Background
HBV is a classical virus that has amazed the researchers and clinicians around the world first with geographic relationship of its genotypes then secondly the association of its different genotypes with a wide spectrum of clinical manifestations. In the recent years, there has been an explosion of knowledge regarding clinical significance of HBV genotypes in terms of clinical outcomes and therapeutic response to antiviral therapy in patients with HBV related severe liver conditions
Initially studies on the effect of genotypes on disease progression were reported from South-east Asian countries where HBV is hyperendemic. Since genotypes B and C are most prevalent in this region severity of liver dysfunction was found associated with these genotypes. Patients infected with genotype C were found having higher HBV-DNA levels compared with those infected with genotype B
Results
Two hundred and ninety five HBsAg positive registered patients were selected from the PMRC OPD. Two hundred and twenty six (76.6%) were males, 69 (23.4%) were females (M to F ratio 3.3:1) Table
Genotype distribution according to disease and gender
Diagnosis/Genotype
Male n = 226(76.6%)
Female n = 69(23.4%)
Total (n = 295)
Acute (CAH)
124
32
156(52.9%)
Genotype
D
88 (71.0%)
20 (62.5%)
108 (69.2%)
A
23 (18.5%)
5 (15.6%)
28 (18.0%)
AD
13 (10.5%)
7 (21.9%)
20 (12.8%)
Chronic (CLD)
43
11
54(18.3%)
Genotype
D
30 (69.8%)
9 (81.8%)
39 (72.2%)
A
10 (23.3%)
2 (18.2%)
12 (22.2%)
AD
3 (6.9%)
-
3 (5.6%)
Carrier (asymptomatic)
48
23
71(24%)
Genotype
D
38 (79.2%)
15 (65.2%)
53 (74.7%)
A
6 (12.5%)
8 (34.8%)
14 (19.7%)
AD
4 (8.3%)
-
4 (5.6%)
Cirrhosis/HCC
11
3
14(4.7%)
Genotype
D
7 (63.6%)
1(33.3%
8 (57.14%)
A
4(36.3%)
2 (66.6%)
6 (43.8%)
AD
-
-
-
Primer sequences used for HBV genotyping by nested PCR (position, specificity, and polarity). An "M " represents a nucleotide that could be either an A or a C; a "Y" represents a nucleotide that could be either a C or a T. nt, nucleotide.
Primers
Sequence
Gene/CDS
Product
Step-one PCR
P1b universal, sense)
5'-TCA CCA TAT TCT TGG GAA CAA GA-3'
nt2823-2845,
1065 bp
S1-2 universal, antisense)
5'-CGA ACC ACT GAA CAA ATG GC-3'
nt685-704,
Step-two PCR
B2 sense
5'-GGC TCM AGT TCM GGA ACA GT-3'
nt67-86, types A specific, to E
Mix A
BAIR antisense
5'-CTC GCG GAG ATT GAC GAG ATG T-3'
nt113-134, type A specific,
68 bp
BBIR antisense
5'-CAG GTT GGT GAG TGA CTG GAG A-3'
nt324-345, type B specific,
122 bp
BCIR antisense)
5'-GGT CCT AGG AAT CCT GAT GTT G-3'
nt165-186, type C specific,
281 bp
3% agarose gel showing genotype specific bands in patients infected with hepatitis B virus
3% agarose gel showing genotype specific bands in patients infected with hepatitis B virus. Lane 1 and 2 show HBV genotype A specific 68 bp band; Lane 3 show 100 bp marker; Lane 4,5 and 6 show HBV genotype D specific 119 bp band.
Discussion
This is the first study from Pakistancomparing the clinical outcome of HBV-related liver disease in patients infected with different HBV genotypes using a PCR based method. Out of 295 HBsAg positive registered patients, 225 (77%) were males, and 69 (23%) were females (M to F ratio approximately 3.3:1) who were suffering from various liver conditions were genotyped (Table
The clinical significance of different HBV genotypes has become increasingly recognized in patients with acute and chronic infection
In Chronic infection levels of viremia are generally low. The strong determinant of chronicity is age at the time of infection. Long-term prognosis is poorer among HBeAg-negative individuals compared to their counterparts who are HBeAg-positive. In this study 18.4% had Chronic (CLD) Hepatitis. Out of 54 chronic patients, 72.2% had genotype D, 22.2% had A and 5.6% had AD. This is in contrast to a study by Mayerat et al.
During the Carrier state, low HBsAg levels are marked by HBeAg negativity with anti-HBe positivity, low HBV DNA level and repeatedly normal ALT. In this study the highest prevalence of Genotype D was found in HBV asymptomatic carriers (74.7%). Borchani
Cirrhosis and Hepatocellular Carcinoma (HCC) are two major long-term complications of chronic HBV infection which developed in 14 of our patients (11 males and 3 females). Five had developed cirrhosis and 9 hepatocellular carcinoma. Chronically infected subjects have a 100 times increased risk of hepatocellular carcinoma compared to non-carriers. HBsAg positivity increases risk of developing HCC by 10 folds and HBeAg positivity by 60 folds, whereas, a detectable HBV DNA level yields a 4 fold increased risk of HCC
Among the nine patients in this study who developed HCC two were females and seven were males. Age ranged from 35 yrs to 68 yrs. Genotype D being most prevalent was present in 7(77.7%) patients, whereas genotype A in two patients, who developed HCC from chronic infection. Out of 5 with genotype D, five males, age range 50 yrs to 68 yrs, were long time carriers (fifteen years after suffering from HBV infection) and the rest of the two, one male and other female were in the age range 35 yrs and 45 yrs. Thakur et al.
Generally, all categories of liver diseases showed male dominance, especially in HCC it is well documented. HCC incidence is three to six times higher in males than in females, suggesting a tumorigenic effect of androgens
Combination of AD exist where ever genotype A and D are prevalent such as India
Gerner et al.
Conclusion
Genotyping of HBV may remain a research tool unless we prove that it can predict the risk of adverse outcomes (fulminant disease, cirrhosis, HCC) or can influence decision-making in managing these conditions. Studies so far around the world have lead us to believe that different genotypes may be associated with different rates of progression from acute to chronic HBV infection. However, differences in host and environmental factors make it difficult to extrapolate findings from one geographical region to another. Therefore, larger, in-depth longitudinal prospective studies are necessary, in various regions of the world, that could provide more information on the relationship of HBV genotypes to the severity of liver disease and thereby clinical outcome.
Methods
Selection of subjects
HBsAg positive 295 registered patients wereselected. irrespective of age and gender, with HBV-related liver disease such as Acute, Chronic, Cirrhosis, HCC, attending the outpatient Department of Pakistan Medical and Research Council(PMRC), Gastroenterology unit JPMC during the years 2006 to 2007, were selected for the study. All patients were HBV positive, registered patients Clinical data were retrieved from medical records, as were laboratory test results including hemogram, liver function tests, coagulation profile, and findings at abdominal ultrasonography, upper gastrointestinal endoscopy and liver biopsy. Liver cirrhosis and HCC were diagnosed either on the basis of histology, or on a combination of radiological, endoscopic and laboratory data. Serum samples were collected from the study patients when they came for the follow-up. A written as well as verbal informed consent was taken from each subject; however, in case of patients who were under the age of 18, parental consent was obtained. Prior to this approval of ZMUH ethical review committee was obtained. The following inclusion and exclusion criteria were applied while selecting patients for this study:
Inclusion Criteria
All healthy and diseased HbsAg positive individuals (healthy carriers, acute hepatitis, chronic hepatitis).
Exclusion Criteria
Patients with other hepatic viral markers (A, C, D, E) with HBV were excluded.
DNA extraction
DNA extraction from serum was done by DNA extraction kit (Promega Minipreps). The HBV genome was amplified by nested PCR using the universal primers (P1 and S1-2) for the outer primers, followed by two different mixtures containing type-specific inner primers as described above.
PCR Amplification
A modified version of nested PCR developed by Naito et al.
Diagnosis according to gender in different categories of patients
Diagnosis
Male (n = 226) (76.6%)
Female (n = 69) (23.4%)
Total (n = 295)
Number
Percent
Number
Percent
Number
Percent
Acute (CAH)
124
54.86
32
46.3
156
52.7
Chronic (CLD)
43
19.0
11
16.0
54
18.2
Carrier
48
21.2
23
33.3
71
24
Cirrhosis/HCC
11
4.8
3
4.3
14
4.7
Primer sequence and detail
Step one PCR
The first PCR was carried out in a tube containing 50 μl of a reaction buffer made up of the following components: 50 ng each of the outer primer, a 200 μM concentration of each of the four deoxynucleotides, 1U of Taq DNA polymerase (Perkin-Elmer, Norwalk, Conn.), and 1× PCR buffer containing 1.5 mM MgCl2. The extracted DNA was given an initial 10 min incubation at 95°C for a hot start reaction. After 10 min the PCR program was paused to dispense the master-mix in all tubes. The thermocycler (GeneAmp PCR system 2400,9600, and 9700A; Perkin-Elmer) was programmed to first incubate the samples for 10 min at 95°C, followed by 35 cycles consisting of 94°C for min., 94°C for 20s, 55°C for 20s, and 72°C for 1 min. with a final extension of 5 min. at 72°C and 4°C.
Step two PCR
Two second-round PCRs were performed for each sample, with the common universal sense primer (B2) and mix A for types A through C and the common universal antisense primer (B2R) and mix B for types D through F.A 2.5 μl aliquot of the first PCR product was added to two tubes containing the second sets of each of the inner primer pairs, each of the deoxynucleotides, AmpliTaq Gold DNA polymerase, and PCR buffer, as in the first reaction. These were amplified for35 cycles with the following parameters: preheating at 94°C for 3 min, 15 cycles of amplification at 94°C for 20s, 58°C for 30s, and 72°C for 40s, and an additional 20 cycles of 94°C for 30s, 60°C for 30s, and 72°C for 45s with an extension of 7 min at 72°C and incubation at 4°C. Genotypes of HBV for each sample were determined by identifying the genotype-specific DNA bands. The two different second-round PCR products from one sample were separately electrophoresed on a 3% agarose gel,(1% agarose plus 2% Nusieve Agarose) stained with ethidium bromide, and evaluated under UV light. The sizes of PCR products were estimated according to the migration pattern of a 50-bp DNA ladder (Pharmacia Biotech, Uppsala, Sweden).
Competing interests
The author(s) declare that they have no competing interests.
Authors' contributions
SB, AAS and WA designed the Research project. SB did all the bench work. SB and AAS wrote the manuscript. WA, HQ and AA clinically assessed the patients prior to selection and also helped in the clinical data retrieval from the medical records (all were their registered patients).