Varicella ( Human Herpes Virus-3 ) Vaccine Potential Role Against Herpes ( HSV-1 / HSV-2 ) Viruses to Prevent HIV-1 Pandemic in Sub-Saharan Africa

SYSTEMATIC REVIEW Varicella (Human Herpes Virus-3) Vaccine Potential Role Against Herpes (HSV-1/HSV-2) Viruses to Prevent HIV-1 Pandemic in SubSaharan Africa Jacqueline Le Goaster, Patrice Bourée, Franck N. El Sissy, Johanna Pokossy Epee, Frédéric Tangy, Anne-Lise Haenni and Allan Goldstein Department of Tropical Diseases, Hôtel-Dieu, University Paris V, Paris, France Viral Genomics, Vaccinations, CNRS, Pasteur Institute, Paris, France Jacques Monod Institute, CNRS, University Paris VII, Paris, France Department Biochemistry and Molecular Medicine, The George Washington University, Washington, DC 20037, USA


INTRODUCTION
For more than a century, unexplained cancers such as Hodgkin lymphomas and Kaposi sarcoma have occurred in Subtropical Africa (Fig. 1).Fig. (1).Correlation between Kaposi's sarcoma and Bantu ethnies in subtropical Africa.
Location of Bantu populations.
Sites of medical centers, in tropical Africa .Chimpanzee observatories .
In 1981 in San Francisco, this same type of tumors was related to unidentified viral infections; in 1983, HIV-1 was identified as being at the origin of AIDS cancer pandemic.Later in 2000, it was discovered that herpes viruses have a pathogenic power at the origin of tumors such as Hodgkin lymphomas, Kaposi sarcomas, etc.
It was established that these herpes viruses play a key role related to HIV-1 infections [1].
The human herpes simplex viruses HSV-1/HSV-2 and the varicella zoster virus HHV-3 are members of the subfamily Alphaherpesvirinae following the morphological order of herpes viruses distinct from all other viruses [2].(Fig. 2).Fig. (2).Phylogenetic tree of the members of the Herpesviridae family [2].
Infections caused by HSV-1 or HSV-2 result of cell-to-cell transmission, involve cell-mediated immunity [4].The HHV-3/HSV-1/HSV-2 viruses must have a close relationship, that has however been sparsely explored by researchers in fundamental virology [5,6]."Varicella is a common and very infectious disease in children" caused by VZV, known as varicella zoster virus (HHV-3) [7]."The causative agent of varicella is one of the eight herpes viruses that include humans as natural hosts."The Varicella Zoster Virus exhibits a low genomic diversity relatively to other studied herpesviruses" [8].
The varicella zoster virus (VZV/HHV-3) can be considered as a primordial event with a specific immunogenic Human Leucocyte Antigen (HLA) as a final result.
It is speculated that a varicella virus (HHV-3) immune defect could originate HSV-1/HSV-2 recurrent herpes diseases which can be cured by varicella vaccine.Since 2005, based on this hypothesis, the varicella vaccine is used against herpes viruses, it has been efficient.It is possible to acquire positive long-term clinical results as it has been observed [9].There have been no relapses concerning more than 70 patients (10 to 80 years old) so far.
The HSV-1/HSV-2 recurrent herpes diseases play a key role related to HIV-1 infections.The varicella vaccine will be used to cure herpes diseases and it could play a role, first against HSV-1/HSV-2 recurrent herpes diseases, further HIV-1 infections [9].
The first HHV-3 vaccine was the "Oka strain" vaccine, created by Takahashi et al. (1974) [7].The original virus strain was used initially to prevent varicella in high-risk leukemic children who remained free from varicella with safety.
The varicella vaccine is a live attenuated herpes virus vaccine (1,350 UFP), available for children and adults.In the USA, in 1995, varicella vaccination program was decided using: an universal one dose childhood.It became an obligation for all children in 3 states: California, Massachusetts, Pennsylvania.The incidence of Varicella has fallen by 80%.
Studies of geographical variations of the varicella virus (VZV/HHV-3) have been performed.Isolates from Caucasian populations are represented by just one genome sequence.The strain related to the OKA vaccine is constituted by Japanese origin and an incomplete VZV Sub-Saharan African genome sequence [2].
Therefore the OKA varicella vaccine is originated partly from Japan and partly from Sub-Sahara.This underlines the ancient human origin from sub-tropical Africa.This varicella vaccine is used to prevent shingles and zoster in immunodepressed individuals.The varicella vaccine has potential pharmacodynamic properties but these have not been deeply investigated [8].However, recently the efficiency of such anti-VZV vaccine against recurrent HSV-1/HSV-2 infections has been already reported [9].
It appeared essential to increase the efficient HHV-3 (VZV) power to raise the immungenetic ability against recurrent HSV-1/HSV-2 herpes diseases.Then, as it is reported it is possible to prevent recurrent herpes diseases linked to HIV-1 infections [1,9,10].
The effect of the varicella vaccine on recurrent herpes diseases must be attributed to a cell-mediated immune response as it has been reported [9,11].It suggests immunological induction of cell-mediated reactivity between HSV-1/HSV-2 and HHV-3 revealed by a specific raise of anti-HHV-3 Ab. induced by Varicella Vaccine.
Lymphocyte stimulation triggers the observed clinical anti-HSV-1/anti-HSV-2 efficiency using the varicella vaccine to prevent recurrent herpes diseases.It is clearly in favor of this hypothesis, a cell-mediated reactivity might be involved between HSV-1/HSV-2 and HHV-3.As a matter of fact, a specific serological increase of anti-HHV-3 Ab levels correlated with the recurrent herpes diseases cure can be observed.
In 2000, a link was established between the sexually recurrent herpes disease HSV-1/HSV-2 with HIV-1 AIDS diseases which were prevalent in Subtropical Africa [12].
It is important to underline the role played by the other members of the Betaherpesvirinae as HHV-5, the other members of the Gammaherpesvirinae include HHV-4 known as Epstein-Barr viruses are involved in lymphomas including Hodgkin lymphomas.Finally the HHV-8 viruses are linked to Kaposi sarcomas (Table 1).

METHODS -DATA ANALYSIS
Subtropical African Cancer Epidemics in Bantu populations were reported in the early 20 th century as an epicentre of Kaposi sarcomas and lymphoma epidemics.
Many clinicians in Central Africa proposed an infectious viral origin for outdoor Bantu tribes workers (1914).They failed to prove it.A resurgence of interest was stimulated by the high incidence of these cancers observed in South African histological samples tested in Johannesburg [13,14].Clinicians observed that outdoor Bantu hunters were the selected targets of these cancer epidemics [15].They were exposed to the blood of chimpanzees which could be infected by Simian Immunodeficiency Virus (SIV).AIDS IS A ZOONOSIS [16].Primates are reservoirs for SIV and if they carry SIV they can contaminate the Bantu hunters, SIV thus became HIV-1 in human-beings.SIV and HIV-1 are both RNA viruses [16].Central Africa remains the global HIV-1 epicentre (Fig. 1).
HIV-1 viruses escape from immune and drug pressures.It appears to be a co-activator of micro-organisms such as Pneumocystis jiroveci and viruses such as herpes viruses: lymphomas and Kaposi sarcomas as it was observed in the San Francisco epidemic (1981) [17].In 2008 close similarities were observed between the African Kaposi sarcomas epidemics and the same epidemics in San Francisco.Mostly young adults were affected by these similar fatal diseases called Acquired Immune Deficiency Syndrome, AIDS disease, which then emerged worldwide.
The production of deficient anti-HHV-3 antibodies is postulated in front of recurrent herpes viruses HSV-1/HSV-2, this could enhance the herpes immune deficiency facing HIV-1.
All human beings suffer from shingles caused by varicella virus (HHV-3/VZV) during childhood but an immunogenetic HHV-3 failure can be a first prerequisite to favour HSV-1/HSV-2 recurrent herpes diseases followed by the fatal outcome HIV-1 cell anchorage as stated by Lawrence Corey [18].

RESULTS
The evaluation of cancer epidemic data showed, Specific Environmental Factors that were proposed to play a key role in cancer epidemics in Subtropical Africa [19].These cancers are most frequent in South Africa as well as East Africa where the main part of the Bantu population is composed of outdoor forest farmers and where bare footedness is the rule.This suggested an etiological role of chronic injury among Bantu hunter inhabitants of tropical forests.Surprisingly, no case was reported among booted Bantu clerks living in cities in South Africa [19] (Figs. 4 and 5).  in [16] Among black African populations report by Findlay [28].

Fig. (5).
Kaposi's sarcoma and lymphoma epidemics among all cancers from 1988 to 1997 in Gambia.Compared to the USA these cancers were related to AIDS diseases in Bah et al. [27].
In Tropical Africa, Whites and Indians remained relatively unaffected by Kaposi sarcomas and lymphomas.We can wonder why they were able to save their lives compared to the native tropical forest Bantu populations?
In industrialized countries such as in Europe and in the USA, Kaposi sarcomas are known as a disease of the elderly compared to the large infected young Bantu populations (Fig. 6).6).Symposium in Kampala, Uganda, on Kaposi sarcomas, lymphomas and all cancers in Africa , series in black populations, Findlay [28].
These Kaposi sarcomas and lymphomas were already proposed to be contagious [20,21] with an incubation period of 1 to 10 years respectively in Mozambique [22] linked to occupations, occurring among farmers who constitute 95% of the Bantu population in Cameroon, Gabon, Congo [13].
Kaposi sarcomas identified at the histological level appeared at that time as clinically unique compared to American or European Kaposi sarcomas in terms of symptoms and fatal evolution [23].

DISCUSSION
Subtropical African human populations living in tropical forests were contaminated by zoonotic or cross-species transmission.Monkeys represent the natural reservoir of simian viruses, their infected females by SIV breast-fed for 4 years, so their simian babies were infected by SIV and these orphan animal were kept as pets which are able to contaminate all the hunter families [24,25].
For over several centuries, there have been frequent opportunities for human beings to become infected by SIVinfected chimpanzees but it is important to note that genetic mechanisms have been operating to enhance the immunogenic power of human beings to escape and survive attacks by endemic HIV-1 strains in Subtropical Africa.
It is necessary to help people in their immunological power against HIV-1.It is the medical priority of all physicians, as Lawrence Corey wrote it: the "two unrelated pathogens,HSV-1/HSV-2 and HIV-1, occupy the same ecological space in Central Africa" [18].The observations reported here underline the basic role played by members of the Herpesviridae family at the onset of the HIV-1 pandemic worldwide [26].
Bantu simian hunters could have presented an immungenetic weakness against VZV with an another reason: consanguinity.They became the deficient victims of the HSV-1/HSV-2 recurrent herpes diseases.Then exposed to be infected by SIV, the chimpanzee hunters and their families became eligible for SIV/HIV-1 contaminations and AIDS disease.

CONCLUSION
Following the recent discovery of the links between HSV-1/HSV-2 recurrent herpes diseases with a first varicella (HHV-3) immune deficiency, it appears that there is a preliminary biological herpes viral defect able to precede and to Fig.(6).Symposium in Kampala, Uganda, on Kaposi sarcomas, lymphomas and all cancers in Africa, series in black populations, Findlay[28].