Classification of Marek's disease viruses according to pathotype: Philosophy and methodology

El concepto de patotipo en la enfermedad de Marek (MD) data probablemente de finales de los 1950s cuando se reconoció una forma más virulenta de enfermedad Benton y Cover, 1957). Las distinciones entre las diferentes cepas de virus de MD (MDV) fueron aún mayores al describirse el patotipo vv a principios de los ochenta y el vv+ en los noventa. La designación de patotipo refleja propiedades biológicas importantes que se correlacionan con la capacidad de romper la inmunidad maternal en el campo. A pesar de ello, los métodos de clasificación de los diferentes patotipos en varios laboratorios no han sido uniformes, lo cual ha impedido una comparación crítica de los resultados. El método utilizado en el Avian Disease and Oncology Laboratory (ADOL) se basa en la inducción de lesiones linfoproliferativas en pollos vacunados. Este método ha sido utilizado para clasificar más de 45 aislados y es la base para la clasificación actual de los patotipos de cepas de MDV. Las limitaciones de este método son varias: necesidad de un tipo específico de pollos (15x7 ab+), uso de un gran número de animales y de un método estadístico para comparar las respuestas lesionales con las de las cepas control JM/102W y Md5. Debido a estas limitaciones no ha sido y no es probablemente usado en otros laboratorios. La comparación en el patotipado puede ser mejorada mediante la comparación de aislados de campo con cepas prototipo como las JM/102W, Md5 y 648A (American Type Culture Collection) o sus equivalentes. Los datos pueden ser generados mediante diferentes procedimientos in vivo que miden la inducción de tumores, enfermedad neurològica (por lesiones neoplásicas o no neoplásicas), o únicamente por criterios no neoplásicos (como el peso de los órganos linfoides o la replicación vírica). Los métodos basados en criterios neoplásicos, especialmente cuando son generados en pollos inmunizados de MD, probablemente se correlacionarán mejor con el método del ADOL y serán más relevantes en cuanto a la evolución de los virus de MD en el campo. En base a los datos de diferentes experimentos, se propone una modificación del método ADOL que utiliza menos animales y puede ser llevado a cabo en pollos SPF comerciales. El método modificado se basa en una comparación con el que mejor clasifica las cepas prototipo, y se espera que de resultados en general comparables con el método original. Otros criterios alternativos (ver abajo) también se evalúan como métodos primarios de patotipificación o como adjuntos a otros métodos de patotipificación. Se presentan las ventajas y desventajas de estos métodos alternativos.The concept of pathotype in Marek's disease (MD) probably dates from the recognition of a more virulent form of the disease in the late 1950s (Benton & Cover, 1957). Distinctions between MD virus strains were further expanded with the description of the vv pathotype in the early 1980s and of the vv + pathotype in the 1990s. Pathotype designations reflect important biological properties that correlate with the break-through of vaccinal immunity in the field. However, pathotyping methods applied by various laboratories have not been uniform, preventing critical comparison of results. Better uniformity of pathotyping procedures is desirable. The Avian Disease and Oncology Laboratory (ADOL) method is based on induction of lymphoproliferative lesions in vaccinated chickens. This method has been used to pathotype more than 45 isolates and is the basis for the current pathotype classification of MD virus strains. Its limitations include requirements for a specific type of chickens (15 x 7 ab+), large numbers of animals, and a statistical method to compare lesion responses to those of JM/102W and Md5 control strains. Because of these limitations, it has not been and is not likely to be used in other laboratories. Comparability in pathotyping can be improved by the comparison of field isolates with standard prototype strains such as JM/102W, Md5 and 648A (American Type Culture Collection) or their equivalents. Data may be generated by different in vivo procedures that measure tumour induction, neurological disease (both neoplastic and non-neoplastic lesions), or solely non-neoplastic criteria (such as lymphoid organ weights or virus replication). Methods based on neoplastic criteria, especially when generated in MD-immunized chickens, will probably correlate most closely with that of the ADOL method and be most relevant to evolution of MD virus in the field. Based on data from several trials, a modification of the ADOL method that utilizes fewer chickens and can be conducted with commercial specific pathogen free strains is proposed. The modified method is based on "best fit" comparisons with prototype strains, and is expected to provide results generally comparable with the original method. A variety of other alternative criteria (see earlier) are also evaluated both for primary pathotyping and as adjuncts to other pathotyping methods. Advantages and disadvantages of alternative methods are presented.Facultad de Ciencias Veterinaria

Multibaryons in the collective coordinate approach to the SU(3) Skyrme model

We obtain the rotational spectrum of strange multibaryon states by performing the SU(3) collective coordinate quantization of the static multi-Skyrmions. These background configurations are given in terms of rational maps, which are very good approximations and share the same symmetries as the exact solutions. Thus, the allowed quantum numbers in the spectra and the structure of the collective Hamiltonians we obtain are also valid in the exact case. We find that the predicted spectra are in overall agreement with those corresponding to the alternative bound state soliton model.Comment: 16 pages, 1 figur

Classification of Marek's disease viruses according to pathotype: Philosophy and methodology

El concepto de patotipo en la enfermedad de Marek (MD) data probablemente de finales de los 1950s cuando se reconoció una forma más virulenta de enfermedad Benton y Cover, 1957). Las distinciones entre las diferentes cepas de virus de MD (MDV) fueron aún mayores al describirse el patotipo vv a principios de los ochenta y el vv+ en los noventa. La designación de patotipo refleja propiedades biológicas importantes que se correlacionan con la capacidad de romper la inmunidad maternal en el campo. A pesar de ello, los métodos de clasificación de los diferentes patotipos en varios laboratorios no han sido uniformes, lo cual ha impedido una comparación crítica de los resultados. El método utilizado en el Avian Disease and Oncology Laboratory (ADOL) se basa en la inducción de lesiones linfoproliferativas en pollos vacunados. Este método ha sido utilizado para clasificar más de 45 aislados y es la base para la clasificación actual de los patotipos de cepas de MDV. Las limitaciones de este método son varias: necesidad de un tipo específico de pollos (15x7 ab+), uso de un gran número de animales y de un método estadístico para comparar las respuestas lesionales con las de las cepas control JM/102W y Md5. Debido a estas limitaciones no ha sido y no es probablemente usado en otros laboratorios. La comparación en el patotipado puede ser mejorada mediante la comparación de aislados de campo con cepas prototipo como las JM/102W, Md5 y 648A (American Type Culture Collection) o sus equivalentes. Los datos pueden ser generados mediante diferentes procedimientos in vivo que miden la inducción de tumores, enfermedad neurològica (por lesiones neoplásicas o no neoplásicas), o únicamente por criterios no neoplásicos (como el peso de los órganos linfoides o la replicación vírica). Los métodos basados en criterios neoplásicos, especialmente cuando son generados en pollos inmunizados de MD, probablemente se correlacionarán mejor con el método del ADOL y serán más relevantes en cuanto a la evolución de los virus de MD en el campo. En base a los datos de diferentes experimentos, se propone una modificación del método ADOL que utiliza menos animales y puede ser llevado a cabo en pollos SPF comerciales. El método modificado se basa en una comparación con el que mejor clasifica las cepas prototipo, y se espera que de resultados en general comparables con el método original. Otros criterios alternativos (ver abajo) también se evalúan como métodos primarios de patotipificación o como adjuntos a otros métodos de patotipificación. Se presentan las ventajas y desventajas de estos métodos alternativos.The concept of pathotype in Marek's disease (MD) probably dates from the recognition of a more virulent form of the disease in the late 1950s (Benton & Cover, 1957). Distinctions between MD virus strains were further expanded with the description of the vv pathotype in the early 1980s and of the vv + pathotype in the 1990s. Pathotype designations reflect important biological properties that correlate with the break-through of vaccinal immunity in the field. However, pathotyping methods applied by various laboratories have not been uniform, preventing critical comparison of results. Better uniformity of pathotyping procedures is desirable. The Avian Disease and Oncology Laboratory (ADOL) method is based on induction of lymphoproliferative lesions in vaccinated chickens. This method has been used to pathotype more than 45 isolates and is the basis for the current pathotype classification of MD virus strains. Its limitations include requirements for a specific type of chickens (15 x 7 ab+), large numbers of animals, and a statistical method to compare lesion responses to those of JM/102W and Md5 control strains. Because of these limitations, it has not been and is not likely to be used in other laboratories. Comparability in pathotyping can be improved by the comparison of field isolates with standard prototype strains such as JM/102W, Md5 and 648A (American Type Culture Collection) or their equivalents. Data may be generated by different in vivo procedures that measure tumour induction, neurological disease (both neoplastic and non-neoplastic lesions), or solely non-neoplastic criteria (such as lymphoid organ weights or virus replication). Methods based on neoplastic criteria, especially when generated in MD-immunized chickens, will probably correlate most closely with that of the ADOL method and be most relevant to evolution of MD virus in the field. Based on data from several trials, a modification of the ADOL method that utilizes fewer chickens and can be conducted with commercial specific pathogen free strains is proposed. The modified method is based on "best fit" comparisons with prototype strains, and is expected to provide results generally comparable with the original method. A variety of other alternative criteria (see earlier) are also evaluated both for primary pathotyping and as adjuncts to other pathotyping methods. Advantages and disadvantages of alternative methods are presented.Facultad de Ciencias Veterinaria

Radiative decays of decuplet hyperons

We calculate the radiative decay widths of decuplet hyperons in a chiral constituent quark model including electromagnetic exchange currents between quarks. Exchange currents contribute significantly to the E2 transition amplitude, while they largely cancel for the M1 transition amplitude. Strangeness suppression of the radiative hyperon decays is found to be weakened by exchange currents. Differences and similarities between our results and other recent model predictions are discussed.Comment: 11 pages, 1 eps figure, revtex, accepted for publication in Phys. Rev.

Clonal Structure of Rapid-Onset MDV-Driven CD4+ Lymphomas and Responding CD8+ T Cells

Lymphoid oncogenesis is a life threatening complication associated with a number of persistent viral infections (e.g. EBV and HTLV-1 in humans). With many of these infections it is difficult to study their natural history and the dynamics of tumor formation. Marek's Disease Virus (MDV) is a prevalent α-herpesvirus of poultry, inducing CD4+ TCRαβ+ T cell tumors in susceptible hosts. The high penetrance and temporal predictability of tumor induction raises issues related to the clonal structure of these lymphomas. Similarly, the clonality of responding CD8 T cells that infiltrate the tumor sites is unknown. Using TCRβ repertoire analysis tools, we demonstrated that MDV driven CD4+ T cell tumors were dominated by one to three large clones within an oligoclonal framework of smaller clones of CD4+ T cells. Individual birds had multiple tumor sites, some the result of metastasis (i.e. shared dominant clones) and others derived from distinct clones of transformed cells. The smaller oligoclonal CD4+ cells may represent an anti-tumor response, although on one occasion a low frequency clone was transformed and expanded after culture. Metastatic tumor clones were detected in the blood early during infection and dominated the circulating T cell repertoire, leading to MDV associated immune suppression. We also demonstrated that the tumor-infiltrating CD8+ T cell response was dominated by large oligoclonal expansions containing both “public” and “private” CDR3 sequences. The frequency of CD8+ T cell CDR3 sequences suggests initial stimulation during the early phases of infection. Collectively, our results indicate that MDV driven tumors are dominated by a highly restricted number of CD4+ clones. Moreover, the responding CD8+ T cell infiltrate is oligoclonal indicating recognition of a limited number of MDV antigens. These studies improve our understanding of the biology of MDV, an important poultry pathogen and a natural infection model of virus-induced tumor formation

The nature of the Lambda(1405)

We present here some results supporting the nature of the $\Lambda(1405)$ resonance as dynamically generated from the meson baryon interaction in coupled channels and resulting from the superposition of two close-by poles. We find support for this picture in the $K^- p \to \pi^0 \pi^0 \Sigma^0$ reaction, which shows a different shape than the one obtained from the $\pi ^- p \to K^0 \pi \Sigma$ reaction. We also call the attention to the $K^- p \to \gamma \pi \Sigma$ with $\pi \Sigma$ in the $\Lambda(1405)$ region, which shows a narrow peak in the calculations around 1420 MeV. We also report on recent calculations of the radiative decay of the two $\Lambda(1405)$ states and on reactions to obtain information on these decay modes. Finally, we present results for the $pp\to p K^+\Lambda(1405)$ reaction recently measured at ANKE/COSY and compare them with theoretical results.Comment: Talk given at the NSTAR2007 Workshop, Bonn September 200

Masses of the 70- Baryons in Large Nc QCD

The masses of the negative parity 70-plet baryons are analyzed in large N_c QCD to order 1/N_c and to first order in SU(3) symmetry breaking. The existing experimental data are well reproduced and twenty new observables are predicted. The leading order SU(6) spin-flavor symmetry breaking is small and, as it occurs in the quark model, the subleading in 1/N_c hyperfine interaction is the dominant source of the breaking. It is found that the Lambda(1405) and Lambda(1520) are well described as three-quark states and spin-orbit partners. New relations between splittings in different SU(3) multiplets are found.Comment: 11 pages; references were added and a couple of improvements to the text were mad

Magnetic moments of the low-lying JP= 1/2−J^P=\,1/2^-, 3/2−3/2^- Λ\Lambda resonances within the framework of the chiral quark model

The magnetic moments of the low-lying spin-parity $J^P=$ $1/2^-$, $3/2^-$ $\Lambda$ resonances, like, for example, $\Lambda(1405)$ $1/2^-$, $\Lambda(1520)$ $3/2^-$, as well as their transition magnetic moments, are calculated using the chiral quark model. The results found are compared with those obtained from the nonrelativistic quark model and those of unitary chiral theories, where some of these states are generated through the dynamics of two hadron coupled channels and their unitarization

Multibaryons with heavy flavors in the Skyrme model

We investigate the possible existence of multibaryons with heavy flavor quantum numbers using the bound state approach to the topological soliton model and the recently proposed approximation for multiskyrmion fields based on rational maps. We use an effective interaction lagrangian which consistently incorporates both chiral symmetry and the heavy quark symmetry including the corrections up to order 1/m_Q. The model predicts some narrow heavy flavored multibaryon states with baryon number four and seven.Comment: 8 pages, no figures, RevTe

Negative Parity 70-plet Baryon Masses in the 1/Nc Expansion

The masses of the negative parity SU(6) 70-plet baryons are analyzed in the 1/Nc expansion to order 1/Nc and to first order in SU(3) breaking. At this level of precision there are twenty predictions. Among them there are the well known Gell-Mann Okubo and equal spacing relations, and four new relations involving SU(3) breaking splittings in different SU(3) multiplets. Although the breaking of SU(6) symmetry occurs at zeroth order in 1/Nc, it turns out to be small. The dominant source of the breaking is the hyperfine interaction which is of order 1/Nc. The spin-orbit interaction, of zeroth order in 1/Nc, is entirely fixed by the splitting between the singlet states Lambda(1405) and Lambda(1520), and the spin-orbit puzzle is solved by the presence of other zeroth order operators involving flavor exchange.Comment: 31 pages, 3 figure