Garlic and vitamin C may be the best remedy for treating weak errection.
Infertility is a multi-parameter phenomenon with a wide range of
factors that affects spermatogenesis and sperm quality. Spermatogenesis is a process in which male sex cells
are produced and the disorder in each of these stages can cause infertility. Fertility in men depends largely on the number, quality, motility, and morphology of the sperm, and the disruption of each of these factors leads to infertility in men. Infertility, as a psychological
crisis, imposes a lot of stress on infertile couples and in different ways threatens their mental health
Failure to have a child is an unpleasant event in the lives of infertile people. Inability to become pregnant after one
year of regular intercourse, without using contraception, is defined as infertility. About 30%-50% of the causes of infertility are related to male problems. Each day, the number of medical reports about the extent of
infertility in the world increases, according to a systematic review in this regard, about 48.5 million couples around the world affected by this problem.
Fertility in men depends largely
on the number, quality, motility, and morphology of the sperm, and the disruption of each of these factors leads to infertility in men. Infertility, as a psychological crisis, imposes a lot of stress on infertile couples and in
different ways threatens their mental health.
The results in the study by Oi et al
indicated that garlic supplementation boosts LH from the pituitary gland, and this stimulates testosterone secretion
from the testicle. Nonetheless, in the study by Bahrami et al, it was recommended that the cooked garlic has better therapeutic effects and, while affecting the reproduction of the sexual cells in testes and epididymis, improves spermatogenesis. Due to presence of dialyldisulfide in its biochemical
structure, garlic affects the hypothalamic-pituitary axis. Diallyldisulfide stimulates the basophilic cells and secretion of LH sex hormones by affecting the anterior pituitary. LH stimulates Leydig cells in the testes, which in turn is a precursor to secretion and regulation of testosterone. Also, diallyldisulfide reduces oxygen free radicals, enhances and strengthens the blood-testis barrier and increases the circulation in the testicles, thus protects the sexual Organs. By increasing blood flow to the testicles (due to the consumption of garlic), phenol and phenolic glycosides are released which increase the glutathione peroxidase enzyme. The role of this enzyme is to protect sperms in testicular and epididymal tissue. The enzyme protects the sperm from the damage of free radicals by placement in the plasma membrane and the nucleus of sperm, epididymal fluid and epididymis, and leads to ultimate maturation and development of the
sperm.
Combining garlic and vitamin C restores erectile strength.
The combination of vitamin C and garlic was proven to be effective to erectile strength. This may not have been scientifically proven. However, most men who chew garlic and 1g of vitamin C reported restoration of strong errection. To get a better benefit from this combination, It is recommended to take garlic and vitamin C at night after dinner and morning before breakfast for at least a period of three days.
Vitamin C improves blood flow, which results in blood flow reaching to the pelvic regions and thus the urethra. This enhances rigidity of the pennis.
References
Mohammadi F, Nikzad H, Taherian A, Amini Mahabadi J, Salehi M. Effects of herbal medicine on male infertility. Anat Sci J. 2013;10(4):3-16.
Kim SJ, Kim MR, Hwang SY, Bae WJ, Kim S, Hong SH, et al. Preliminary report on the safety of a new herbal formula
and its effect on sperm quality. World J Mens Health. 2013;31(3):254-61. doi: 10.5534/wjmh.2013.31.3.254.
Roozbeh N, Rostami S, Abdi F. A review on herbal medicine with fertility and infertility characteristics in males. Iranian Journal of Obstetrics, Gynecology and Infertility. 2016;19(13):18-32.
Mascarenhas MN, Flaxman SR, Boerma T, Vanderpoel S, Stevens GA. National, regional, and global trends in infertility prevalence since 1990: a systematic analysis of 277 health surveys. PLoS Med.2012; 9(12):e1001356. doi: 10.1371/journal.pmed.1001356.
Bahrami KH, Mahjor AA, Johary H, Bahrami R, Bahrami A. Comparative study on histopatological and
histomorphometric effect of raw and cooked garlic on spermatogenesis in testis and epidydims of rats. J Fasa Univ Med Sci. 2014;3(4):371-9
Ouarda M, Abdennour C. Evaluation of the therapeutic efficiency of raw garlic on reproduction of domestic rabbits
under lead induced toxicity. Ann Biol Res. 2011;2(3):38993
Oi Y, Imafuku M, Shishido C, Kominato Y, Nishimura S, Iwai K. Garlic supplementation increases testicular testosterone and decreases plasma corticosterone in rats fed a high protein diet. J Nutr. 2001;131(8):2150-6. doi: 10.1093/jn/131.8.2150
Pal R, Vaiphei K, Sikander A, Singh K, Rana SV. Effect of garlic on isoniazid and rifampicin-induced hepatic injury in rats. World J Gastroenterol. 2006;12(4):636-9.
Amin A, Hamza AA. Effects of Roselle and Ginger on cisplatin-induced reproductive toxicity in rats. Asian J Androl. 2006;8(5):607-12. doi: 10.1111/j.1745-7262.2006.00179.x.
Garlic and vitamin C may be the best remedy for treating weak errection.
Infertility is a multi-parameter phenomenon with a wide range of
factors that affects spermatogenesis and sperm quality. Spermatogenesis is a process in which male sex cells
are produced and the disorder in each of these stages can cause infertility. Fertility in men depends largely on the number, quality, motility, and morphology of the sperm, and the disruption of each of these factors leads to infertility in men. Infertility, as a psychological
crisis, imposes a lot of stress on infertile couples and in different ways threatens their mental health
Failure to have a child is an unpleasant event in the lives of infertile people. Inability to become pregnant after one
year of regular intercourse, without using contraception, is defined as infertility. About 30%-50% of the causes of infertility are related to male problems. Each day, the number of medical reports about the extent of
infertility in the world increases, according to a systematic review in this regard, about 48.5 million couples around the world affected by this problem.
Fertility in men depends largely
on the number, quality, motility, and morphology of the sperm, and the disruption of each of these factors leads to infertility in men. Infertility, as a psychological crisis, imposes a lot of stress on infertile couples and in
different ways threatens their mental health.
The results in the study by Oi et al
indicated that garlic supplementation boosts LH from the pituitary gland, and this stimulates testosterone secretion
from the testicle. Nonetheless, in the study by Bahrami et al, it was recommended that the cooked garlic has better therapeutic effects and, while affecting the reproduction of the sexual cells in testes and epididymis, improves spermatogenesis. Due to presence of dialyldisulfide in its biochemical
structure, garlic affects the hypothalamic-pituitary axis. Diallyldisulfide stimulates the basophilic cells and secretion of LH sex hormones by affecting the anterior pituitary. LH stimulates Leydig cells in the testes, which in turn is a precursor to secretion and regulation of testosterone. Also, diallyldisulfide reduces oxygen free radicals, enhances and strengthens the blood-testis barrier and increases the circulation in the testicles, thus protects the sexual Organs. By increasing blood flow to the testicles (due to the consumption of garlic), phenol and phenolic glycosides are released which increase the glutathione peroxidase enzyme. The role of this enzyme is to protect sperms in testicular and epididymal tissue. The enzyme protects the sperm from the damage of free radicals by placement in the plasma membrane and the nucleus of sperm, epididymal fluid and epididymis, and leads to ultimate maturation and development of the
sperm.
Combining garlic and vitamin C restores erectile strength.
The combination of vitamin C and garlic was proven to be effective to erectile strength. This may not have been scientifically proven. However, most men who chew garlic and 1g of vitamin C reported restoration of strong errection. To get a better benefit from this combination, It is recommended to take garlic and vitamin C at night after dinner and morning before breakfast for at least a period of three days.
Vitamin C improves blood flow, which results in blood flow reaching to the pelvic regions and thus the urethra. This enhances rigidity of the pennis.
References
Mohammadi F, Nikzad H, Taherian A, Amini Mahabadi J, Salehi M. Effects of herbal medicine on male infertility. Anat Sci J. 2013;10(4):3-16.
Kim SJ, Kim MR, Hwang SY, Bae WJ, Kim S, Hong SH, et al. Preliminary report on the safety of a new herbal formula
and its effect on sperm quality. World J Mens Health. 2013;31(3):254-61. doi: 10.5534/wjmh.2013.31.3.254.
Roozbeh N, Rostami S, Abdi F. A review on herbal medicine with fertility and infertility characteristics in males. Iranian Journal of Obstetrics, Gynecology and Infertility. 2016;19(13):18-32.
Mascarenhas MN, Flaxman SR, Boerma T, Vanderpoel S, Stevens GA. National, regional, and global trends in infertility prevalence since 1990: a systematic analysis of 277 health surveys. PLoS Med.2012; 9(12):e1001356. doi: 10.1371/journal.pmed.1001356.
Bahrami KH, Mahjor AA, Johary H, Bahrami R, Bahrami A. Comparative study on histopatological and
histomorphometric effect of raw and cooked garlic on spermatogenesis in testis and epidydims of rats. J Fasa Univ Med Sci. 2014;3(4):371-9
Ouarda M, Abdennour C. Evaluation of the therapeutic efficiency of raw garlic on reproduction of domestic rabbits
under lead induced toxicity. Ann Biol Res. 2011;2(3):38993
Oi Y, Imafuku M, Shishido C, Kominato Y, Nishimura S, Iwai K. Garlic supplementation increases testicular testosterone and decreases plasma corticosterone in rats fed a high protein diet. J Nutr. 2001;131(8):2150-6. doi: 10.1093/jn/131.8.2150
Pal R, Vaiphei K, Sikander A, Singh K, Rana SV. Effect of garlic on isoniazid and rifampicin-induced hepatic injury in rats. World J Gastroenterol. 2006;12(4):636-9.
Amin A, Hamza AA. Effects of Roselle and Ginger on cisplatin-induced reproductive toxicity in rats. Asian J Androl. 2006;8(5):607-12. doi: 10.1111/j.1745-7262.2006.00179.x.
Thursday, 21 March 2019
Wednesday, 20 March 2019
Hepatitis B virus as a risk factor for gastric cancer
Gastric cancer (GC) is one of the most common malignant diseases in the digestive system, contributing to ∼10% of annual deaths from cancer. Although the incidence of GC has been declined for several decades, it is still the fourth most common cancer in men and fifth in women. Several risk factors have been explored. The most thoroughly investigated and commonly recognised factor is the infection of
Helicobacter pylori (Hp).
The prevalence of hepatitis B virus (HBV) infection varies largely worldwide. The relatively high prevalence areas are located in some developing countries, including China.
Hepatitis B virus is considered to be a hepatotrophic virus, and it has long been confirmed to be the most important risk factor for hepatocellular carcinoma. However, several studies have probed the existence of HBV in some extrahepatic organs and tissues, such as the kidneys, skin, lymph nodes, bone marrow, vessel walls, colon, pancreas as well as stomach.
In a study by Chen et al (2004 ), the coexistence of Hepatitis B surface antigen (HBsAg) and hepatitis B core antigen (HBcAg) with Hp immunoglobulin G antigen in gastric antrum mucosa was observed in patients with chronic HBV infection or HBV-related cirrhosis. In addition, they found that there was no difference in the rates of HBV antigen expression between the Hp- positive and -negative patients. It was also found that patients with liver cirrhosis had a high prevalence of gastric ulcers and an increased risk of GC. Besides, the impact of Hp on gastric ulcers in patients with liver cirrhosis was found to be relatively weak. It is well known that HBV infection is the most important risk factor for liver cirrhosis in China. We therefore speculate that HBV infection may play a role in the risk of GC in China, as China is an endemic region for both GC and HBV infection. However, the markers of either past or present HBV infection could possibly be also frequently detectable in patients with GC. The relation between HBV infection and GC might be a casual association.
HBV infection has been confirmed to be a risk factor for several cancers of other organs and tissues involved in HBV infection. Hepatocellular carcinoma is well known as one of the HBV-related cancers. As HBV infection also exists in gastric mucosa epithelial cells, it may be possible that HBV infection increases the risk of GC in a similar mechanism of HBV-related hepatocellular carcinoma. The HBV infection has been commonly recognised as a risk factor for hepatocellular carcinoma.
The mechanism of HBV-induced hepatocellular carcinoma has been thoroughly researched, and it is complex, including direct enhancement of chromosomal instability by integration of HBV DNA into the host genome that results in alterations of host gene expression and signalling pathways. Indirect mechanisms, such as persistent inflammation, oxidative stress, hypoxia caused by cirrhosis and sequential angiogenesis, are also raised up. Recently, the epigenetic changes generated by the HBV-encoded X (HBx) protein became another focus in the exploration for mechanism of HBV-induced hepatocellular carcinoma. However, to understand the authentic and detailed mechanism of HBV infection-related GC, more studies should be conducted.
Journal References
Dehesa-Violante M, Nunez-Nateras R (2007) Epidemiology of hepatitis virus B and C. Arch Med Res 38 : 606–611.
Dejean A, Lugassy C, Zafrani S, Tiollais P,
Brechot C (1984) Detection of hepatitis B virus DNA in pancreas, kidney and skin of two human carriers of the virus. J Gen Virol 65 (Pt 3): 651–655.
Lu FM, Li T, Liu S, Zhuang H (2010)
Epidemiology and prevention of hepatitis B virus infection in China. J Viral Hepat
17(Suppl 1): 4–9.
Tan YJ (2011) Hepatitis B virus infection and the risk of hepatocellular carcinoma.
World J Gastroenterol 17: 4853–4857.
Arzumanyan A, Reis HM, Feitelson MA (2013) Pathogenic mechanisms in HBV- and HCV-associated hepatocellular carcinoma. Nat Rev Cancer 13 : 123–135.
Wei, et al.,( 2015) Hepatitis B virus infection is associated with gastric cancer in China: an endemic area of both diseases. British Journal of cancer. 112:1283-1290
Chen NL, Bai L, Deng T, Zhang C, Kong QY, Chen H (2004) Expression of hepatitis B virus antigen and Helicobacter pylori infection in gastric mucosa of patients with chronic liver disease. Hepatobiliary Pancreat Dis Int 3 : 223–225.
Gastric cancer (GC) is one of the most common malignant diseases in the digestive system, contributing to ∼10% of annual deaths from cancer. Although the incidence of GC has been declined for several decades, it is still the fourth most common cancer in men and fifth in women. Several risk factors have been explored. The most thoroughly investigated and commonly recognised factor is the infection of
Helicobacter pylori (Hp).
The prevalence of hepatitis B virus (HBV) infection varies largely worldwide. The relatively high prevalence areas are located in some developing countries, including China.
Hepatitis B virus is considered to be a hepatotrophic virus, and it has long been confirmed to be the most important risk factor for hepatocellular carcinoma. However, several studies have probed the existence of HBV in some extrahepatic organs and tissues, such as the kidneys, skin, lymph nodes, bone marrow, vessel walls, colon, pancreas as well as stomach.
In a study by Chen et al (2004 ), the coexistence of Hepatitis B surface antigen (HBsAg) and hepatitis B core antigen (HBcAg) with Hp immunoglobulin G antigen in gastric antrum mucosa was observed in patients with chronic HBV infection or HBV-related cirrhosis. In addition, they found that there was no difference in the rates of HBV antigen expression between the Hp- positive and -negative patients. It was also found that patients with liver cirrhosis had a high prevalence of gastric ulcers and an increased risk of GC. Besides, the impact of Hp on gastric ulcers in patients with liver cirrhosis was found to be relatively weak. It is well known that HBV infection is the most important risk factor for liver cirrhosis in China. We therefore speculate that HBV infection may play a role in the risk of GC in China, as China is an endemic region for both GC and HBV infection. However, the markers of either past or present HBV infection could possibly be also frequently detectable in patients with GC. The relation between HBV infection and GC might be a casual association.
HBV infection has been confirmed to be a risk factor for several cancers of other organs and tissues involved in HBV infection. Hepatocellular carcinoma is well known as one of the HBV-related cancers. As HBV infection also exists in gastric mucosa epithelial cells, it may be possible that HBV infection increases the risk of GC in a similar mechanism of HBV-related hepatocellular carcinoma. The HBV infection has been commonly recognised as a risk factor for hepatocellular carcinoma.
The mechanism of HBV-induced hepatocellular carcinoma has been thoroughly researched, and it is complex, including direct enhancement of chromosomal instability by integration of HBV DNA into the host genome that results in alterations of host gene expression and signalling pathways. Indirect mechanisms, such as persistent inflammation, oxidative stress, hypoxia caused by cirrhosis and sequential angiogenesis, are also raised up. Recently, the epigenetic changes generated by the HBV-encoded X (HBx) protein became another focus in the exploration for mechanism of HBV-induced hepatocellular carcinoma. However, to understand the authentic and detailed mechanism of HBV infection-related GC, more studies should be conducted.
Journal References
Dehesa-Violante M, Nunez-Nateras R (2007) Epidemiology of hepatitis virus B and C. Arch Med Res 38 : 606–611.
Dejean A, Lugassy C, Zafrani S, Tiollais P,
Brechot C (1984) Detection of hepatitis B virus DNA in pancreas, kidney and skin of two human carriers of the virus. J Gen Virol 65 (Pt 3): 651–655.
Lu FM, Li T, Liu S, Zhuang H (2010)
Epidemiology and prevention of hepatitis B virus infection in China. J Viral Hepat
17(Suppl 1): 4–9.
Tan YJ (2011) Hepatitis B virus infection and the risk of hepatocellular carcinoma.
World J Gastroenterol 17: 4853–4857.
Arzumanyan A, Reis HM, Feitelson MA (2013) Pathogenic mechanisms in HBV- and HCV-associated hepatocellular carcinoma. Nat Rev Cancer 13 : 123–135.
Wei, et al.,( 2015) Hepatitis B virus infection is associated with gastric cancer in China: an endemic area of both diseases. British Journal of cancer. 112:1283-1290
Chen NL, Bai L, Deng T, Zhang C, Kong QY, Chen H (2004) Expression of hepatitis B virus antigen and Helicobacter pylori infection in gastric mucosa of patients with chronic liver disease. Hepatobiliary Pancreat Dis Int 3 : 223–225.
Monday, 25 September 2017
HBVx could be a drug target for HBV induced hepatocellular carcinoma.
Hepatitis B Virus X
Protein: A Key Regulator of the Virus Life Cycle
Hepatitis B
virus (HBV) infection is the main risk factor for hepatocellular carcinoma
(HCC) worldwide. Epidemiologic studies have shown that individuals who are
chronic HBV carriers have a greater than 100-fold increase in the risk of
developing liver cancer. The HBV genome is a partially double-stranded,
circular DNA containing four overlapping genes: S/preS, C/preC, P, and X. The X
gene encodes a 17-kd HBV X protein (HBx), which is a multifunctional
transactivator of both viral and cellular genes. It is widely accepted that HBx
plays crucial roles in the pathogenesis of HBV-induced HCC. HBV belongs to the
family hepadnaviridae. It is a
small, enveloped DNA virus that replicates via reverse transcription of an RNA
intermediate. HBV virions, also called Dane particles, are spherical
lipid-containing structures with a diameter of ~42 nm. The inner shell of the
virus consists of an icosahedral capsid, which is assembled from 180 or 240 subunits
of the core protein. The capsid is covered by a lipid bilayer membrane densely
packed with the three envelope proteins, large (L), middle (M), and
predominantly small (S) protein, and is acquired by budding into the
endoplasmic reticulum. They are translated from individual start codons but
share the open reading frame and the same C-terminal amino acids, called the S
domain. As a consequence, the M protein shares the S and has an extra
N-terminal domain called preS2, and the L protein encompasses the S and two
extra domains: preS2 and preS1. Capsids contain a single copy of the HBV genome
consisting of a 3.2-kb partially double-stranded relaxed circular (rc) DNA
molecule. The viral polymerase serves as a protein primer and remains
covalently linked to the 5’ end of the complete strand, also called viral (–)
strand DNA of the rcDNA after reverse transcription. Besides virions, HBV infection
leads to secretion of huge amounts of subviral particles, which consist of
empty viral envelopes with filamentous or spherical shapes containing mainly S
and little L protein. Subviral particles are the most abundant HBV structures
released into the blood stream, are commonly defined as hepatitis B surface
(HBs) antigen and are thought to facilitate virus spread and persistence in the
host by adsorbing virus-neutralizing antibodies and tolerizing T cell
responses. In addition to polymerase and the structural proteins, the HBV
genome also encodes for two non-structural proteins, which have less
well-defined functions.
Life cycle of
HBV
HBV
infection is restricted to hepatocytes. HBV entry into these cells is thought
to be a multistep process. Virions are first trapped at the surface of the cell
by heparan sulfate proteoglycans and then bind to a receptor allowing uptake
into the cells via an endocytosis process. So far, this cellular receptor has
not been identified. Proteolytic cleavage of the surface protein occurs within
the endosomal compartment, probably resulting in a conformational change that
exposes some translocation motifs at the surface of the viral particle allowing
fusion of viral and cellular membranes and release of the capsid into the
cytosol. The
naked capsid is then directed towards the nucleus, and the HBV genome is
translocated to the nucleus. In the nucleus,
the rcDNA genome is converted by cellular enzymes
into a covalently closed circular DNA (cccDNA), the episomal persistance form
of the virus serving as transcription
template. The 3.5 kb RNA species serves as pregenomic RNA (pgRNA) and as messenger
RNAs for the synthesis of polymerase and core proteins as well as HBeAg. The
2.1 and 2.4 kb subgenomic RNAs encode for the three viral envelope proteins, a
small 0.7 kb RNA for the HBx. The pgRNA is exported in an unspliced form, encapsidated
together with the viral polymerase and used as a template for reverse transcription. The capsid spontaneously
self-assembles from core dimers present in the cytoplasm due to the nucleic
acid-binding domain of the core protein. Specific packaging of pgRNA into the
capsid is mediated by binding of the primer region of the viral polymerase to
the stem-loop in the 5’ region of
pgRNA. The pgRNA is then reverse transcribed by the reverse transcriptase
domain of the polymerase within the capsid in the cytoplasm of the infected
cell. Upon minus and then plus strand DNA synthesis the capsid matures and can
be enveloped or reimported into the nucleus to fill up a cccDNA pool.
General features
and functions of HBVx
HBx is
translated from a small subgenomic RNA controlled by the HBx promoter.
Alternatively, HBx may be produced form a very long RNA (3.9 kb) containing all
the HBV open reading frames (ORF). The ORF was originally designated X because
of the lack of homology with known sequences. HBx is a protein composed of 154 amino
acid residues with a molecular mass of around 17.5 kDa.
HBx selectively
promotes degradation of Smc5/6 via an E3-ubiquitin ligase pathwaw by hijacking the
DDB1–E3 ligase to target Smc5/6 for degradation. Smc5/6
is a complex that directly binds DNA and is required for chromosome dynamics
and stability. Smc5/6 play a role in homologous recombination as well as in
resolving replication-induced DNA supercoiling. In addition, a recent study
demonstrated that Smc5/6 binds and topologically entraps plasmid DNA in an
ATP-dependent manner. Smc5/6 binds episomes (including cccDNA) and blocks
episome transcription.
REFERENCES
Michielsen P, Ho E. Viral hepatitis B
and hepatocellular carcinoma. Acta Gastroenterol Belg 2011;74:4–8.
Henkler FF, Koshy R. Hepatitis B virus
transcriptional activators: mechanisms and possible role in oncogenesis. J
Viral Hepat 1996;3:109–21.
Tang H, Oishi N, Kaneko S, Murakami S.
Molecular functions and biological roles of hepatitis B virus x protein. Cancer
Sci 2006;97: 977–83.
Motavaf M, Safari S, Saffari JM, Alavian
SM. Hepatitis B virus-induced hepatocellular carcinoma: the role of the virus x
protein. Acta Virol 2013;57:389–96
Bertoletti, A. & Gehring, A. J.
(2006). The immune response during hepatitis B virus infection. J Gen Virol 87,
1439-1449.
Chen, M., Sallberg, M., Hughes, J.,
Jones, J., Guidotti, L. G., Chisari, F. V., Billaud, J. N. & Milich, D. R.
(2005). Immune tolerance split between hepatitis B virus precore and core
proteins. J Virol 79, 3016-3027.
Chen, M. T., Billaud, J. N., Sallberg,
M., Guidotti, L. G., Chisari, F. V., Jones, J., Hughes, J. & Milich, D. R.
(2004). A function of the hepatitis B virus precore protein is to regulate the
immune response to the core antigen. Proc Natl Acad Sci U S A 101, 14913-14918.
Visvanathan, K., Skinner, N. A.,
Thompson, A. J., Riordan, S. M., Sozzi, V., Edwards, R., Rodgers, S., Kurtovic,
J., Chang, J., Lewin, S., Desmond, P. & Locarnini, S. (2007). Regulation of
Toll-like receptor-2 expression in chronic hepatitis B by the precore protein.
Hepatology 45, 102-110.
Schulze, A., Gripon, P. & Urban, S.
(2007). Hepatitis B virus infection initiates with a large surface
protein-dependent binding to heparan sulfate proteoglycans. Hepatology 46,
1759-1768.
Stoeckl, L., Funk, A., Kopitzki, A.,
Brandenburg, B., Oess, S., Will, H., Sirma, H. & Hildt, E. (2006).
Identification of a structural motif crucial for infectivity of hepatitis B viruses.
Proc Natl Acad Sci U S A 103, 6730-6734.
Kott, N., König, A., Glebe, D. (2010).
Hepatitis B virus (HBV) bypasses classical endocytic pathways to infect primary
hepatocytes in vitro. Journal of Hepatology 52, S48-S49.
Leistner, C. M., Gruen-Bernhard, S.
& Glebe, D. (2008). Role of glycosaminoglycans for binding and infection of
hepatitis B virus. Cell Microbiol 10, 122-133.
Rabe, B., Glebe, D. & Kann, M.
(2006). Lipid-mediated introduction of hepatitis B virus capsids into
nonsusceptible cells allows highly efficient replication and facilitates the
study of early infection events. J Virol 80, 5465-5473.
Zlotnick, A., Johnson, J. M., Wingfield,
P. W., Stahl, S. J. & Endres, D. (1999). A theoretical model successfully
identifies features of hepatitis B virus capsid assembly. Biochemistry 38,
14644-14652.
Hirsch, R. C., Lavine, J. E., Chang, L.
J., Varmus, H. E. & Ganem, D. (1990). Polymerase gene products of hepatitis
B viruses are required for genomic RNA packaging as wel as for reverse
transcription. Nature 344, 552-555.
Junker-Niepmann, M., Bartenschlager, R.
& Schaller, H. (1990). A short cis-acting sequence is required for
hepatitis B virus pregenome encapsidation and sufficient for packaging of
foreign RNA. EMBO J 9, 3389-3396.
Knaus, T. & Nassal, M. (1993). The
encapsidation signal on the hepatitis B virus RNA pregenome forms a stem-loop
structure that is critical for its function. Nucleic Acids Res 21, 3967-3975.
Nassal, M. (1992). The arginine-rich
domain of the hepatitis B virus core protein is required for pregenome
encapsidation and productive viral positive-strand DNA synthesis but not for
virus assembly. J Virol 66, 4107-4116.
Porterfield, J. Z., Dhason, M. S., Loeb,
D. D., Nassal, M., Stray, S. J. & Zlotnick, A. (2010). Full-length
hepatitis B virus core protein packages viral and heterologous RNA with
similarly high levels of cooperativity. J Virol 84, 7174-7184.
Doitsh, G. & Shaul, Y. (2003). A
long HBV transcript encoding pX is inefficiently exported from the nucleus.
Virology 309, 339-349.
Guo, W. T., Wang, J., Tam, G., Yen, T.
S. & Ou, J. S. (1991). Leaky transcription termination produces larger and
smaller than genome size hepatitis B virus X gene transcripts. Virology 181,
630-636.
BIOMET RESOURCES: Eukaryotic Translation Initiation Factor 3b is bot...
BIOMET RESOURCES: Eukaryotic Translation Initiation Factor 3b is bot...: Eukaryotic Translation Initiation Factor 3b is both a Promising Prognostic Biomarker and a Potential Therapeutic Target for Patients with...
Saturday, 16 September 2017
FLAVONOIDS AND THEIR HEALTH BENEFITS
FLAVONOIDS AND THEIR HEALTH BENEFITS
Flavonoids are low molecular weight bioactive polyphenols
which play a vital role in photosynthesising cells. They are a large family of
over 5,000 hydroxylated polyphenolic compounds that carry out important
functions in plants. The original "flavonoid" research apparently
began in 1936, when Hungarian scientist Albert Szent-Gyorgi was uncovering a
synergy between pure vitamin C and as yet unidentified co-factors from the
peels of lemons, which he first called "citrin," and, later,
"vitamin P". Flavonoids are secondary metabolites characterised by
flavan nucleus and C6-C8-C6 carbon-skeleton. These are group of structurally
related compounds with a chromane-type skeleton having phenyl substituent in
C2-C3 position. The basic structural feature of flavonoid is
2-phenyl-benzo-γ-pyrane nucleus consisting of two benzene rings (A and B)
linked through a heterocyclic pyran ring (C) as shown in fig (I).
Flavonoids are one of the largest groups of secondary metabolites and widely
distributed in leaves, seeds, bark and flowers
of plants with more than 4000 different structures which are classified according to their chemical structures
as follows; flavones, flavonols, flavanones, dihydroflavonols,
isoflavones, anthocyanins, catechins and calchones. Flavonoids which are part of human diet are thought to have positive
effects on human health such as reducing risk
of cardiovascular diseases and cancer. Most of the beneficial effects of
flavonoids are attributed to their antioxidant
and chelating abilities. Flavonoids are structurally related compounds with a chromane-type skeleton with a
phenyl substituent in the C2 or C3 position .
They are consisting of phenylpropane (C6-C3) unit derived from shikimic acid pathway and C6 unit derived from
polyketide pathway biosynthetically.
Chemical structure of Flavonoids
Figure 1: diphenylpropane, a basic structure of flavonoids
Chemically flavonoids are based upon a fifteen-carbon
skeleton consisting of two benzene rings (A and B as shown in Figure 1) linked
via a heterocyclic pyrane ring (C). They can be divided into a variety of
classes such as flavones (e.g., flavone, apigenin, and luteolin), flavonols
(e.g.,
quercetin, kaempferol, myricetin, and fisetin), flavanones
(e.g., flavanone, hesperetin, and naringenin), and others. Their general
structures are shown in Table 1. The various classes of flavonoidsdiffer in the
level of oxidationandpattern of substitution of the C ring, while individual
compounds within a class differ in the pattern of substitution of the A and B
rings.
Flavonoids occur as aglycones, glycosides, and methylated
derivatives. The basic flavonoid structure is aglycone (Figure 1). Six-member
ring condensed with the benzene ring is either a 𝛼-pyrone (flavonols and flavanones) or its dihydroderivative
(flavonols and flavanones). The position of the benzenoid substituent divides
the flavonoid class into flavonoids (2-position) and isoflavonoids
(3-position). Flavonols differ from flavanones by hydroxyl group at the 3-
position and a C2–C3 double bond. Flavonoids are often hydroxylatedinpositions
3, 5, 7, 2, 3, 4, and5.Methyl ethers and acetyl esters of the alcohol group are
known to occur in nature. When glycosides are formed, the glycosidic linkage is
normally located in positions 3 or 7 and the carbohydrate can be L-rhamnose,
D-glucose, glucorhamnose, galactose, or arabinose.
Classes of flavonoids
Flavonoids are
classified into eight classes based on differences in their arrangement of
hydroxyl, methoxy and glycosidic side groups and in the conjuction between A
and B rings. A variation in C ring provides division of subclasses. According
to their molecular structure, they are divided into eight classes, namely:
Flavone, Flavonones, Flavonol, Isoflavone , Anthocyanidin, Catechin,
Dihydroflavonol and Chalcone.
Metabolism of flavonoids
The absorption of the dietary flavonoids liberated from the
food by chewing will depend on its physicochemical properties such as molecular
size, configuration, lipophilicity, solubility, and pKa. The flavonoid can be
absorbed from the small intestine or has to go to the colon before absorption.
It may depend upon structure of flavonoid, that is, whether it is glycoside or
aglycone. Most flavonoids, except for the subclass of catechins, are present in
plants bound to sugars as b-glycosides. Aglycans can be easily absorbed
by the small intestine, while flavonoid glycosides have to be converted into aglycan
form. The hydrophilic flavonoid glucoside such as quercetin are transported
across the small intestine by the intestinal
Na+-dependent glucose cotransporter (SGLT1). An alternative
mechanism suggests that flavonoid glucosides are hydrolyzed by lactase
phloridzin hydrolase (LPH), a 𝛽-glucosidase on the outside of the brush bordermembrane of
the small intestine. Subsequently, the liberated aglycone can be absorbed
across the small intestine. The substrate specificity of this LPH enzyme varies
significantly in a broad range of glycosides (glucosides, galactosides,
arabinosides, xylosides, and rhamnosides) of flavonoids. The glycosides which
are not substrates for these enzymes are transported toward the colon where
bacteria have ability to hydrolyze flavonoid glycosides, but simultaneously
they will also degrade the liberated flavonoid aglycones . Since absorption
capacity of the colon is far less than that of the small intestine, only
trivial absorption of these glycosides is to be expected. After absorption, the
flavonoids are conjugated in the liver by glucuronidation, sulfation, or
methylation or metabolized to smaller phenolic compounds. Due to these
conjugation reactions, no free flavonoid aglycones can be found in plasma or urine,
except for catechins. Depending on the food source bioavailability of certain
flavonoids differs markedly; for example, the absorption of quercetinfrom
onions is fourfold greater than that from apple or tea. The flavonoids secreted
with bile in intestine and those that cannot be absorbed fromthe small
intestine are degraded in the colon by intestinal microflora which also break
down the flavonoid ring structure (Figure 3). Oligomeric flavonoids may be
hydrolyzed tomonomers and dimers under influence of acidic conditions in the
stomach. Larger molecules reach the colon where they are degraded by bacteria.
The sugar moiety of flavonoid glycosides is an important determinant of their
bioavailability. Dimerization has been shown to reduce bioavailability. Among
all the subclasses of flavonoids, isoflavones exhibit the highest
bioavailability. After ingestion of green tea, flavonoid content is absorbed
rapidly as shown by their elevated levels in plasma and urine. They enter the
systemic circulation soon after ingestion and cause a significant increase in
plasma antioxidant status.
Health benefits of Flavonoids
Flavonoids
act as antioxidants by suppressing reactive oxygen specie (ROS) formation
either by inhibition of enzymes or by chelating trace elements involved in free
radical generation. Flavonoids inhibits the enzymes involved in ROS generation,
that is, microsomal monooxigenase, glutathione s-transferase, mitochondrial succinoxidase,
NADH oxidase etc. they also inhibits lipid peroxidation. Other health benefits
of flavonoids include, anti-inflammation, antibacterial, anticancer antiviral.
Eukaryotic Translation Initiation Factor 3b is both a Promising Prognostic Biomarker and a Potential Therapeutic Target for Patients with Clear Cell Renal Cell Carcinoma
Eukaryotic Translation Initiation Factor 3b is both a
Promising Prognostic Biomarker and a Potential Therapeutic Target for Patients
with Clear Cell Renal Cell Carcinoma
Eukaryotic
initiation factor 3b (el3b) is an RNA-binding component of the eukaryotic
translation initiation factor 3 (eif-3) complex, which is required for several
steps in the initiation of protein synthesis. The elf-3 complex associates with
the 40s ribosome and facilitates the recruitment of elf-1, elf-1A,
elf-2:GTP:methionyl-tRNAi and elf-5 to form the 43s pre-initiation complex (43S
PIC). The elf-3 complex is also required for disassembly and recycling of
post-termination ribosomal complexes and subsequently prevents premature
joining of the 40S and 60S ribosomal subunits prior to initiation. The elf-3
complex specifically targets and initiates translation of a subset of mRNAs
involved in cell proliferation, including cell cycling, differentiation and
apoptosis, and uses different modes of RNA stem-loop binding to exert either
translational activation or repression. Studies
showed that cell proliferation
was significantly inhibited after eIF3b Knockdown. Additionally, cell colony numbers fell after eIF3b depletion. Furthermore, migration capacity
was significantly impaired after eIF3b knockdown. EIF3b depletion reduced the number of cells traversing the membrane.
Therefore, eIF3b depletion impaired both cell migration and invasion. Notably, eIF3b
depletion caused the
cells to become smaller and rounded, suggesting that both migration and adhesion were impaired compared with control cells. In a study conducted to explore the effects of eIF3b depletion on
the cell
cycle, the proportion of cells in S-phase was
lower in eIF3b-depleted cells and the proportion in the G1 phase was higher than that in the negative control. Western blotting showed that the G1/S arrest was caused by
eIF3b depletion.
During the G1/S transition, cyclins D and E combine with cyclin-dependent kinases (CDK) to form the cyclin/CDK
complexes required
for the transition. The complexes phosphorylate the retinoblastoma protein (Rb), releasing the E2F transcription factor that
activates expression
of G1/S progression genes. It was found that the levels of both cyclins D and E
decreased after eIF3b knockdown. Cyclins D and E, Rb, and the inactivated form
of Rb (p-Rb) were downregulated after eIF3b knockdown. In addition, the levels
of p27Kip1 and p21 Cip1, inhibitors of the cyclin/CDK complexes, significantly
increased after eIF3b knockdown. Interestingly, Western blotting of G2/M-related
proteins indicated that the G2/M transition was also inhibited after eIF3b
knockdown Cyclin A, which accumulates steadily during the G2 phase and is
abruptly destroyed at mitosis, was upregulated after eIF3b depletion. Cyclin B
is required for the G2/M transition; we found that the cyclin B level fell.
Also, the levels of Myt1 and Wee1 increased after eIF3b depletion; these
proteins inhibit cell entry into mitosis. The observed decrease in histone H3
phosphorylation indicated that chromosome condensation was reduced by eIF3b depletion;
fewer cells were in the mitotic phase. The levels of apoptosis increased
slightly after eIF3b depletion. Further analysis showed that, after eIF3b
knockdown, the pro-apoptotic factors Bax, caspase-3, and the activated form
thereof (cleaved caspase-3) were all upregulated and the pro-survival factor
Bcl-2 was downregulated. More importantly, cleavage of
poly-ADP-ribosepolymerase (c-PARP), a marker of apoptosis, was also increased.
Therefore, apoptosis increased after eIF3b knockdown. However, interestingly,
knockdown reduced the level of cleaved caspase-12, which is required for
endoplasmic reticulum-stress-induced apoptosis. The EMT is a key event in tumor
invasion and metastasis, including RCC. It was found that the epithelial marker
E-cadherin was upregulated and the levels of repressors thereof (Slug and
Snail) were downregulated after eIF3b depletion. Additionally, the mesenchymal
markers N-cadherin and vimentin were downregulated. Therefore, the EMT was inhibited
by eIF3b depletion (Figure 5A). The β-catenin pathway is involved in regulation
of the EMT. It was found that β-catenin expression was significantly
downregulated after eIF3b depletion. The level of cyclin D1, a target of
β-catenin, was also downregulated after eIF3b depletion. Together, our data
showed that eIF3b depletion inactivated the β-catenin pathway and inhibited the
EMT of ccRCC. The serine/threonine kinase Akt (also termed protein kinase B or
PKB) has attracted a great deal of attention because Akt plays critical roles
in the regulation of many cellular functions including metabolism, growth,
proliferation, survival, transcription, and protein synthesis. Studies found that
eIF3b depletion was not associated with any significant change in Akt levels;
however, the level of the activated form, p-Akt, fell in parallel with the extent
of eIF3b depletion, indicating that the Akt signaling pathway was involved in
such depletion. The significant morphological changes in cells after eIF3b
depletion suggested that the integrin pathway might be affected; integrin links
the extracellular matrix to the intracellular cytoskeleton to facilitate focal
adhesion. After eIF3b knockdown, studies showed that the levels of integrins α2
and α5 fell significantly, as did the level of the upstream phosphorylated
Focal adhesion kinase (p-FAK) protein, suggesting that integrin/FAK/Akt
signaling was inhibited Akt plays a critical role in cell growth by directly phosphorylating
the mechanistic target of rapamycin (mTOR). Studies has shown that p-mTOR was downregulated
after eIF3b knockdown, indicating that the Akt/mTOR pathway was impaired.
Furthermore, the observed downregulation of HIF-1α, HIF-2α, and p-NF-κB after
eIF3b depletion may indicate that the Akt/mTOR/HIF and Akt/mTOR/NF-κB pathways
were also downregulated, compromising cell proliferation and inducing apoptosis.
Akt promotes cell survival by inhibiting apoptosis via phosphorylation
(inactivation) of several proteins, including Bcl-2 and Bax. Apart from the
roles played in survival and apoptosis, the Akt pathway is also involved in
cell cycle regulation, preventing GSK-3β-mediated phosphorylation and degradation
of cyclin D1 and negatively regulating the actions of p27 Kip1 and p21 Waf1/Cip1. Research showed that
GSk-3β and cyclin D1 were upregulated and p27 Kip1 and p21. Cip1 were
downregulated after eIF3b depletion indicating
that the Akt/GSK-3β pathway was involved in cell cycle regulation of A498 and
CAKI-2 cells.
Clear cell renal cell carcinoma (CCRCC) is a renal cortical tumor
typically characterized by malignant epithelial cells with clear cytoplasm and
a compactalveolar (nested) or acinar growth pattern interspersed with
intricate, arborizing vasculature. A variable proportion of cells with granulareosinophilic
cytoplasm may be present. CCRCC is characterized genetically by alterations to
chromosome 3p. CCRCC is proposed to arise from epithelial cellsof the proximal
convoluted tubules of the nephron, within the renal cortex. Extension into the
renal sinus is the most common pathway of spread for most histologic types of
RCC because no connective tissue separates thecortical columns of Bertin from
the abundant lymphatics and vasculature within the sinus fat. Elf-3b will
therefore be a good target for pharmacological response against CCRCC.
REFERENCES
Yuanwei Z., Xiang Z., Lei Y., Gangli G., Dawei L., Yongzhen Z.,
Liang F., Shanshan
F.,
Juchao R
and Zhonghua X. ( 2017).
Eukaryotic
translation initiation factor 3b is both a promising prognostic biomarker and a
potential therapeutic target for patients with clear cell renal cell carcinoma
. Journal of cancer. 8(15): 3049-3061.
He H and Magi-Galluzzi C. Epithelial-to-mesenchymal transition in
renal neoplasms. Adv Anat Pathol 2014; 21: 174-180.
Wang
DX, Zou YJ, Zhuang XB, Chen SX, Lin Y, Li WL, Lin JJ and Lin ZQ. Sulforaphane
suppresses EMT and metastasis in human lung cancer through miR-616-5p-mediated
GSK3beta/beta-catenin signaling pathways. Acta Pharmacol Sin 2016;
Chen
X, Zhang L, Zheng S, Zhang T, Li M, Zhang X, Zeng Z, McCrae MA, Zhao J, Zhuang
H and Lu F. Hepatitis B Virus X Protein Stabilizes Cyclin D1 and Increases
Cyclin D1 Nuclear Accumulation through ERK-Mediated Inactivation of GSK-3beta.
Cancer Prev Res (Phila) 2015; 8: 455-463.
Gesbert F, Sellers WR,
Signoretti S, Loda M and Griffin JD. BCR/ABL
regulates
expression of the cyclin-dependent kinase inhibitor p27Kip1 through
the
phosphatidylinositol 3-Kinase/AKT pathway. J Biol Chem 2000; 275:
39223-39230.
Zhou BP, Liao Y, Xia W, Spohn B, Lee MH and Hung MC. Cytoplasmic
localization of p21Cip1/WAF1 by Akt-induced phosphorylation in
HER-2/neu-overexpressing cells. Nat Cell Biol 2001; 3: 245-252.
Lee KB, Byun HJ, Park SH, Park CY, Lee SH and Rho SB. CYR61
controls p53
and
NF-kappaB expression through PI3K/Akt/mTOR pathways in carboplatin-induced
ovarian cancer cells. Cancer Lett 2012; 315: 86-95.
Shafee N, Kaluz S, Ru N and Stanbridge EJ. PI3K/Akt activity has
variable cell-specific effects on expression of HIF target genes, CA9 and VEGF,
in human cancer cell lines. Cancer Lett 2009; 282: 109-115.
Schwartz MA. Integrin signaling revisited. Trends Cell Biol 2001;
11: 466-470.
Yamada Y, Kohashi K, Fushimi F, Takahashi Y, Setsu N, Endo M,
Yamamoto H, Tokunaga S, Iwamoto Y and Oda Y. Activation of the Akt-mTOR pathway
and receptor tyrosine kinase in patients with solitary fibrous tumors. Cancer
2014; 120: 864-876.
Subscribe to:
Comments (Atom)