ABOUT RISK-FACTORS OF DEVELOPMENT OF SURGICALLY SIGNIFICANT DELAYED TRAUMATIC INTRACRANIAL HEMATOMAS AFTER ASSOCIATED INJURY
Semenov A.V., Krylov V.V., Sorokovikov V.A.
Irkutsk State Medical Academy of Postgraduate
Education – Branch of Russian Medical Academy of Continuous Professional
Education,
Irkutsk City Clinical Hospital No.3, Irkutsk, Russia
Irkutsk Scientific Center of Surgery and Traumatology,
Irkutsk, Russia
Evdokimov Moscow
State University of Medicine and Dentistry, Moscow, Russia
The first documental description of delayed traumatic intracranial bleedings (DTICB) was made by Otto Böllinger, a German pathologist of Munich University, in 1893. He analyzed four cases of deaths after traumatic brain injury (TBI) [1]. José Álvarez-Sabín and coauthors performed more detailed studies of this problem in the era of computer tomography (CT) and found some features of DTICB: 1) DTICB in adult patients with normal brain CT (without bleeding, fractures and vascular abnormalities) within 6 hours after injury are rare (4.6 % of all TBIs); 2) severity of primary TBI does not influence on their development; 3) DTICB dominate in young patients; 4) period without clinical symptoms is 1-15 days after injury; 5) most DTICBs are deep intracerebral bleedings by the type of parenchymous saturation of small or middle size; 6) the clinical course of DTICB is favorable without surgical management; the mortality is null, without recidivation [2]. The causes of development of such type of DTICB are unclear. Possibly, it is a secondary cerebral injury at the background of a local disorder after TBI [3]. This theory lies in the basis of more frequent increase in the volume of primary foci of cerebral contusion with common formation of surgically significant mainly intracerebral, hematomas (Fig. 1).
Figure 1. The brain CT-scans of the patient P. Delayed
intracerebral hemorrhage: a) CT immediately after hospitalization; b) CT 8 days
later at background of conservative treatment
One
may state that delayed bleedings are more severe in primary cerebral injury
with intracranial bleeding in the first hours after the injury.
Another variant of late intracranial bleeding after
TBI is delayed traumatic intracranial hematomas (DTICH), including meningeal
ones, which sometimes require for surgical treatment. The nature of their
development is thrombus detachment or erosion of primarily injured vessel in
TBI, especially at the background of dehydratation [4]. Actually, a secondary
cerebral injury happens by means of delayed formation of hematoma, compression
and dislocation of the brain. Therefore, we deal with the multifactorial (at
the morphological level) disease, but with the single pathogenetic mechanism (Fig.
2).
Figure 2. Importance of the secondary brain injury for both
delayed hemorrhage (parenchymal saturation) and delayed hematoma
Practically,
DTICH is better to consider as one of the variants of DTICB. Considering the
relatively rare development in patients with TBI, there is an important issue
on influence of external factors such as premorbid anticoagulant therapy and DIC
in traumatic hemorrhagic shock. A study by C.E. Albers et al. included 3,088 patients with mild TBI. They did not find any influence of premorbid intake of
anticoagulants on intracranial bleedings, considering the gender and age of
injured persons [5]. Such results were received in studies by D.K. Nishijima at
el. [6]
and
V.G. Menditto et al. [7]. They found that warfarin and clopidogrel did not
influence on development of DTICB before TBI.
The
changes in hemostasis in traumatic and hemorrhagic shock have been well studied
and present a wave-shaped cascade of responses of clotting and anticlotting
systems of the body with alternate dominance [8]. Acute thrombocytopenia at
early stages of DIC and its possible influence on DTICB and DTICH in severe TBI
are interesting (Fig. 3).
Figure 3. The simplified design of the hemostasis changes
as a result of DIC-syndrome in severe associated injury [8]
Objective – to identify possible risk factors of development of surgically significant DTICH in associated injury.
MATERIALS AND METHODS
A
retrospective comparative analysis of diagnostics and treatment of 30 patients
with associated and isolated traumatic brain injury was conducted on the basis
of Irkutsk City Clinical Hospital No.3 in 2012-2017. The study corresponded to
the ethical standards of Helsinki Declare – Ethical Principles for Medical
Research with Human Subjects, and to the Order of Health Ministry of RF No.266,
19 June 2003. Due to the fact that the study was retrospective and did not
require for publication of personal data, the written consent was not required.
The
inclusion criteria were: 1) correspondence of diagnosis to the Russian
classification of injuries [9]; 2) reliable information on presence of
traumatic brain injury; 3) absence of surgically significant intracranial
hematoma in MSCT in the first 6 hours after the injury; 4) absence of
concurrent abnormality of cerebral vessels; 5) for the group of patients with
DTICH – presence of a surgically significant intracranial hematoma during
recurrent MSCT at least 6 hours after the first examination. The exclusion
criteria: 1) childhood; 2) presence of a surgically significant intracranial
hematoma at admission.
Three
groups of patients were retrospectively collected: the group A – 8 deceased
patients with associated TBI with surgically significant DTICH and
correspondence to the selected criteria (meningeal – 7, intracerebral – 1); the
group B – 12 patients with associated TBI without DTICH (8 survivals, 4
deceased); the group C – 10 patients with single TBI with DTICH requiring for
surgical treatment. The results of main clinical and laboratory studies were
examined in all three groups according to our list (coagulograms were collected
for the whole period of hospital stay; totally 1,019 examinations). MSCT was
used for measurement of optic nerve sheath diameter (ONSD) with our technique –
the indirect sign for measurement of intracranial pressure [10] (Fig. 4).
Figure 4. The brain CT-scans of the patient S. Estimation
of optic nerve diameter (OND) on an initial brain CT-scan: a) mild brain injury, OND = 3.9 mm to the
right; b) severe brain injury, OND = 6.8 mm to the right – the sign of high
intracranial pressure
All
received digital data was converted into the simple mean arithmetic (M) with
the formula: М
= Ʃν/n, where v - numeric value of a studied sign, Ʃν – the sum, n – number of observations. Then the mean
quadratic deviation (σ) was calculated for each mean value using the
formula: σ
= Vmax – Vmin / k, where Vmax – the value of
the highest variant (a digital value) of a studied sign, Vmin – the
value of the minimal variant, k – the coefficient from the table calculated by
S.I. Ermolaev [11]. The mean quadratic deviation was used for calculation of
the error in the mean (m) with the formula:
m
= or m =
, if n ≤ 30.
The error in the mean value of the signwas used for calculation of reliability of differences of the studied signs
(Student’s test) in the comparison groups with the formula:
t = (the table
1).
Table 1. Mean values of main clinical and laboratory signs (declinations from normal values are black typed
|
Number of sign at admission; normal values and(or) measurement units are in brackets |
Group A |
Group B |
Group C |
||||||
|
М1 |
σ2 ± |
m3 ± |
М |
Σ ± |
m ± |
М |
σ ± |
m ± |
|
|
1. Age (years) |
66.5 |
13.7 |
5.17 |
53.8 |
21.17 |
6.38 |
63.7 |
17.5 |
5.84 |
|
2. GCS (normal – 15) |
10.87 |
2.5 |
0.93 |
13.4 |
2.454 |
0.739 |
11.8 |
2.59 |
0.86 |
|
3. SAP (100-130 mm Hg) |
87.75 |
24.5 |
9.28 |
99.25 |
30.67 |
9.248 |
133.7 |
29.62 |
10.47 |
|
4. DAP (60-80 mm Hg) |
51.9 |
21.05 |
7.96 |
56.3 |
27.6 |
8.324 |
80.5 |
15.15 |
5.357 |
|
5. Pulse (60-80 per min) |
100.6 |
18.9 |
7.14 |
97.8 |
19.02 |
5.73 |
82.9 |
15.15 |
5.36 |
|
6. ATBII (normal - +6.0)4 |
2.31 |
2.1 |
0.79 |
4.17 |
2.15 |
0.64 |
- |
- |
- |
|
7. ISS (points) |
34.75 |
14.4 |
5.44 |
33.8 |
12.58 |
3.79 |
- |
- |
- |
|
8. Time before first MSCT (hours) |
3.75 |
2.21 |
0.9 |
9.4 |
25.0 |
8.33 |
51.25 |
77.76 |
25.9 |
|
9. Mean OND (normal – 5.1±0.7 mm)5 |
5.03 |
0.24 |
0.167 |
5.63 |
0.454 |
0.203 |
5.37 |
0.83 |
0.37 |
|
10. Alcohol in blood at admission (normal – 0-0.35‰) |
0.66 |
0.49 |
0.18 |
0.49 |
0.89 |
0.27 |
0.9 |
1.03 |
0.51 |
|
11. INR (normal – -0.7-1.3)6 |
1.51 |
0.9 |
0.28 |
1.25 |
0.54 |
0.08 |
1.135 |
0.15 |
0.02 |
|
12. APTT (normal – 24-35 sec.) |
33.6 |
8.8 |
2.78 |
31.1 |
11.16 |
1.88 |
29.33 |
8.01 |
1.37 |
|
13. SFC (normal – 4 mg, %)6 |
11.73 |
6.94 |
2.194 |
16.19 |
5.936 |
0.905 |
20.11 |
5.697 |
0.912 |
|
14. PTT (normal – 12-20 sec.)6 |
21.12 |
8.771 |
3.315 |
16.8 |
6.326 |
1.136 |
16.92 |
1.5 |
0.294 |
|
15. PTI (normal – 95-105 %) |
81.5 |
9.734 |
9.734 |
80.05 |
18.41 |
4.46 |
93.83 |
13.19 |
3.976 |
|
16. Fibrinogen (normal – 2-4 g/l)6 |
4.196 |
2.668 |
0.805 |
4.371 |
1.256 |
0.191 |
5.231 |
0.774 |
0.127 |
|
17. Platelets (normal – 180-320 × 109/l) |
134.5 |
70.91 |
12.34 |
190.9 |
130.8 |
14.19 |
187.5 |
64.21 |
7.674 |
|
18. Hemoglobin (normal – 120-160 × 10 g/l)6 |
85.28 |
33.82 |
5.978 |
99.48 |
21.06 |
2.298 |
107.4 |
19.46 |
2.217 |
|
19. Red blood cells (normal – 3.9-6.0 × 109/l)6 |
2.562 |
0.889 |
0.165 |
3.279 |
0.683 |
0.078 |
3.543 |
0.602 |
0.069 |
|
20. Fat globulemia (normal – 0 points)7 |
3.0 |
0.858 |
0.429 |
3.0 |
0.92 |
0.277 |
- |
- |
- |
|
21. Concurrent pathology (%)8 |
75.0 |
|
16.37 |
83.3 |
|
11.24 |
60.0 |
|
16.3 |
|
22. Gender (male/female) |
4/4 |
9/3 |
7/3 |
||||||
Note: 1 – simple mean arithmetic; 2 – standard deviation; 3 – error of mean; 4 – associated traumatic brain injury index (ATBII) [12]; 5 – optical nerve diameter (OND); 6 – values of coagulogram and total blood analysis are for the whole period of hospital stay (totally, 1,019 examinations in 3 groups); 7 – mean degree of fat globulemia for the whole period of hospital stay according to N.V. Kornilov et al., 2000 [13]; 8 – relative value – % of patients in the group with associated pathology (HD, DM, IHD etc.) with calculation of alternative value and mean error of relative value.
RESULTS AND DISCUSSION
The comparison groups A, B and C were homogenous according to most signs: age, time of conduction of initial MSCT of the brain after trauma, concurrent pathology, alcohol in the blood, pulse and main indices of the coagulogram – INR, PTT, PTI, fibrinogen. The groups A and B did not show any significant differences in the index of associated TBI and ISS; all they had fat globulemia (the table 2).
Table 2. Student’s test for significance of differences in mean values (t > 2 – reliable difference (black typed))
|
Number and name of sign |
Student’s test for significance of differences |
|
|
А and B |
А and C |
|
|
1. Age |
1.54 |
0.35 |
|
2. GCS |
2.142 |
0.7 |
|
3. SAP |
0.877 |
3.28 |
|
4. DAP |
0.387 |
2.989 |
|
5. Pulse |
0.31 |
1.98 |
|
6. IATBI |
1.829 |
- |
|
7. ISS |
0.143 |
- |
|
8. Time before initial MSCT |
0.674 |
1.83 |
|
9. OND |
2.282 |
0.837 |
|
10. Blood alcohol |
0.52 |
0.44 |
|
11. INR |
0.91 |
1.33 |
|
12. APTT |
0.73 |
1.387 |
|
13. SFC |
1.878 |
3.53 |
|
14. PTT |
1.22 |
1.263 |
|
15. PTI |
0.135 |
1.173 |
|
16. Fibrinogen |
0.212 |
1.27 |
|
17. Platelets |
2.998 |
3.646 |
|
18. Hemoglobin |
2.216 |
3.467 |
|
19. Erythrocytes |
3.93 |
5.485 |
|
20. Fat globulemia |
0 |
- |
|
21. Concurrent pathology |
0.417 |
0.64 |
|
22. Gender (male/female) |
4/4 |
9/3 |
The table 3 shows all identified statistically significant differences in the signs with use of the symbols “>” (more), “<” (less) and “=” (equal – for cases with unreliable differences in the signs).
Table 3. Quantitative estimation of differences in signs according to principle «more/less/equal» (explained in the text)
|
GCS, points |
ATBI without DTICH |
> |
ATBI with DTICH |
= |
ITBI with DTICH |
|
OND (mm) |
ATBI without DTICH |
> |
ATBI with DTICH |
= |
ITBI with DTICH |
|
Blood platelets (×109/l) |
ATBI without DTICH |
> |
ATBI with DTICH |
< |
ITBI with DTICH |
|
Red blood cells (×1012/l) |
ATBI without DTICH |
> |
ATBI with DTICH |
< |
ITBI with DTICH |
|
Hemoglobin (g/l) |
ATBI without DTICH |
> |
ATBI with DTICH |
< |
ITBI with DTICH |
|
Plasma SFC (mg/100 ml) |
ATBI without DTICH |
= |
ATBI with DTICH |
< |
ITBI with DTICH |
|
Arterial pressure (mm Hg) |
ATBI without DTICH |
= |
ATBI with DTICH |
< |
ITBI with DTICH |
Note: ATBI – associated traumatic brain injury; ITBI – isolated TBI; DTICH – delayed traumatic intracranial hematoma; OND – optical nerve diameter during initial brain MSCT.
The
presented table shows that two factors are especially interesting with
differences in the groups: consciousness level and ONSD. The consciousness
level according to GCS in associated TBI without DTICH was reliably higher
(> 13 points) than in associated and isolated TBI with DTICH. This fact can
testify more severe primary injury to the brain in TBI with formation of
surgically significant DTICH in associated and isolated injuries.
ONSD
(mm) in associated TBI without DTICH was reliably higher (> 5.5 mm) than in
isolated and associated injuries without DTICH. According to the modern
literature, ONSD is the most available and quite accurate marker of ICP change
[10]. Small ONSD (< 5.05 mm) can testify the absence of intracranial
hypertension in primary MSCT and possibly the presence of intracranial
hypotension. Formation of extensive intracerebral bleedings is not rare after
removal of traumatic meningeal hematomas; it can be related to harp decrease in
ICP during surgery. The issue requires for further investigation with higher
number of cases.
Thrombocytopenia (< 180 × 109/l) was found in patients with
associated TBI and DTICH, whereas the mean value of platelets was within the
normal limits in associated TBI without DTICH. The patients with isolated TBI
had no thrombocytopenia, but had DTICH. Also arterial pressure, red blood cells
and hemoglobin in the blood were reliably lower in patients with associated TBI
with DTICH in comparison with associated TBI without DTICH, but also reliably
lower than in patients with isolated TBI with DTICH. Therefore, the influence
of thrombocytopenia, anemia and arterial hypotension on DTICH in associated
injury was doubtful.
SFC
were above the normal value in all three groups, but without significant
differences in associated TBI with DTICH and without it. There is an
interesting fact of higher SFC (the sign of developing DIC) in isolated TBI
with DTICH. It confirms the possibility of initiation of DIC in isolated TBI,
possibly due to release of high level of tissue thromboplastin in neuronal
tissue [8].
CONCLUSION
The study showed that the
associated injury and traumatic (hemorrhagic) shock do not make a high
influence on development of surgically significant DTICH. Patients with
associated and isolated TBI have the higher risk of surgically significant
DTICH if they demonstrate the following signs at admission: 1) GCS < 12; 2)
ONSD < 5.1 m according to results of MSCT (the indirect sign of low
ICP).
The
future studies of the influence of normal or low intracranial pressure on
development of delayed bleedings with consideration of possible changes in
hemostasis, which are common for DIC in both associated and isolated TBI.
Information on financing and conflict of interests
The study was conducted without sponsorship. The authors declare the absence of any clear or potential conflicts of interests relating to publication of this article.
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