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1. Multiple congenital ocular anomalies in Icelandic horses

Author

Lindgren Gabriella, Dubielzig Richard R, Axelsson Jeanette, Andersson Lisa S, and Ekesten Björn

Subjects
Veterinary medicine, SF600-1100
Abstract

Abstract Background Multiple congenital ocular anomalies (MCOA) syndrome is a hereditary congenital eye defect that was first described in Silver colored Rocky Mountain horses. The mutation causing this disease is located within a defined chromosomal interval, which also contains the gene and mutation that is associated with the Silver coat color (PMEL17, exon 11). Horses that are homozygous for the disease-causing allele have multiple defects (MCOA-phenotype), whilst the heterozygous horses predominantly have cysts of the iris, ciliary body or retina (Cyst-phenotype). It has been argued that these ocular defects are caused by a recent mutation that is restricted to horses that are related to the Rocky Mountain Horse breed. For that reason we have examined another horse breed, the Icelandic horse, which is historically quite divergent from Rocky Mountain horses. Results We examined 24 Icelandic horses and established that the MCOA syndrome is present in this breed. Four of these horses were categorised as having the MCOA-phenotype and were genotyped as being homozygous for the PMEL17 mutation. The most common clinical signs included megaloglobus, iris stromal hypoplasia, abnormal pectinate ligaments, iridociliary cysts occasionally extending into the peripheral retina and cataracts. The cysts and pectinate ligament abnormalities were observed in the temporal quadrant of the eyes. Fourteen horses were heterozygous for the PMEL17 mutation and were characterized as having the Cyst-phenotype with cysts and occasionally curvilinear streaks in the peripheral retina. Three additional horses were genotyped as PMEL17 heterozygotes, but in these horses we were unable to detect cysts or other forms of anomalies. One eye of a severely vision-impaired 18 month-old stallion, homozygous for the PMEL17 mutation was examined by light microscopy. Redundant duplication of non-pigmented ciliary body epithelium, sometimes forming cysts bulging into the posterior chamber and localized areas of atrophy in the peripheral retina were seen. Conclusions The MCOA syndrome is segregating with the PMEL17 mutation in the Icelandic Horse population. This needs to be taken into consideration in breeding decisions and highlights the fact that MCOA syndrome is present in a breed that are more ancient and not closely related to the Rocky Mountain Horse breed.

Published
2011
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2. PRESUMED PHOTORECEPTOR DYSPLASIAS IN PEREGRINE FALCONS ( FALCO PEREGRINUS) AND PEREGRINE FALCON HYBRIDS.

Author

Moore, Bret A, Murphy, Christopher J, Marlar, Annajane, Dubielzig, Richard R, Teixeira, Leandro BC, Ferrier, William T, and Hollingsworth, Steven R

Subjects
Animals, Falconiformes, Humans, Retinal Diseases, Bird Diseases, Female, Male, Photoreceptor Cells, Vertebrate, Avian, bird, cone, eye, genetic, ophthalmology, raptor, vision, Neurodegenerative, Eye Disease and Disorders of Vision, Neurosciences, Aetiology, 2.1 Biological and endogenous factors, Eye, Zoology, Veterinary Sciences
Abstract

We describe a case series of photoreceptor dysplasia with secondary retinal degeneration in juvenile Peregrine Falcons. Six Peregrine Falcons ( Falco peregrinus) and three Peregrine Falcon × Prairie Falcon ( Falco mexicanus) hybrids had early-life visual deficits. Eight birds had visual defects shortly after hatching, and one bird had visual deficits first noticed at 5 mo of age. Complete ophthalmic examinations were performed in each animal. Eight of the animals had electroretinograms, and nine of the animals had their eyes examined histologically after euthanasia. Ophthalmic examinations did not reveal consistent and potentially blinding abnormalities, including an absence of ophthalmoscopic retinal lesions. Electroretinographic findings included subnormal amplitudes (with rod responses more abnormal than cone responses), with a negative b-wave amplitude occurring in one bird. Histologically, a reduction in the number of photoreceptors was present with numerous degenerative changes to the remaining photoreceptors, including frequent blunting and disorganization of photoreceptor outer segments, decreased numbers of cells in the inner nuclear layer, decreased numbers of ganglion cells, decreased thickness of the nerve fiber layer, and decreased myelinated axons within the optic nerve. Ultrastructurally, only minor cone outer segment changes and occasional phagocytic cells were seen. Results strongly suggested a primary retinopathy, characterized by photoreceptor dysplasia and secondary retinal degeneration with loss of cellular elements throughout the retina. The presence of a similar spectrum of findings in related individuals, the early age of onset, and the relative lack of other environmental, ocular, or systemic abnormalities suggested possible heritability.

Published
2019

3. Anchoring a cytoactive factor in a wound bed promotes healing

Author

Chattopadhyay, Sayani, Guthrie, Kathleen M, Teixeira, Leandro, Murphy, Christopher J, Dubielzig, Richard R, McAnulty, Jonathan F, and Raines, Ronald T

Subjects
Prevention, Animals, Biomimetic Materials, Collagen, Disease Models, Animal, Immobilized Proteins, Male, Mice, Mice, Mutant Strains, Peptides, Substance P, Wound Healing, Wounds and Injuries, collagen, extracellular matrix, Mus musculus, peptide, synthetic biology, Biomedical Engineering, Clinical Sciences, Medical Physiology
Abstract

Wound healing is a complex process that requires the intervention of cytoactive factors. The one-time application of soluble factors to a wound bed does not maintain a steady, sufficient concentration. Here we investigated the benefits of anchoring a factor in a wound bed via a tether to endogenous collagen. We used a collagen-mimetic peptide (CMP) as a pylon. The CMP binds to damaged but not intact collagen and thus localizes a pendant cytoactive factor in the regions of a wound bed that require intervention. As a model factor, we chose substance P, a peptide of the tachykinin family that promotes wound healing. Using splinted wounds in db/db mice, we found that the one-time application of a CMP-substance P conjugate enhances wound healing compared to unconjugated substance P and other controls. Specifically, all 16 wounds treated with the conjugate closed more thoroughly and, did so with extensive re-epithelialization and mitigated inflammatory activity. These data validate a simple and general strategy for re-engineering wound beds by the integration of beneficial cytoactive factors. Copyright © 2014 John Wiley & Sons, Ltd.

Published
2016

4. Presumed solitary intraocular or conjunctival lymphoma in dogs and cats: 9 cases (1985-2013).

Author

Wiggans, K Tomo, Skorupski, Katherine A, Reilly, Christopher M, Frazier, Sara A, Dubielzig, Richard R, and Maggs, David J

Subjects
Hematology, Eye Disease and Disorders of Vision, Rare Diseases, Lymphoma, Cancer, Animals, Cat Diseases, Cats, Dog Diseases, Dogs, Eye Neoplasms, Female, Male, Retrospective Studies, Veterinary Sciences
Abstract

ObjectiveTo determine prevalence, reason for evaluation, treatment, and outcome for dogs and cats with presumed solitary ocular lymphoma (PSOL).DesignRetrospective case series.Animals7 dogs and 2 cats with PSOL.ProceduresMedical records were reviewed. Progression-free survival time (PFST) and overall survival time (OST) were determined.ResultsAnimals with intraocular (4 dogs and 1 cat) or conjunctival (3 dogs and 1 cat) lymphoma represented 0.1% and 0.08% of patients with lymphoma evaluated at the hospital during the study period, respectively. Animals with intraocular lymphoma represented 0.19% of all patients with uveitis; animals with conjunctival lymphoma represented 0.16% of all patients with conjunctivitis. Tumors included B-cell (2 intraocular and 1 conjunctival), non-B-cell, non-T-cell (1 intraocular), and T-cell (3 conjunctival) neoplasms; immunophenotype of 2 uveal lymphomas was not determined. Treatments included enucleation (4 intraocular) and chemotherapy (3 intraocular and 2 conjunctival). All dogs with intraocular lymphoma developed neurologic signs. Lymph node metastasis was detected in 2 patients with conjunctival lymphoma. Median PFST and OST were 178 days for all animals with PSOL, dogs with PSOL, and animals with intraocular lymphoma. Median PFST and OST for animals with conjunctival lymphoma were 221 and 549 days, respectively.Conclusions and clinical relevanceResults indicated PSOL was uncommon, but should be considered a differential diagnosis for animals with uveitis or conjunctivitis. Performance of MRI and cytologic analysis of CSF and regional lymph node aspirate samples may be beneficial for such patients. Prognosis seemed to be better for animals with conjunctival lymphoma than it was for those with intraocular lymphoma.

Published
2014

5. Integration of Silver Nanoparticle-impregnated Polyelectrolyte Multilayers Into Murine-Splinted Cutaneous Wound Beds

Author

Guthrie, Kathleen M, Agarwal, Ankit, Teixeira, Leandro BC, Dubielzig, Richard R, Abbott, Nicholas L, Murphy, Christopher J, Singh, Harpreet, McAnulty, Jonathan F, and Schurr, Michael J

Subjects
Medical Biotechnology, Biomedical and Clinical Sciences, Bioengineering, Nanotechnology, Diabetes, Skin, Animals, Diabetes Mellitus, Experimental, Disease Models, Animal, Male, Mice, Mice, Inbred Strains, Nanoparticles, Occlusive Dressings, Pilot Projects, Polymers, Random Allocation, Silver Compounds, Splints, Wound Healing, Clinical Sciences, Emergency & Critical Care Medicine, Clinical sciences, Allied health and rehabilitation science, Nursing
Abstract

Silver is a commonly used topical antimicrobial. However, technologies to immobilize silver at the wound surface are lacking, while currently available silver-containing wound dressings release excess silver that can be cytotoxic and impair wound healing. We have shown that precise concentrations of silver at lower levels can be immobilized into a wound bed using a polyelectrolyte multilayer attachment technology. These silver nanoparticle-impregnated polyelectrolyte multilayers are noncytotoxic yet bactericidal in vitro, but their effect on wound healing in vivo was previously unknown. The purpose of this study was to determine the effect on wound healing of integrating silver nanoparticle/polyelectrolyte multilayers into the wound bed. A full-thickness, splinted, excisional murine wound healing model was employed in both phenotypically normal mice and spontaneously diabetic mice (healing impaired model). Gross image measurements showed an initial small lag in healing in the silver-treated wounds in diabetic mice, but no difference in time to complete wound closure in either normal or diabetic mice. Histological analysis showed modest differences between silver-treated and control groups on day 9, but no difference between groups at the time of wound closure. We conclude that silver nanoparticle/polyelectrolyte multilayers can be safely integrated into the wound beds of both normal and diabetic mice without delaying wound closure, and with transient histological effects. The results of this study suggest the feasibility of this technology for use as a platform to affect nanoscale wound engineering approaches to microbial prophylaxis or to augment wound healing.

Published
2013

6. List of Contributors

Author

Alden, Carl L., primary, Berridge, Brian R., additional, Bolon, Brad, additional, Bounous, Denise I., additional, Butt, Mark T., additional, Cattley, Russell C., additional, Chapin, Robert E., additional, Chebekoue, Sandrine F., additional, Creasy, Dianne M., additional, Cullen, John M., additional, Danilenko, Dimitry M., additional, Davis, Barbara, additional, Diegel, Kelly L., additional, Dorman, David C., additional, Dubielzig, Richard R., additional, Elmore, Susan A., additional, Fenton, Suzanne E., additional, Ferguson, Duncan C., additional, Foley, George L., additional, Garman, Robert H., additional, Gropp, Kathryn E., additional, Gunson, Diane, additional, Hard, Gordon C., additional, Harkema, Jack R., additional, Haschek, Wanda M., additional, Herman, Eugene, additional, Hoenerhoff, Mark J., additional, Janovitz, Evan B., additional, Khan, Kanwar N.M., additional, Krishnan, Kannan, additional, Kuper, C. Frieke, additional, Lehman-McKeeman, Lois D., additional, Li, Xiantang, additional, Malarkey, David E., additional, Maronpot, Robert R., additional, Nikula, Kristen J., additional, Ochoa, Ricardo, additional, Parker, George A., additional, Ramaiah, Lila, additional, Rousseaux, Colin G., additional, Rudmann, Daniel G., additional, Ruehl-Fehlert, Christine, additional, Ruepp, Stefan U., additional, Schafer, Kenneth A., additional, Sullivan, John M., additional, Teixeira, Leandro, additional, Van Vleet, John F., additional, Varela, Aurore, additional, Wallig, Matthew A., additional, and Wojcinski, Zbigniew W., additional

Published
2018
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9. Pathology in Practice

Author

Khorsand, Matthew, primary, Martabano, Brittany B., additional, MacNeill, Amy, additional, Ehrhart, Nicole, additional, Dubielzig, Richard R., additional, Teixeira, Leandro, additional, and Henriksen, Michala de Linde, additional

Published
2022
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17. Contributors

Author

Adams, E. Terence, primary, Adler, Rick, additional, Alden, Carl L., additional, Bartholomew, Phillip M., additional, Basu, Joydeep, additional, Beasley, Val R., additional, Berridge, Brian R., additional, Bertram, Timothy A., additional, Bhang, Hyo-eun, additional, Black, Hugh E., additional, Bolon, Brad, additional, Boorman, Gary A., additional, Bounous, Denise I., additional, Boyce, Rogely Waite, additional, Bracken, William M., additional, Brix, Amy E., additional, Brown, Danielle, additional, Butt, Mark T., additional, Cantor, Glenn H., additional, Car, Bruce D., additional, Castranova, Vincent, additional, Cattley, Russell C., additional, Chan, Curtis, additional, Chapin, Robert E., additional, Cohen, Samuel M., additional, Colegate, Steve, additional, Cook, Daniel, additional, Cooke, Paul S., additional, Crabbs, Torrie A., additional, Creasy, Dianne M., additional, Crissman, James W., additional, Cullen, John M., additional, Danilenko, Dimitry M., additional, Davis, Barbara, additional, Davis, Myrtle A., additional, Davis, T. Zane, additional, DeLellis, Ronald A., additional, Denslow, Nancy D., additional, Diegel, Kelly L., additional, Dorman, David C., additional, Dubielzig, Richard R., additional, Durham, Stephen K., additional, Eldridge, Sandy, additional, Elmore, Susan A., additional, Everitt, Jeffrey I., additional, Fenton, Suzanne, additional, Ferguson, Duncan C., additional, Field, Reuel, additional, Foley, George L., additional, Foster, William R., additional, Frantz, Jerry D., additional, Gabrielson, Kathy, additional, Gad, Shayne C., additional, Galbreath, Elizabeth J., additional, Gardner, Dale R., additional, Garman, Robert H., additional, Gill, Santokh, additional, Glerup, Peter, additional, Goad, Dale L., additional, Pecquet Goad, Mary Elizabeth, additional, Grand, Nanna, additional, Green, Benjamin T., additional, Gropp, Kathryn E., additional, Gundersen, Hans Jørgen G., additional, Gunson, Diane, additional, Gupta, Ramesh C., additional, Gwaltney-Brant, Sharon M., additional, Hall, Jeffery O., additional, Halpern, Wendy, additional, Hard, Gordon C., additional, Hardisty, Jerry F., additional, Harkema, Jack R., additional, Harvey, Philip W., additional, Haschek, Wanda M., additional, Heinz-Taheny, Kathleen, additional, Herbert, Ronald A., additional, Herman, Eugene, additional, Hoenerhoff, Mark, additional, Hubbs, Ann, additional, Hutto, David, additional, Janovitz, Evan B., additional, Khan, Kanwar Nasir M., additional, Keenan, Kevin P., additional, Kerlin, Roy L., additional, Kreeger, John M., additional, Krishnan, Kannan, additional, Kuper, C. Frieke, additional, Lee, Stephen T., additional, Lehman-McKeeman, Lois D., additional, Li, Xiantang, additional, Lombardini, Eric D., additional, Louden, Calvert, additional, Ludlow, John W., additional, Malarkey, David E., additional, Mann, Peter C., additional, Maronpot, Robert R., additional, McDorman, Kevin S., additional, Melanson, Mark A., additional, Mercer, Robert, additional, Mirabile, Rosanna, additional, Moch, Ronald W., additional, Morrison, James P., additional, Morton, Daniel, additional, Morton, Laura Dill, additional, Muthupalani, Sureshkumar, additional, Nikula, Kristen J., additional, Ochoa, Ricardo, additional, Pacheco-Thompson, Michelle E., additional, Pulido, Olga M., additional, Panter, Kip E., additional, Parker, George A., additional, Porter, Dale W., additional, Patterson, Douglas Reid, additional, Pfister, James A., additional, Pinkert, Carl A., additional, Ramaiah, Lila, additional, Rao, Deepa B., additional, Robertson, Donald G., additional, Rojko, Jennifer, additional, Rosol, Thomas J., additional, Rousseaux, Colin G., additional, Rudmann, Daniel G., additional, Ruehl-Fehlert, Christine, additional, Sargent, Linda, additional, Satterwhite, Christina M., additional, Schafer, Kenneth A., additional, Solter, Philip F., additional, Sills, Robert C., additional, Simon, Liz, additional, Skydsgaard, Mikala, additional, Smith, Graham S., additional, Sriram, Krishnan, additional, Stegelmeier, Bryan L., additional, Sullivan, John M., additional, Sutcliffe, Catherine, additional, Swenberg, James A., additional, Sysa-Shah, Polina, additional, Teixeira, Leandro, additional, Tsuchiya, Noriko, additional, Vahle, John L., additional, Van Vleet, John F., additional, Varela, Aurore, additional, Voss, Kenneth A., additional, Walker, Robin M., additional, Wallig, Matthew A., additional, Walter, Gail L., additional, Welch, Kevin D., additional, White, Paul, additional, Winkelmann, Christopher T., additional, Wojcinski, Zbigniew W., additional, and Wolf, Jeffrey C., additional

Published
2013
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19. Contributors

Author

Argyle, David J., primary, Avery, Anne C., additional, Bergman, Philip J., additional, Bonnett, Brenda N., additional, Butler, Lesley M., additional, Clifford, Craig A., additional, Culp, William T.N., additional, Dewey, Curtis W., additional, Dow, Steven, additional, Dubielzig, Richard R., additional, Ehrhart, E.J., additional, Ehrhart, Nicole P., additional, Fan, Timothy M., additional, Farese, James P., additional, Forrest, Lisa J., additional, Friedrichs, Kristen R., additional, Garrett, Laura D., additional, Goldschmidt, Michael H., additional, Gordon, Ira K., additional, Gustafson, Daniel L., additional, Guth, Amanda M., additional, Hauck, Marlene L., additional, Henry, Carolyn J., additional, Kamstock, Debra A., additional, Kent, Michael S., additional, Khanna, Chand, additional, Kisseberth, William C., additional, Knapp, Deborah W., additional, Kraft, Susan L., additional, Lana, Susan E., additional, LaRue, Susan M., additional, Lascelles, B. Duncan X., additional, Lawrence, Jessica A., additional, Liptak, Julius M., additional, London, Cheryl A., additional, Lunn, Katharine F., additional, Macy, Dennis W., additional, McEntee, Margaret C., additional, McMillan, Sarah K., additional, Miller, Paul E., additional, Modiano, Jaime F., additional, Moore, Peter F., additional, Mutsaers, Anthony J., additional, Olver, Christine, additional, Page, Rodney L., additional, Paoloni, Melissa C., additional, Pinkerton, Marie E., additional, Powers, Barbara E., additional, Rebhun, Robert B., additional, Robinson, Narda G., additional, Ryan, Stewart D., additional, Saba, Corey F., additional, Selting, Kim A., additional, Shaw, Jane R., additional, Skorupski, Katherine A., additional, Sorenmo, Karin U., additional, de Mello Souza, Carlos Henrique, additional, Thamm, Douglas H., additional, Turek, Michelle M., additional, Vail, David M., additional, Wakshlag, Joseph J., additional, Withrow, Stephen J., additional, Woods, J. Paul, additional, Worley, Deanna R., additional, and Young, Karen M., additional

Published
2013
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20. Eye

Author

Teixeira, Leandro, primary and Dubielzig, Richard R., additional

Published
2013
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22. Ocular anatomy and correlation with histopathologic findings in two common octopuses ( Octopus vulgaris ) and one giant Pacific octopus ( Enteroctopus dofleini ) diagnosed with inflammatory phakitis and retinitis

Author

Linde Henriksen, Michala, primary, Ofri, Ron, additional, Shomrat, Tal, additional, Nesher, Nir, additional, Cleymaet, Allison, additional, Ross, Maya, additional, Pe’er, Oren, additional, Arad, Dikla, additional, Katzenbach, Julia, additional, and Dubielzig, Richard R., additional

Published
2021
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25. The Retina

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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27. Diseases of the Lens

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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29. The Glaucomas

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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32. Non-surgical trauma

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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33. Introduction

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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34. Diseases of the orbit

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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36. The uvea

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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37. The Optic Nerve

Author

Dubielzig, Richard R., primary, Ketring, Kerry, additional, McLellan, Gillian J., additional, and Albert, Daniel M., additional

Published
2010
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40. Clinical and pathologic evaluation of chorioretinal lesions in wild owl species.

Author

Keenan, Alessandra V., Oster, Seth, McMullen, Richard J., Shaw, Gillian C., Dubielzig, Richard R., Teixeira, Leandro B. C., Bellah, Jamie R., Moore, Phillip A., and Boveland, Shannon D.

Subjects
AVIAN influenza, WEST Nile virus, OPTICAL coherence tomography, BLOOD cell count, OWLS, RETINAL detachment, TONOMETERS
Abstract

Objective: Investigate histopathology and spectral‐domain optical coherence tomography (OCT) imaging of wild owls with chorioretinitis and identify any potential correlation with an infectious etiology. Materials and Methods: Ophthalmic examination and retinal OCT imaging were performed on fifteen great horned (Strix varia) and barred (Bubo virginianus) owls (30 eyes) with chorioretinitis and five owls with normal eyes (10 eyes). Testing to investigate the presence of potential infectious diseases included a complete blood count, biochemistry, protein electrophoresis, West Nile virus (WNV) plaque reduction neutralization test, Toxoplasma gondii modified direct agglutination test, WNV RT‐PCR, and Avian Influenza RT‐PCR. A necropsy was performed on all owls, including ocular histopathology. Results: Fundus lesions included retinal detachment (7/15 owls), depigmented lesions (12/15), pigment clumping (8/15), and retinal tear (4/15). All birds were negative for WNV and Avian Influenza on RT‐PCR. Of the owls with chorioretinitis, 3/15 were seropositive for WNV and 7/15 for T. gondii. Optical coherence tomography of 25/30 affected eyes revealed outer retinal lesions (19/25 eyes), retinal detachment (16/25), and retinal tears (3/25). Histopathological examination revealed outer nuclear layer atrophy (19/30 eyes), retinal detachment (18/30), retinal tears (7/30), suprachoroidal hemorrhage (12/30), scleral rupture (3/30), and ossicle fracture (3/30). Conclusions: Although 20% of birds were seropositive for WNV and 46.6% for T. gondii, histopathologic findings supported that the posterior segment lesions in the study group were likely due to blunt ocular trauma rather than an infectious etiology. The results of OCT imaging and histopathology documented retinal changes most consistent with blunt ocular trauma. [ABSTRACT FROM AUTHOR]

Published
2022
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43. Metastases

Author

Dubielzig, Richard R., primary, Grendahl, Robin L., additional, Orcutt, James C., additional, Syed, Nasreen A., additional, and Simons, Kenneth B., additional

Published
2008
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