Abstract
Introduction: Ischemic stroke is the third leading cause of death worldwide. The purpose of the current study was to assess the preliminary effects of Coffea arabica (CA) in experimentally-induced stroke in an animal model in the context of neuroprotection. The study was also designed to document the prophylactic use of CA in patients experiencing stroke symptoms.
Methods: A total of 25 male albino rats, 12 months of age, were purchased from the local market. They were acclimatized for seven days and divided into 5 groups. Each group consists of 5 subjects. Each subject was trained on a specific test for behavioral assessment. Behavioral modulation of each rat was performed using four tests, namely cylinder test, staircase test, forelimb flexion test, and pasta test. All the tests were performed as per standard criteria at the 4th, 8th, 12th, and 14th day of drug administration. The subjects were administered with caffeine (2.4 mg/kg) and CA (100 mg/kg and 200 mg/kg extract) doses for 14 days to assess the prophylactic use of CA. After 14 days of treatment, rats were subject to ischemic stroke induction using the middle cerebral artery ligation method. All four tests used for behavior modulation were applied at 24, 48, and 72 hours intervals of postsurgery. The subjects were further sacrificed for histopathological investigations. Statistical analysis was performed with SPSS (V. 22) software using one-way ANOVA.
Results: Our findings suggest that treatment with CA, 100 mg/kg and 200 mg/kg orally, decreases the infarct volume. However, there are not many considerable differences that were found in both doses. Histopathological investigations revealed characteristic structural changes occurring in both gray and white brain regions, depending on the severity, location, and duration of the ischemic stroke.
Conclusion: CA is a harmless and active mediator in the dissolution of blood clots and the recovery of stroke in rats. It is an agent that has been found to be efficient for brain activity with few side effects and behavioral modifications.
Introduction
Stroke is generally well-defined as an abnormality of blood supply to a principal area of the brain. This primary abnormality might be a diminution of nutrients (commonly ischemia) or hemorrhage; the abnormality may vary in time interval and extent, producing an enormous number of temporary or permanent neurological defects1. Acute ischemic stroke is the third primary cause of death in developed countries and Europe2. It is one of the most recurring causes of disability around the globe3. Irrespective of pathophysiological understanding of cerebral ischemia and its advances in modern science, there are minimal numbers of pharmacotherapy protocols3. Only Recombinant Tissue-Plasminogen Activator (rt-PA) for thrombolysis has been approved for practice in the management of this disease4. Various Chinese5 and herbal medicines, including alternative therapies6, have been used in the treatment of ischemic stroke for a long time; one of these significant medicinal plants is Coffea arabica (CA).
CA is a species of Coffea, and is rich in phytochemical constituents like caffeine, trigonelline, chlorogenic acids, and sucrose7. Several studies have reported its anti-inflammatory effects8 and anti-fungal properties9.
The purpose of the current study was to assess the preliminary effects of CA in experimentally-induced stroke in an animal model in the context of neuroprotection. The study was also designed to document the prophylactic use of CA in patients experiencing stroke symptoms.
Materials - Methods
Animals
A total of 25 male albino rats (12 months of age) were purchased. All subjects were weighed for dose and food administration. The weight variation ranged from 290 to 300 g. The subjects were kept in standard confinement (length = 450 mm × width = 340 mm × height = 210 mm) for animal housing; animals were kept in a controlled environment at standard conditions of temperature (22 ± 1 ºC) and humidity (40 to 60%). Animals were exposed to twelve hours of light and dark cycles.
Preparation of Coffea arabica (CA) extract
Aqueous extract of CA was prepared through mechanical pressing and solvent extraction methods using soxhlet apparatus and rotary vacuum evaporator.
Method of ischemic stroke induction
Rats were anesthetized with Ketamine. Blood pressure and oxygen supply were monitored. Ischemic stroke was induced using the ligation technique (Figure 1) of the Middle Cerebral Artery Occlusion (MCAO) method10.
Treatment protocol
Rats were acclimatized for 7 days, and the bodyweight of each subject was recorded. They were divided into 5 groups (n = 5 per group). Each rat was trained on a specific test for behavioral assessment. Behavioral modulation (Figure 2) of each rat was performed using four tests, namely cylinder test11, staircase test12, forelimb flexion test, and pasta test13. All the tests were performed as per standard criteria at the 4th, 8th, 12th, and 14th day of drug administration.
The subjects were administered with caffeine and CA doses (Table 1) for 14 days to assess the prophylactic use of CA. We used two different doses to assess its efficacy. In our pilot study, 300 mg and 500 mg/kg doses of CA were found to be fatal and possessed adverse effects. Therefore, we used these two doses, 100 mg/kg and 200 mg/kg, in our current study. All the subjects received an oral dose once a day.
Groups | Dose | Days | |||||||||||||
1 | 2 | 3 | 4 | 5 | 6 | 7 | 8 | 9 | 10 | 11 | 12 | 13 | 14 | ||
Control | Normal saline | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ |
Sham | Nil | - | - | - | - | - | - | - | - | - | - | - | - | - | - |
Caffeine | 2.4 mg/kg | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ |
CA 100 mg/kg | 100 mg/kg | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ |
CA 200 mg/kg | 200 mg/kg | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ | √ |
Methods for evaluation
Time latency (seconds) was observed in forelimb flexion and staircase tests. The use of impaired forelimbs in cylindrical test and the number of falls in pasta test were observed. The latency was observed for time and limb movement. Histopathology examination was performed by slicing of the brain, and this was further confirmed by brain staining with 2,3,5-Triphenyl Tetrazolium Chloride (TTC) reagent.
Statistical analysis
Statistical analysis was performed using the Statistical Package for Social Sciences software (version 22.0). One-way analysis of variance (ANOVA) was applied using a Tukey range post-hoc test. The level of significance was considered as p < 0.05.
Ethical Statement
The current study was approved by the Committee on Animal Ethics, Hajvery University, Lahore, Pakistan, under the ethical approval letter no. HU-EC-07-2017.
RESULTS
The current study was aimed to assess the neuroprotective action of CA in a rat model of ischemic stroke. Animals were acclimatized for one week, and behavioral modelling was performed. This behavioral modelling was conducted to evaluate a measure of performance at a latency period of 4th, 8th, 12th, and 14th day during Caffeine and CA administration (Figure 3). All the subjects in the study groups showed normal behavior and accomplished specific tasks. However, few subjects in both control and sham groups responded spontaneously while performing forelimb flexion and staircase test. This impulsive behavior may owe a change in their physiological function. It was also observed that rats receiving CA became slightly aggressive; this observation warrants further evaluation in future research studies.
The mean latency time in cylinder test of control, sham, caffeine, CA 100 mg/kg, and CA 200 mg/kg groups were noted as 6.6, 5.4, 7.1, 5.2, and 6.8 seconds, respectively. The mean latency time of forelimb flexion group was observed as 12.8, 13.1, 12.5, 11.6, and 12.2 seconds for the control, sham, caffeine, CA 100 mg/kg, and CA 200 mg/kg groups, respectively. Observations (mean) of the staircase test were recorded as 9.4, 10.4, 8.4, 9.1, and 9.8 seconds for the respective groups. The results (movement) monitored in the pasta test were documented as 4.1, 3.9, 4.0, 3.6, and 4.4 seconds, respectively. Consequently, we found no statistically significant difference (p = 0.271) in the rats' behavior among the groups (Figure 3). All subjects were found to be under the appropriate conditions for surgical procedures.
Ischemic stroke was induced through the MCAO method. All mentioned tests were applied after induction of stroke at intervals of 24, 48, and 72 hours.
Cylinder test
Subjects were assisted to perform cylinder test. There was a significant statistical difference found between the control and sham group (p = 0.001), and the very least statistical significance was observed between CA 100 mg/kg and CA 200 mg/kg groups (p = 0.645). Statistical results were not encouraging in comparison of the control and CA 100 mg/kg group (p = 0.295). However, these insignificant statistical results show a significant effect of the CA 100 mg/kg dose. Moreover, a higher dose of 200 mg/kg minimally exhibits the reversal phenomenon of the ischemic stroke (Figure 4).
Forelimb flexion test
Our study subjects were also assessed for forelimb extension. Statistically significant differences were found among CA 100 mg/kg (5.933 + 0.733), control (12.800 + 0.000), and sham (0.600 + 0.115) groups after 24, 48, and 72 hours intervals (p = 0.000), respectively (Figure 5). However, CA 100 mg/kg dose (5.933 + 0.733) and CA 200 mg/kg dose (4.666 + 0. 635) groups were comparatively insignificant in their differences (p = 0.442). Moreover, CA powder at the 100 mg/kg dose was more effective at inducing or alleviating stroke at all levels of treatment intervals. On the other hand, CA 200 mg/kg dose (4.666 + 0. 635) showed less improvement of stroke recovery.
Staircase test
Rats were subject to the staircase test. The results were statistically significant among all groups (p = 0.000). However, CA 100 mg/kg group was significantly different from sham (p = 0.000) and caffeine (p = 0.030) groups. On contrary, it was less different from the control (p = 0.143) and CA 200 mg/kg dose (p = 0.174) groups. These observations showed that the effect of CA 100 mg /kg dose was almost similar to the control group. It also revealed that both doses show almost equivalent response (Figure 6).
Pasta test
The pasta test was performed on subjects receiving established treatment. Statistical analysis showed significantly different results between control (4.200 + 0.577) and sham (18.133 + 0.982) groups (p = 0.000). We documented similar observations between sham (p = 0.000) and CA 100 mg/kg dose (p = 0.000) group. The results revealed that CA 100 mg/kg dose is more protective to MCAO-induced stroke, than compared to caffeine and CA 200 mg/kg (Figure 7).
Histopathological studies
The histopathological significances of ischemic stroke are multifaceted. Their outcomes may lead to several deficits, including severe motor and cognitive disturbances. The histopathological consequences in our study show typical structural changes in both gray and white matter. However, the location, duration, and severity of ischemic stroke need to be considered (Figure 8). Our findings of severe focal ischemia are well-described with characteristic structural changes occurring in both gray and white brain regions, depending on the severity, location, and duration of the ischemic stroke. The white region in our stained brain slice image of the sham group depicted reduced blood flow to the brain, resulting in ischemia. Furthermore, this area was very reduced and compact in the CA 100 mg/kg dose group, which depicted functional recovery against ischemic stroke.
DISCUSSION
The present study aimed to assess the preliminary effects of CA in neuroprotection of experimentally-induced stroke in rats. Animals were administered with doses of 100 and 200 mg/kg of CA. The doses of CA were selected based on dose-ranging studies; these are the clinical trials to determine the most appropriate doses that are not exceeding the maximum dose limit or the toxic levels14. After the administration of the recommended protocol of 14 days, animals were subjected to induction of ischemic stroke15. The subjects were passed through a series of testing procedures for assessing their neurological activity after exposure to surgery. These testing procedures included cylinder test, forelimb flexion test, staircase test, and pasta test.
The cylinder test was used to assess the locomotor function in rodents with central nervous system disorders. It was also used to detect mild neurological defects in subjects under study. It was observed during the evaluation that the CA 100 mg/kg dose showed maximum response against ischemic stroke among all-time intervals (Figure 4). Several studies indicate that coffee is a rich source of flavonoids like catechins and their neuroprotective potential is primarily associated with protection against neurotoxin-induced injuries and suppression of neuro-inflammatory mechanisms, plus the promotion of cognitive functions, learning, and memory16, 17. The main ingredient in CA neuroprotection is caffeine 18, 19, 20, 21.
A forelimb flexion test was performed to detect the neurological impairments in rodents. Our results indicated that both 100 mg and 200 mg/kg doses showed significant protective response (Figure 5). However, CA 100 mg/kg dose was found more effective than 200 mg/kg after 24, 48, and 72 hours of post-surgery. A similar study was conducted by Novitzky et al. in 2016 to examine the comparison of the neuroprotective effect of Bevacizumab and Sildenafil after stroke induction in rodents. The study revealed a minor effect of neuroprotection with Bevacizumab, while Sildenafil showed no response22. Conversely, our investigations recognized the healthier connection between paw grasping and brain functions in the rat in association with previous studies.
The staircase test was designed for the exploration of the independent use of forelimbs in rats12. Side-specific deficiencies in coordinated paw reaching in rats were efficiently measured by this test. Our findings exposed that the pharmacological effects of the CA 100 mg/kg treated group are almost similar to that of the control group (Figure 6). Freret et al. in 2006 used this test to evaluate the above-defined limitations. Our similar findings with that of Freret et al. suggest that CA 100 mg/kg dose induced more sensitive repair efforts, in contrast to the evaluation of contralateral limb use in rats23. This finding was also observed by Grabowski et al. with the staircase test, in corroboration with our study24.
After experiencing any kind of damage in the central nervous system, manual dexterity is often impaired. Therefore, it is crucial to develop a primary measurement method of forepaw dexterity quantitatively. The pasta test also corroborates with our findings of previous tests. The CA 100 mg/kg dose was more responsive than caffeine and CA 200 mg/kg dose (Figure 7). However, the recovery mechanisms might be different according to specific regions of brain damage25. For a better understanding of the rehabilitation mechanisms in specific regions of brain damage in rat stroke models, valuable research should continue to examine behavioral tests and functional recovery of stroke so that they discoveries might be translated to human patients of stroke23.
The histopathological studies in our study showed typical structural changes in the brain (Figure 8). Our findings of severe focal ischemia are well-described with characteristic structural changes occurring in both gray and white brain regions, depending on the severity, location, and duration of the ischemic stroke. The white region in our stained brain slice image of the sham group depicts the diminished blood flow to the brain that results in ischemia. Furthermore, this area is very reduced and compact in the CA 100 mg/kg treated group, demonstrating functional recovery against ischemic stroke. For the evaluation of enhanced plasticity of brain tissue after stroke occurrence, a long-term functional recovery is essential. Neural tissues are complex, and caution should be used in attempting to identify neuroprotective drugs.
It was a preliminary study considering only twenty-five subjects on rats. There were two large doses of 100 mg, and 200 mg/kg were used. Future studies should be carried out on more animal subjects with more refined doses. CA should also be studied in human subjects for its potential medicinal properties.
Conclusion
Our findings conclude that CA is a harmless and active mediator in the dissolution of blood clots and recovery of stroke in rats. It is an agent that is effective at inducing brain activity with few side effects and modifications in behavior. This is because coffee contains many biologically active substances and antioxidants, like polyphenols, that can potentially protect brain cells from death and can help in recovery from stroke. Thus, there is a great need for the evaluation, assessment, and appraisal of its therapeutic characteristics in humans soon.
Abbreviations
CA: Coffea arabica
MCAO: Middle cerebral artery occlusion
TTC: 2,3,5-Triphenyl tetrazolium chloride
ANOVA: Analysis of variance
Acknowledgments
I am greatly indebted to my loving parents for their valuable and most precious prayers.
Author’s contributions
All authors made substantial contributions to conception and design, acquisition of data, or analysis and interpretation of data; took part in drafting the article or revising it critically for important intellectual content; gave final approval of the version to be published; and agree to be accountable for all aspects of the work.
Funding
Not applicable.
Availability of data and materials
Data and materials used and/or analysed during the current study are available from the corresponding author on reasonable request.
Ethics approval and consent to participate
Not applicable.
Consent for publication
Not applicable.
Competing interests
The authors declare that they have no competing interests.
References
-
Millikan
C.,
Animal stroke models. Stroke.
1992;
23
(6)
:
795-797
.
View Article PubMed Google Scholar -
Lo
E.H.,
Dalkara
T.,
Moskowitz
M.A.,
Mechanisms, challenges, and opportunities in stroke. Nature reviews neuroscience.
2003;
4
(5)
:
399-414
.
View Article PubMed Google Scholar -
Strong
K.,
Mathers
C.,
Bonita
R.,
Preventing stroke: saving lives around the world. The Lancet Neurology.
2007;
6
(2)
:
182-187
.
View Article Google Scholar -
Furlan
A.J.,
Katzan
I.L.,
Caplan
L.R.,
Thrombolytic therapy in acute ischemic stroke. Current treatment options in cardiovascular medicine.
2003;
5
(3)
:
171-180
.
View Article PubMed Google Scholar -
Yu
M.,
Sun
Z.J.,
Li
L.T.,
Ge
H.Y.,
Song
C.Q.,
Wang
A.J.,
The beneficial effects of the herbal medicine Di-huang-yin-zi (DHYZ) on patients with ischemic stroke: a randomized, placebo-controlled clinical study. Complementary therapies in medicine.
2015;
23
(4)
:
591-597
.
View Article PubMed Google Scholar -
Pandian
J.D.,
Liu
M.,
Misbach
J.,
Venketasubramanian
N.,
Alternative therapies for stroke treatment in Asia. International Journal of Stroke.
2011;
6
(6)
:
541-543
.
View Article PubMed Google Scholar -
Ky
C.L.,
Louarn
J.,
Dussert
S.,
Guyot
B.,
Hamon
S.,
Noirot
M.,
Caffeine, trigonelline, chlorogenic acids, and sucrose diversity in wild Coffea arabica L. and C. canephora P. accessions. Food chemistry.
2001;
75
(2)
:
223-230
.
View Article Google Scholar -
Castro
M.M.E.,
Pereira
R.G.F.A.,
Dias
D.F.,
Gontijo
V.S.,
Vilela
F.C.,
Moraes
G.O.I.,
Anti-inflammatory effect of aqueous extracts of roasted and green Coffea arabica L. Journal of functional foods.
2013;
5
(1)
:
466-474
.
View Article Google Scholar -
Rizvi
S.,
Jaiswal
V.,
Mukerji
D.,
Mathur
S.,
Antifungal properties of 1, 3, 7-trimethylxanthine, isolated from Coffea arabica. Naturwissenschaften.
1980;
67
(9)
:
459-460
.
View Article PubMed Google Scholar -
Tamura
A.,
Graham
D.,
McCulloch
J.,
Teasdale
G.,
Focal cerebral ischaemia in the rat: 1. Description of technique and early neuropathological consequences following middle cerebral artery occlusion. Journal of Cerebral Blood Flow & Metabolism.
1981;
1
(1)
:
53-60
.
View Article PubMed Google Scholar -
Gharbawie
O.A.,
Whishaw
P.A.,
Whishaw
I.Q.,
The topography of three-dimensional exploration: a new quantification of vertical and horizontal exploration, postural support, and exploratory bouts in the cylinder test. Behavioural brain research.
2004;
151
(1-2)
:
125-135
.
View Article PubMed Google Scholar -
Montoya
C.,
Campbell-Hope
L.,
Pemberton
K.,
Dunnett
S.,
The "staircase test": a measure of independent forelimb reaching and grasping abilities in rats. Journal of neuroscience methods.
1991;
36
(2-3)
:
219-228
.
View Article Google Scholar -
Ballermann
M.,
Metz
G.A.,
McKenna
J.E.,
Klassen
F.,
Whishaw
I.Q.,
The pasta matrix reaching task: a simple test for measuring skilled reaching distance, direction, and dexterity in rats. Journal of neuroscience methods.
2001;
106
(1)
:
39-45
.
View Article Google Scholar -
Ting
A.H.,
McGarvey
K.M.,
Baylin
S.B.,
The cancer epigenome-components and functional correlates. Genes & development.
2006;
20
(23)
:
3215-3231
.
View Article PubMed Google Scholar -
Ginsberg
M.D.,
Adventures in the pathophysiology of brain ischemia: penumbra, gene expression, neuroprotection: the 2002 Thomas Willis Lecture. Stroke.
2003;
34
(1)
:
214-223
.
View Article PubMed Google Scholar -
Zhang
R.,
Wang
Y.,
Zhang
L.,
Zhang
Z.,
Tsang
W.,
Lu
M.,
Sildenafil (Viagra) induces neurogenesis and promotes functional recovery after stroke in rats. Stroke.
2002;
33
(11)
:
2675-2680
.
View Article PubMed Google Scholar -
Zhao
X.,
Liu
S.J.,
Zhang
J.,
Strong
R.,
Aronowski
J.,
Grotta
J.C. ,
Combining insulin-like growth factor derivatives plus caffeinol produces robust neuroprotection after stroke in rats. Stroke.
2005;
36
(1)
:
129-134
.
View Article PubMed Google Scholar -
Trinh
K.,
Andrews
L.,
Krause
J.,
Hanak
T.,
Lee
D.,
Gelb
M.,
Decaffeinated coffee and nicotine-free tobacco provide neuroprotection in Drosophila models of Parkinson's disease through an NRF2-dependent mechanism. Journal of Neuroscience.
2010;
30
(16)
:
5525-5532
.
View Article PubMed Google Scholar -
Yan
R.,
Zhang
J. ,
Park
H.J.,
Park
E.S.,
Oh
S.,
Zheng
H.,
Synergistic neuroprotection by coffee components eicosanoyl-5-hydroxytryptamide and caffeine in models of Parkinson's disease and DLB. Proceedings of the National Academy of Sciences.
2018;
115
(51)
:
E12053-E12062
.
View Article PubMed Google Scholar -
Xu
K.,
Xu
Y.H.,
Chen
J.F.,
Schwarzschild
M.A.,
Caffeine's neuroprotection against 1-methyl-4-phenyl-1, 2, 3, 6-tetrahydropyridine toxicity shows no tolerance to chronic caffeine administration in mice. Neuroscience letters.
2002;
322
(1)
:
13-16
.
View Article Google Scholar -
Chen
J.F.,
Xu
K.,
Petzer
J.P.,
Staal
R.,
Xu
Y.H.,
Beilstein
M.,
Neuroprotection by caffeine and A2A adenosine receptor inactivation in a model of Parkinson's disease. Journal of Neuroscience.
2001;
21
(10)
:
RC143-RC
.
View Article PubMed Google Scholar -
Novitzky
I.,
Marianayagam
N.J.,
Weiss
S.,
Muhsinoglu
O.,
Fridman
M.,
Leibovitch
T.A.,
Comparison of neuroprotective effect of bevacizumab and sildenafil following induction of stroke in a mouse model. BioMed research international.
2016
.
View Article Google Scholar -
Freret
T.,
Bouet
V.,
Improvements of the stroke model guidelines--animal body weight and long-term functional concerns. J Exp Stroke Transl Med.
2009;
2
(2)
:
28-31
.
View Article Google Scholar -
Grabowski
M.,
Brundin
P.,
Johansson
B.B.,
Paw-reaching, sensorimotor, and rotational behavior after brain infarction in rats. Stroke.
1993;
24
(6)
:
889-895
.
View Article PubMed Google Scholar -
Barth
P.G.,
Pontocerebellar hypoplasia-how many types?. European Journal of Paediatric Neurology.
2000;
4
(4)
:
161-162
.
View Article PubMed Google Scholar
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Volume & Issue : Vol 7 No 5 (2020)
Page No.: 3768-3777
Published on: 2020-05-25
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