“In His Arm the Scar”: Medicine, Race, and the Social Implications of the 1721 Inoculation Controversy on Boston

Hurford, Christianna Elrene Thomas

22 October 2010

No description available.

African Americans

American History

European History

History

Medicine

Disease

Race

Smallpox

Inoculation

Boston

Onesimus

Predicting epidemiological transitions in infectious disease dynamics: Smallpox in historic London (1664-1930)

Krylova, Olga

10 1900

<p>Mathematical modelling has become a powerful tool used to predict the spread of infectious diseases in populations. Successful analysis and modeling of historical infectious disease data can explain changes in the pattern of past epidemics and lead to a better understanding of epidemiological processes. The lessons learned can be used to predict future epidemics and help to improve public healthstrategies for control and eradication.</p> <p>This thesis is focused on the analysis and modelling of smallpox dynamics based on the weekly smallpox mortality records in London, England, 1664-1930. Statistical analysis of these records is presented. A timeline of significant historical events related to changes in variolation and vaccination uptake levels and demographics was established. These events were correlated with transitions observed in smallpox dynamics. Seasonality of the smallpox time series was investigated and the contact rate between susceptible and infectious individuals was found to be seasonally forced. Seasonal variations in smallpox transmission and changes in their seasonality over long time scale were estimated. The method of transition analysis, which is used to predict qualitative changes in epidemiological patterns, was used to explain the transitions observed in the smallpox time series. We found that the standard SIR model exhibits dynamics similar to the more realistic Gamma distributed SEIR model if the mean serial interval is chosen the same, so we used the standard SIR model for our analysis. We conclude that transitions observed in the temporal pattern of smallpox dynamics can be explained by the changes in birth, immigration and intervention uptake levels.</p> / Doctor of Philosophy (PhD)

transition analysis

smallpox

SIR model

London Bills of Mortality

Other Applied Mathematics

Other Applied Mathematics

Gold fever: death and disease during the Klondike gold rush, 1898-1904

Highet, Megan J.

12 September 2008

This thesis represents the first anthropological perspective to be offered on the nature of the Klondike Gold Rush population. In order to better understand the experience of the average gold rusher, morbidity and mortality patterns are examined for the residents of the Yukon Territory following the discovery of gold in the region (1898-1904). Infectious diseases such as measles, pneumonia, smallpox and typhoid fever are the primary focus of this study, however local factors such as the severe climate and the seclusion of the gold fields from the outside world also offers an interesting opportunity to examine the consequences of leading a particularly harsh and physically demanding lifestyle in an inhospitable environment. / October 2008

Klondike Gold Rush

Dawson City

Typhoid Fever

Smallpox

Pneumonia

Scurvy

Measles

Infectious Disease

Anthropological Demography

Accidental Death

Gold fever: death and disease during the Klondike gold rush, 1898-1904

Highet, Megan J.

12 September 2008

This thesis represents the first anthropological perspective to be offered on the nature of the Klondike Gold Rush population. In order to better understand the experience of the average gold rusher, morbidity and mortality patterns are examined for the residents of the Yukon Territory following the discovery of gold in the region (1898-1904). Infectious diseases such as measles, pneumonia, smallpox and typhoid fever are the primary focus of this study, however local factors such as the severe climate and the seclusion of the gold fields from the outside world also offers an interesting opportunity to examine the consequences of leading a particularly harsh and physically demanding lifestyle in an inhospitable environment.

Klondike Gold Rush

Dawson City

typhoid fever

smallpox

pneumonia

scurvy

measles

infectious disease

anthropological demography

accidental death

Gold fever: death and disease during the Klondike gold rush, 1898-1904

Highet, Megan J.

12 September 2008

This thesis represents the first anthropological perspective to be offered on the nature of the Klondike Gold Rush population. In order to better understand the experience of the average gold rusher, morbidity and mortality patterns are examined for the residents of the Yukon Territory following the discovery of gold in the region (1898-1904). Infectious diseases such as measles, pneumonia, smallpox and typhoid fever are the primary focus of this study, however local factors such as the severe climate and the seclusion of the gold fields from the outside world also offers an interesting opportunity to examine the consequences of leading a particularly harsh and physically demanding lifestyle in an inhospitable environment.

Klondike Gold Rush

Dawson City

Typhoid Fever

Smallpox

Pneumonia

Scurvy

Measles

Infectious Disease

Anthropological Demography

Accidental Death

The Unwelcomed Traveler: England's Black Death and Hopi's Smallpox

January 2014

abstract: This dissertation analyzes the fourteenth-century English and nineteenth-century Hopi experiences with the unwelcomed traveler of disease, specifically the Black Death and the smallpox outbreak of 1898-1899. By placing both peoples and events beside one another, it becomes possible to move past the death toll inflected by disease and see the role of diseases as a catalyst of historical change. Furthermore, this study places the Hopi experience with smallpox, and disease in general, in context with the human story of disease. The central methodical approach is ethnohistory, using firsthand accounts to reconstruct the cultural frameworks of the Hopi and the English. In analyzing the English and Hopi experiences this study uses the Medicine Way approach of three dimensions. Placing the first dimension approach (the English and the bubonic plague) alongside the third dimension approach (the Hopi and smallpox) demonstrates, not only the common ground of both approaches (second dimension), but the commonalities in the interactions of humans and disease. As my dissertation demonstrates, culture provides the framework, a system for living, for how individuals will interpret and react to events and experiences. This framework provides a means, a measure, to identify and strive for normalcy. There is a universal human drive to restore normalcy after one's world turns upside down, and in seeking to restore what was lost, society undergoes transformation. Disease creates opportunity for change and for balance to be restored. This study concludes disease is a catalyst of change because of how humans respond to it. / Dissertation/Thesis / Doctoral Dissertation History 2014

History

Medieval history

Native American studies

14th Century English

Black Death

history of disease

Hopi

Oraibi Split of 1906

Smallpox

Développement d'un vecteur virus de la vaccine, réplicatif et atténué, pour la vaccination antivariolique et pour la vaccination contre la fièvre hémorragique à virus Ebola / Development of an attenuated replicative Vaccinia virus vector to protect against Variola and Ebola haemorragic fever

Dimier, Julie

30 October 2012

Le virus Ebola, responsable d'une fièvre hémorragique virale létale et le virus de la variole, agent étiologique de la variole, sont des armes biologiques potentielles. Il n'existe pas de traitement ou de prophylaxie autorisés contre le virus Ebola, quelques candidats vaccins étant en cours de développement. Concernant la variole, des vaccins dits de première génération (virus de la vaccine) ont permis l'éradication de la maladie cependant ils sont à l'origine de complications post-vaccinales parfois sévères alors que des vaccins plus récents dits de troisième génération, non-réplicatifs, ont été développés pour leur innocuité mais restent faiblement immunogènes. Nous avons récemment développé plusieurs vecteurs viraux de type virus de la vaccine (VACV) par délétion d'un certain nombre de facteurs de virulence. Nous avons évalué leur innocuité, leur immunogénicité et leur efficacité en tant que candidats vaccins antivarioliques chez la souris puis utilisé l'un de ces vecteurs pour développer un candidat vaccin bivalent antivariolique et anti-virus Ebola. Ces virus de la vaccine délétés sont réplicatifs mais fortement atténués. Ils induisent une réponse en anticorps neutralisants spécifiques anti-vaccine similaire à celle induite par le vaccin antivariolique de première génération et induisent des réponses immunitaires cellulaires CD4+ et CD8+ spécifiques suffisantes pour protéger l'animal d'un challenge létal de cowpoxvirus en intranasal, simulant une infection par le virus de la variole. Le virus délété le plus immunogène et le plus sûr, nommé MVL, a été utilisé pour construire un vecteur viral codant pour la glycoprotéine du virus Ebola (EGP). Le gène entier d'EGP ou une forme chimérique d'EGP (fusion entre l'ectodomaine d'EGP et le domaine transmembranaire de la glycoprotéine B5 du VACV) ont été clonés dans le génome du vecteur viral. Ces deux vecteurs produisent des virus ayant incorporé EGP dans leur enveloppe. Ces deux candidats vaccins recombinants induisent de fortes réponses humorales spécifiques anti-EGP et anti-vaccine chez la souris immunocompétente. En conclusion, nous avons développé plusieurs candidats vaccins antivarioliques aussi immunogènes et efficaces que le vaccin historique et avec une atténuation similaire aux vaccins de troisième génération. L'un de ces candidats (MVL) a été utilisé comme vecteur viral pour exprimer la glycoprotéine hétérologue EGP, contre laquelle il induit une réponse immunitaire humorale forte / Ebola virus, causing a lethal haemorrhagic fever and variola virus, the agent of smallpox are potential biological weapons. There is no treatment and no prophylaxis authorised against Ebola, although some vaccine viral vectors were developed these last years. Concerning smallpox, several types of vaccines exist against smallpox (based on vaccinia virus), first generation that allowed the disease eradication but responsible of some post-vaccination complications and some non-replicative 3rd generation vaccines which are safe but not very immunogenic. We have recently developed several vaccinia virus (VACV) vectors by deletion of some virulence genes, and we have evaluated their safety, immunogenicity and efficacy as smallpox vaccine in mice and used one of them as a bivalent vaccine against Ebola and smallpox. These viral vectors are higly attenuated and replicative competent. They induce a neutralizing specific-VACV antibodies response similar to that of the historical vaccine and induce VACV-specific CD8+ and CD4+ immune responses efficient to protect immunocompetent mouse model intranasally infected by cowpox virus, simulating variola virus infection.The most safety and immunogenic vaccinia virus vector, named MVL, has been used to construct a vector encoding the Ebola glycoprotein (EGP) for immunization against Ebola. The native EGP gene or a chimeric EGP gene (a fusion between the EGP ectodomain and the transmembrane domain of the VACV B5 glycoprotein) have been cloned into the viral vector genome. These two recombinant vaccine candidates induce specific humoral immune responses against Ebola and vaccinia virus in immunocompetent mice. In conclusion, we have developed several vaccine candidates against smallpox as immunogenic and protective as the historical vaccine and as safe as 3rd generation vaccines. One of these candidates, MVL, has been used as a viral vector to express the heterologous glycoprotein EGP, against which it induce a strong humoral immune response.

Vaccin

Virus de la vaccine

Virus Ebola

Variole

Fièvre hémorragique virale

Vaccine

Vaccinia virus

Ebola virus

Smallpox

Viral haemorrhagic fever

Pathogenesis of orthopoxvirus (OPXV) infection in common CM and identification of immune correlates after vaccination with differently attenuated vaccines / Pathogenesis of orthopoxvirus (OPXV) infection in common CM and identification of immune correlates after vaccination with differently attenuated vaccines

Gan, Li Lin

17 January 2018

No description available.

570

Calpox virus

pathogenesis

non-human primate model

calpox virus/marmoset model

smallpox vaccine

MVTT

MVA

New World

Biologie (PPN619462639)

Pus, Pox, Propaganda and Progress: The Compulsory Smallpox Vaccination Controversy in Utah, 1899-1901

Bluth, Eric L.

01 January 1993

This thesis examines the compulsory smallpox vaccination controversy in Utah, 1899-1901. It looks at the two smallpox epidemics during 1899-1901 and follows the boards of health attempts to eradicate smallpox primarily by compelling the vaccination of school children.Dr. Theodore B. Beatty, secretary of the State Board of Health, championed the effort to vaccinate all Utahns; however, the opposition led by Charles W. Penrose, editor of the Deseret Evening News, produced anti-compulsion and vaccination information which influenced Utahns to generally oppose vaccination. Consequently, the legislature passed an anti-compulsory vaccination statute over the governor's veto to annul the courts decision that the health boards had the authority to compel vaccination.The research reveals that Utah's opposition to compulsory vaccination impeded medical progress. It also claims that this was the first controversy experienced by the members of the dominant religion in Utah which resulted in the expression of divergent viewpoints.

Smallpox

Vaccination

Utah

History

Law

legislation

Charles W. Penrose

Charles William

1832-1925

Mormon Studies

Public Health

Infections of common marmosets with calpox virus

Kramski, Marit

29 January 2009

Die vorsätzliche Freisetzung von Variola Virus (VARV) und schwere Erkrankungen des Menschen durch zoonotische Affen- (MPXV) und Kuh- (CPXV) pocken Viren stellen nach wie vor eine Bedrohung für die Bevölkerung dar. Klassische Pockenimpfstoffe bergen die Gefahr einer schweren Erkrankung. Deshalb ist die Entwicklung neuer Impfstoffe und Therapeutika von entscheidender Bedeutung. Deren Wirksamkeit und Sicherheit muss zunächst in verschiedenen Tiermodellen bewiesen werden. Existierende Makakken-Primatenmodelle leiden unter sehr artifiziellen Bedingungen der letalen Krankheitsinduktion durch VARV oder MPXV. Aus diesem Grund wurde das Calpox Virus/Krallenaffen-modell etabliert, welches auf einem CPXV aus natürlich infizierten Neuweltaffen (Marmosets) basiert. Das neue Modell hat drei wesentliche Vorteile: Die Arbeit mit Calpox Virus kann unter Sicherheitsstufe 2 durchgeführt werden und ist folglich einfacher in der Handhabung. 2. Die intranasale (i.n.) Infektion von Marmosets (Krallenaffen; Callithrix jacchus) spiegelt den natürlichen Infektionsweg von VARV wieder. Infizierte Affen entwickelten Pocken ähnliche Symptome und verstarben innerhalb von 2-3 Tagen nach Auftreten erster Symptome. Hohe Viruslasten wurden im Blut, Speichel und allen untersuchten Organen nachgewiesen. 3. Die i.n. Titration des Calpox Virus ergab eine 50 % Affen-Infektions-Dosis (MID50) von 8.3x102 pfu. Diese ist um den Faktor 10000 niedriger als in anderen Pocken-Primatenmodellen. Neun bis zehn Wochen nach einer Immunisierung mit dem Lister-Elstree Impfstoff waren alle Krallenaffen gegen eine letale Dosis des Calpox Virus (10 MID50) geschützt. Damit konnte der Nutzen des Calpox Virus/Krallenaffen-modells für die Erforschung neuer Impfstoffe gezeigt werden. Das Calpox Virus/Krallenaffen-modell überwindet wesentliche Nachteile bestehender Primatenmodelle und ist somit ein geeignetes Model für die Evaluierung von neuen Impfstoffen, Impfstrategien und antiviralen Therapien. / The intentional re-introduction of Variola virus (VARV), the agents of smallpox, into the human population remains of concern today. Moreover, zoonotic infections with Cowpox (CPXV) and Monkeypox virus (MPXV) cause severe diseases in humans. Smallpox vaccines presently available can have severe adverse effects that are no longer acceptable. The efficacy and safety of new vaccines and antivirals have to be demonstrated by different animal models. The existing primate models, using VARV and MPXV, need very high viral doses that have to be applied intravenously to induce a lethal infection in macaque monkeys. To overcome these drawbacks, the main objective of this study was to develop a primate model in which a smallpox-like disease could be induced by a CPXV virus designated calpox virus which was isolated from a lethal orthopox virus (OPV) outbreak in New World monkeys (marmosets). The new non-human primate model has three major advantages: 1. Working with calpox virus is less challenging and can be done under bio-safety-level two. 2. Mimicking the natural route of VARV infection, intranasally infected marmosets (Callithrix jacchus) reproducibly developed clinical symptoms of an OPV infection and died within two to three days after onset of the first symptoms. High viral loads of calpox virus were detected in blood, saliva and all analyzed organs. 3. Intranasal titration of the virus resulted in a 50 % monkey infectious dose (MID50) of 8.3x102 pfu, a lethal infectious dose 10,000 lower than those used in any other primate model. Moreover, we showed the aptitude of the primate model for the testing of new vaccines since nine to ten weeks after immunization with Vaccinia virus Lister-Elstree marmosets were completely protected against intranasal challenge with 10 MID50 of calpox virus. As the calpox virus/marmoset model overcomes major limitations of current primate models it is suitable to evaluate new vaccines, new vaccination strategies and antiviral therapies.

Immunisierung

Primatenmodell

intranasale Infektion

Krallenaffen

humane Pocken

non-human primate model

intranasal infection

vaccination

Callithrix jacchus

smallpox

570 Biowissenschaften, Biologie

32 Biologie

WF 3000

ddc:570