STUDY THE ROLE OF HEPATITIS C VIRUS INFECTION IN PATIENTS WITH CEREBRAL INFARCTION

Document Type : Original Article

Authors

1 Department of Internal Medicine, Faculty of Medicine, Al-Azhar University

2 Department of Diagnostic Radiology, Faculty of Medicine, Al-Azhar University

3 Department of Clinical Pathology, Faculty of Medicine, Al-Azhar University

Abstract

Background: Chronic hepatitis C virus (HCV) infection has been linked to numerous co-existing conditions including metabolic abnormalities and cardiovascular disease. Stroke is a major public health crisis world-wide. About 87% of strokes are ischemic. Between 25- 40% of ischemic stroke may be cryptogenic. HCV infection is associated with a wide spectrum of extra-hepatic manifestations, affecting different organ systems. Neurological complications occur in a large number of patients and range from peripheral neuropathy to cognitive impairment and/or cerebral infarctions (CI). 
Objective: Studying the role of HCV infection in patients having CI.
Patients and Methods: After departmental ethics committee approval and patient consents were obtained, 60patients included in this work: 20 patients having CI and chronic hepatitis C (CHC), 20 patients having CI without CHC, and 20 patients having CHC without CI. All patients were subjected to history taking and clinical examination, complete blood count (CBC), evaluation of HCV antibodies, polymerase chain reaction (PCR) for HCV ribonucleic acid (RNA), hepatitis B surface antigen (HBs-Ag), liver function tests, renal function tests, lipid profile, antinuclear antibody (ANA), anticardiolipin antibodies immunoglobulin G (ACL-IgG), antineutrophil cytoplasmic antibodies (ANCA), cryoglobulin, fasting plasma glucose (FPG) and post-prandial plasma glucose (PPPG). In addition, ultrasound (U/S) abdomen, magnetic resonance imaging (MRI) brain, doppler study of the carotid arteries and echocardiography.
Results: Group A (CI and CHC) patients were significantly younger and females were predominant in these patients than those of either group B (CI without CHC) or C (CHC without CI) .Group B patients were significantly overweighed compared to group A or C. Total cholesterol (TC), triglyceride (TG), FPG and low density lipoprotein (LDL) significantly decreased in group A and C compared with group B .Patients of group A showed significantly higher positive of HCV viremia, cryoglobulins, ANA, c-ANCA and ACL-IgG, compared with group C, while those of group B were negative for same parameters. Carotid atherosclerosis and ischemic heart disease (IHD) were significantly higher in patients of group A, compared with group (B and C), respectively.
Conclusion: Chronic HCV infection is a risk factor in development of CI by multiple mechanisms including atherosclerosis, thromboembolism and vasculitis. Also, it increases stroke risk and might be considered as an important and independent risk factor.

Keywords


STUDY THE ROLE OF HEPATITIS C VIRUS INFECTION IN PATIENTS WITH CEREBRAL INFARCTION

 

By

 

Abd El-Hamid Al-Noby Khalil*, Salem Soliman Ahmed*,

Abd El-Moneim Mohamed Barrak*, Gouda Mohamed Khalifa**, Ebrahim Ali Ebrahim***, Rabea Fathy Abbbas*

and Mostafa Ahmed Roshdy Hussein*

                                                                                                              

Department of *Internal Medicine, **Diagnostic Radiology and *** Clinical Pathology,

Faculty of Medicine, Al-Azhar University

 

ABSTRACT

Background: Chronic hepatitis C virus (HCV) infection has been linked to numerous co-existing conditions including metabolic abnormalities and cardiovascular disease. Stroke is a major public health crisis world-wide. About 87% of strokes are ischemic. Between 25- 40% of ischemic stroke may be cryptogenic. HCV infection is associated with a wide spectrum of extra-hepatic manifestations, affecting different organ systems. Neurological complications occur in a large number of patients and range from peripheral neuropathy to cognitive impairment and/or cerebral infarctions (CI). 

Objective: Studying the role of HCV infection in patients having CI.

Patients and Methods: After departmental ethics committee approval and patient consents were obtained, 60patients included in this work: 20 patients having CI and chronic hepatitis C (CHC), 20 patients having CI without CHC, and 20 patients having CHC without CI. All patients were subjected to history taking and clinical examination, complete blood count (CBC), evaluation of HCV antibodies, polymerase chain reaction (PCR) for HCV ribonucleic acid (RNA), hepatitis B surface antigen (HBs-Ag), liver function tests, renal function tests, lipid profile, antinuclear antibody (ANA), anticardiolipin antibodies immunoglobulin G (ACL-IgG), antineutrophil cytoplasmic antibodies (ANCA), cryoglobulin, fasting plasma glucose (FPG) and post-prandial plasma glucose (PPPG). In addition, ultrasound (U/S) abdomen, magnetic resonance imaging (MRI) brain, doppler study of the carotid arteries and echocardiography.

Results: Group A (CI and CHC) patients were significantly younger and females were predominant in these patients than those of either group B (CI without CHC) or C (CHC without CI) .Group B patients were significantly overweighed compared to group A or C. Total cholesterol (TC), triglyceride (TG), FPG and low density lipoprotein (LDL) significantly decreased in group A and C compared with group B .Patients of group A showed significantly higher positive of HCV viremia, cryoglobulins, ANA, c-ANCA and ACL-IgG, compared with group C, while those of group B were negative for same parameters. Carotid atherosclerosis and ischemic heart disease (IHD) were significantly higher in patients of group A, compared with group (B and C), respectively.

Conclusion: Chronic HCV infection is a risk factor in development of CI by multiple mechanisms including atherosclerosis, thromboembolism and vasculitis. Also, it increases stroke risk and might be considered as an important and independent risk factor.

Keywords: Hepatitis C virus, ANA, c-ANCA.

  

 

INTRODUCTION

     HCV infection is a common and chronic disorder with numerous extra-hepatic manifestations (Acharya and Pacheco, 2008). HCV infection has been found to be strikingly associated with autoimmune phenomenon with autoantibodies commonly seen (Cojocaru et al., 2007). HCV infection is a condition that has increased the risk of stroke (Cojocaru et al., 2005).

     People with HCV infection appear to have a higher likelihood of dying from strokes than non-infected individuals. Ischemic stroke can occur when blood clots triggered by atherosclerosis especially build-up of plaque in the carotid arteries that supply the brain, break off and lodge in small blood vessels (Lee et al., 2010).

     Neurological complications of HCV occur in a large number of patients and range from peripheral neuropathy to cognitive impairment and/or cerebral infarctions (CI). Pathogenetic mechanisms responsible for nervous system dysfunction are mainly related to production of autoantibodies, immune complexes, cryoglobulins, extra-hepatic replication of HCV in neural tissues and the effects of circulating inflammatory cytokines and chemokines (Salvatore et al., 2012).

PATIENTS AND METHODS

Patients:

Sixty patients were included in this study. They were divided into 3 equal groups:

● Group (A) having CI and CHC,

● Group (B) having CI without CHC,

● Group (C) having CHC without CI.

     Patients were presented to Emergency Department of Sayed Galal Hospital, Al-Azhar University, and the outpatient clinic, and admitted to the Internal Medicine Department. 

     The study was carried out during the period from March 2013-June2016.

Exclusion criteria:

● Smokers or alcoholics or had any other special habits of significant importance.

● Those receiving IFN therapy.

● Diabetics, hypertensives or hyperlipi-demics.

● Those having renal impairment, endo-crine diseases, cardiac problems or collagen diseases.

● Those having history of contraceptive pills intake.

● Those having any other liver disease.

Methods:

● Thorough history taking and full clinical examination were done for all patients.

● Laboratory investigations for selected patients included assessment of HCV-Ab and HBs-Ag by using  3rdgeneration ELISA technique, detection of HCV-RNA by PCR (Cobas amplicor analyzer), viral load in international unit (IU) and degree of viremia, liver function tests evaluation including alanine transaminase (ALT), aspartate transaminase (AST), serum albumin, serum bilirubin, prothrombin time (PT), and international normalized ratio (INR) using (Hitachi, 911automatic analyzer), renal function tests assessment including blood urea and serum creatinine using (Hitachi, 911automatic analyzer), CBC including hemoglobin(Hb), white blood cells (WBCs) and platelets (PLT), lipid profile assessment including TC, TG, LDL and high density lipo-protein (HDL), assessment of ANA, ANCA (anti-proteinase-3 antibody), ACL-IgG and cryoglobulinemia evaluation by simple blood test (Ferri, 2008).

● Abdominal ultrasonography to assess the chronic liver diseases and its complications.

● Echocardiography to detect criteria suggestive of ischemic heart diseases.

● Doppler study of the carotid system to assess carotid intima media thickening (C-IMT).

● MRI brain to diagnose cerebral infarction (CI).

● Informed consents were taken from all patients.

Statistical analysis of data by IBM computer using statistical program for social science (SPSS) version 20: Chi-square test to compare qualitative variables between groups, unpaired (Independent) t-test to compare quantita-tive variables between groups, and one way analysis of variance (ANOVA) followed by post hoc analysis (LSD test) to compare between more than two groups regarding quantitative data with parametric distribution.

RESULTS

Group (A) patients were significantly younger than those of groups (B) and (C). Females were predominant in group (A) patients, while males were predominant in group (B) patients, and both sexes were equally distributed in group (C) patients. Group (B) patients were significantly overweighed compared with either that of groups (A) or (C) (Table 1).

 

 

Table (1): Age, sex and BMI among the studied groups.

Groups

 

Parameters

Group A

(CI+ CHC)

Group B

(CI without CHC)

Group C

(CHC without CI)

One way ANOVA

No = 20

No = 20

No = 20

F/X²*

P

Age (years)

M± SD

50.6 ± 3.65

59.4 ± 6.34

55.3 ± 4.41

15.951

0.000*

Range

44 – 58

43 - 70

48 – 65

Sex

Female

15 (75%)

6 (30%)

10 (50%)

8.142

0.017*

Male

5 (25%)

14 (70%)

10 (50%)

BMI (kg/m2)

M ± SD

23.28 ± 3.86

27.95 ± 3.63

24.80 ± 5.38

8.222

0.001*

Range

16 - 32

23 – 32

17 – 34

 

 

     Total cholesterol, TG, FPG and LDL significantly decreased in groups (A) and (C) compared with group (B).  There was an insignificant difference between the 3 groups as regards 2-hr PPPG (Table 2).

 

Table (2): Results of FPG, 2hrs-PPPG, TC, TG, LDL & HDL in the 3 groups.

Groups

 

Parameters                              

Group

(A)

Group

(B)

Group

(C)

One way ANOVA

Post hoc analysis

No= 20

No= 20

No= 20

F

P

P1

P2

P3

FPG

(mg/d)

M±SD

92.55

±21.28

106.40

±15.60

92.45

±20.59

3.450

0.039

0.043

0.214

0.002

Range

60 - 134

60 - 134

80 - 145

PPPG

(mg/d)

M±SD

143.75

±20.64

150.70

±30.60

131.75

±24.09

2.838

0.067

0.073

0.064

0.003

Range

110 - 200

110 – 200

110 - 210

TC

(mg/d)

M±SD

162.65±21.40

210.85

±57.10

131.25

±32.22

20.277

0.000

0.001

0.001

0.000

Range

113-  200

113-  200

118 - 352

TG

(mg/d)

M±SD

104.55

±25.81

163.50

±52.79

88.20

± 31.00

21.330

0.000

0.000

0.078

0.000

Range

67 -  145

67 -  145

89 -  320

LDL

(mg/d)

M±SD

79.25

± 19.08

105.00

±26.21

70.75

± 22.65

12.203

0.000

0.001

0.207

0.000

Range

45 - 110

45 - 110

65 - 155

HDL

(mg/d)

M±SD

57.30

± 17.35

49.90

± 16.78

58.90

± 17.79

1.539

0.223

0.178

0.775

0.108

Range

29 - 100

29 - 100

20 – 87

 

     HCV-viremia was significantly higher in group (A) compared with group (C) (Table 3).

 

Table (3): Comparison between groups (A) and (C) as regards HCV-viremia.

HCV-RNA

Group (A)

Group (C)

P

No = 20

No = 20

Mean ± SD

2446152.25 ± 2338691.00

365870.45 ± 289148.80

0.000

Range

150321 -  9805500

12069.00  -  930100.00

 

 

   Cryoglobulinemia significantly increased in group A (50%), compared to either group C (10%) or group B (0%). Patients of group (A) showed significantly higher positive ANA (55%), c-ANCA (65%) and ACL-IgG(30%), compared with those of group C (20%), (15%), (5%) respectively, while those of group (B) were negative for these parameters (Table 4).

 

 

 

Table (4): Cryoglobulins, ANA, c-ANCA and ACL-IgG in the studied groups.

                               Groups

Parameters

Group (A)

Group (B)

Group (C)

Chi-Square tests

No

%

No

%

No

%

P-Value

 

Cryoglobulin

Negative

10

50%

20

100%

18

90%

17.500

0.000*

Positive

10

50%

0

0%

2

10%

ANA

Negative

9

45%

20

100%

16

80%

17.883

0.007

Positive

11

55%

0

0%

4

20%

c-ANCA

Negative

7

35%

20

100%

17

85%

23.693

0.000*

Positive

13

65%

0

0%

3

15%

ACL-IgG

Negative

14

70%

20

100%

19

95%

11.170

0.043*

Positive

6

30%

0

0%

1

5%

 

 

     Carotid atherosclerosis and IHD were significantly higher in group A (70%, 45%), compared with group B (30%, 20%) and group C (10%, 10%), respectively (Table 5).

 

 

 

Table (5): Carotid Doppler and Echo finding among the studied groups.

Groups

 

Parameters

Group A

Group B

Group C

One way ANOVA

No = 20

No = 20

No =20

F/X2

P

Carotid IMT

Negative

6 (30%)

14 (70%)

18(90)

21.073

0.000*

Mild

7 (35%)

6 (30%)

1 (5%)

Moderate

7 (35%)

0 (0%)

1 (5%)

IHD

Negative

11 (55%)

16 (80%)

18(90)

6.933

0.031*

Positive

9 (45%)

4 (20%)

2(10%)

 

 

DISCUSSION

     The obtained results in the current study showed that the female predominance was evident in group A compared with groups B and group C. This difference was highly significant between the 3 groups. Also, the mean age of group (A) was younger than groups (B and C), this difference was highly significant between the 3 groups. So, the CI associated with HCV was more in females particularly the younger women.

    This result was not in agreement with Chen and Morgan (2006) who found that male predominance was evident in the infected group compared with other groups, and the rate of chronicity in HCV infection appears to be lower in women particularly younger women. The reason of the difference was because in our study we discussed HCV with CI, while previous study discussed the chronicity of HCV only. So, we found that HCV infection with CI more in females suggested theory of vasculitis which was more common in females as a contributing factor in occurrence of CI in these patients. Moreover, stroke occurred at a younger age in HCV-infected patients as well as the negative prognostic impact of HCV-RNA serum levels on outcome, as opposed to a more limited role for gender and classic predisposing conditions (Zampino et al., 2013 and Adinolfi et al., 2014).

     In this study, non-infected HCV group (B) was overweighed more than infected HCV groups (A and C), with a significant difference between the 3 groups regarding BMI. On the other hand, Aksöz et al. (2008) found that BMI is not statistically different between patients with HCV infection and healthy subjects. So, increased BMI is not a risk factor for development of cerebral infarctions in CHC patients.

    In this study, there was a highly significant difference between the 3 groups regarding TC, TG, LDL and FPG. Infected HCV groups (A and C) have low lipid profile, while infected HCV group (B) has a higher level. These findings were in agreement with those obtained by Dai et al. (2008) who found that TC and TG levels were significantly lower in anti-HCV positive patients with high HCV-RNA than in anti-HCV positive patients with HCV-RNA negative. This could be explained by the binding of HCV particles to HDL, LDL and VLDL, the impaired hepatocyte assembly of VLDL and the entry of HCV into hepatocytes through the LDL receptor. Thus, chronic HCV can impair the synthesis of TC and TG (Andre´ et al., 2002 and Perlemuter et al., 2002).

    In this study, HCV-RNA levels were higher (high viremia) in group A compared with group (C) with a significant difference. An elevation of serum HCV-RNA level was associated with an increased risk of cerebrovascular death, suggesting that individuals with an active HCV infection may trigger a stronger inflammation response by host-virus interaction, leading to atherothrombosis (Werner et al., 2007). Also, localization of HCV-RNA in human carotid plaques provides strong evidence for an association between HCV infection and atherosclerosis (Boddi et al., 2010).

    In the current study, the immunological markers, ANA, c-ANCA and ACL-IgG in all the studied groups revealed high positivity in infected HCV group (A) with CI, 55%, 65% and 30% respectively, while in infected HCV group (C) without CI, were 20%, 15% and 5% and non- infected group (B), were negative. This result was highly significant which suggested theory of vasculitis in developing of cerebral infarctions in HCV patients.

    This result was in agreement with Cojocaru et al. (2007) who reported that c-ANCA were positive in 58 % patients with ischemic stroke and HCV infection. All sera with ANCA showed c-ANCA patterns and contained anti-PR3 specificity. HCV patients with ANCA showed a higher prevalence of cerebral vasculitis.

    In addition, Cojocaru et al. (2005) reported that the mean levels of serum IgG-aCL antibodies were significantly higher among the HCV patients with acute ischemic stroke than those with acute ischemic stroke without HCV. So, c-ANCA and anticardiolipin antibodies associated with HCV may be an important marker for acute ischemic stroke.

     In this study, cryoglobulinemia was demonstrated in 10 patients of group (A), in 2 patients of group (C), and no patients of group (B). This difference was highly significant. High level of cryoglobuli-nemia in group (A) suggested the role of cryoglobulins inducing CNS vasculitis. This result was supported by the result of Giordano et al. (2007) who reported that HCV infection is associated with an increased risk of cryoglobulinemia, which is thought to participate in the formation of immune complexes precipitating in vessel walls then leads to vasculitis.

Occlusive cerebral vascular diseases can also occur in the context of HCV-related vasculitis such as mixed cryoglobuli-nemia, antiphospholipid syndrome and ANCA-associated vasculitis (Castro et al., 2014). In addition, Gulliaet al. (2016) reported higher percentage of ANA was found in CGs HCV-patients, suggesting that the production of ANA seems strictly related to CGs production.

     C-IMT in the current study showed a highly significant difference between the 3 groups, group (A) had carotid atherosclerosis (70%) comparing with group (B) (30%), while group C had 10% regardless the gender. These results were in agreement with those reported by Aslam et al. (2010) and Boddi et al. (2010) who found positive correlations between HCV infection and carotid IMT, plaque and stroke.

     In this study, the stroke groups (A and B), HCV positive patients showed a higher prevalence of IHD, while group (C) non-stroke has only 10%. This result was in agreement with that seen by Forde et al. (2012) who reported a higher prevalence of past ischemic cardiovas-cular events in HCV positive subjects. However, such previous cardiovascular event was not associated with an increased risk of cerebral ischemic stroke in studied population who HCV negative subjects.

     In patients having CI and HCV (group A), there were high HC viremia, increased vasculitis markers as cryoglobulinemia (70%), ANA (55%), c-ANCA (65%) and ACL-IgG (30%). These were in addition to more IHD affection (45%) and carotid atherosclerosis as indicated by increased IMT (70%). These results supported the suggestion that HCV infection may cause CI through multiple mechanisms including vasculitis and development of early atherosclerosis as an extra-hepatic manifestations.

CONCLUSION

    Chronic HCV infection is a risk factor in the development of CI by multiple mechanisms including atherosclerosis, thromboembolic and vasculitis. Also, it increases stroke risk and might be considered as an important and independent risk factor.

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دراسة دور الإصابة بالفیروس الکبدى (سى) فى مرضى الجلطة الدماغیة

 

عبـد الحمیـد النـوبـى خلیـل* ، سالم سلیمان أحمد* ، عبد المنعم محمد براک*، جوده محمد خلیفة**، إبراهیم على إبراهیم*** ، ربیع فتحى عباس*، ومصطفی أحمد رشدى حسین*

 

أقسام الأمراض الباطنة* والأشعة التشخیصیة** والباثولجیا الإکلینیکیة***- کلیة الطب - جامعة الأزهـر

خلفیة البحث : یصاحب الإلتهاب الکبدى المزمن " سى" بالعدید من الأمراض منها التمثیل الغذائى الغیر طبیعى وأمراض  الأوعیة الدمویة  والقلب . وتعتبر الجلطات الدماغیه من أکثر الأمراض شیوعاً فى أنحاء العالم . ومعظم الجلطات الدماغیة تحدث  بسبب قطع الإمداد الدموى للمخ  فى 87% من الحالات  غیر أن  حوالی 25% -  40% من حالات الجلطات المخیة غیر معروفة السبب . وتؤدى العدوى بالإلتهاب الکبدى المزمن " سى" إلى أعراض خارج الکبد تؤثر على أعضاء أخرى بالجسم وتحدث مضاعفات مختلفة للجهاز العصبى لکثیر من مرضى فیروس" سى" بدایة من إلتهاب الاعصاب الطرفیة والإضطرابات النفسیة إلى حدوث جلطات بالمخ.

الهدف من البحث : دراسة دور الإصابة بفیروس الکبد "سى" المزمنة فى حدوث الجلطة المخیة.

المرضى وطرق البحث: أجریت هذه الدراسة على 60 مریضاً بعد أخذ الموافقة منهم وتم تقسیمهم إلی ثلاث مجموعات متساویة : مجموعه (أ) مصابون بالإلتهاب الکبدى الفیروسى المزمن " سى" والجلطات الدماغیة، ومجموعه (ب) مصابون بجلطات دماغیة وغیر مصابون بالإلتهاب الکبدى الفیروسى المزمن " سى"، ومجموعه (ج) مصابون بالإلتهاب الکبدى الفیروسى المزمن " سى" وغیر مصابون بجلطات دماغیة.

وقد تم عمل الآتى لکل المرضى : أخذ التاریخ المرضى الکامل وفحص اکلینیکى شامل وعمل تحالیل (صورة دم کاملة وقیاس الأجسام المضادة لفیروس "سى"  وعمل  (PCR)الکمى وقیاس دلائل الإصابة بفیروس الکبد المزمن "بی" ، ووظائف الکبد و الکلى ، وقیاس نسبة کثافة الدهون بالدم ، وقیاس مستوى السکر الصائم وبعد الأکل بساعتین ، وقیاس نسبة الکریوجلوبیولین بالدم ، وقیاس دلائل مناعیة (c-ANCA, ACL-IgG , ANA) ، وعمل موجات صوتیة على البطن ودوبلرملون على الشرایین الثباتیة بالرقبة ورنین مغناطیسى على المخ وموجات صوتیة على القلب. 

النتائج :

● مرضى المجموعة (أ) اصغر عمراً ومعظمهم إناث مقارنة بمرضى المجموعتین (ب) و(ج) ، کما وجد زیادة ذات دلالة إحصائیة فى متوسط وزن مرضى المجموعة (ب) مقارنة بالمجموعتین (أ) و(ج).

● وجود نقص ذو دلالة إحصائیة فى الکولیسترول والدهون الثلاثیة والسکر الصائم والدهون قلیلة الکثافة بالدم لدى مرضى المجموعتین (أ) و(ج)  مقارنة بمرضى المجموعة (ب).

● وجود زیادة ذات دلالة إحصائیة فى نسبة الفیروس الکمی والکریوجلوبیولین والدلالات المناعیة فی الدم لدى مرضى المجموعة (أ) مقارنة بمرضى المجموعة (ج) ، بینما مرضى المجموعة (ب) سلبیة لهذه الدلالات.

● وجود زیادة ذات دلالة إحصائیة لتصلب الشرایین الثباتیة و قصور الشرایین التاجى للقلب  لدى مرضى المجموعة (أ) مقارنة بمرضى المجموعة (ب)  و (ج).

الاستنتاج : تعتبر الإصابة بفیروس الکبد المزمن "سى" عامل خطورة منفصل لحدوث الجلطات الدماغیة سواءً عن طریق تصلب الشرایین أو تکوین جلطة أو سدادة دمویة أو عن طریق إلتهاب الأوعیة الدمویة المخیة المناعى ، وکذلک تزید من خطورة حدوث الجلطات الدماغیة .    

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