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9. A Nonsynonymous Change in Adhesion G Protein–Coupled Receptor L3 Associated With Risk for Equine Degenerative Myeloencephalopathy in the Caspian Horse

Author

Posbergh, C J, Pollott, G E, Southard, T L, Divers, T J, and Brooks, S A

Abstract

Equine degenerative myeloencephalopathy (EDM), a neurological disease of young horses, causes progressive development of symmetric ataxia predominantly in the pelvic limbs. Equine degenerative myeloencephalopathy is likely inherited and with no known treatment affected horses frequently need euthanasia. Alpha-tocopherol deficiency during early life appears to contribute to the phenotype. This study sought to identify any genetic variants correlated with EDM in Caspian foals. Two half-sibling EDM-diagnosed cases were genotyped at 52,063 loci and evaluated by the Autozygosity by Difference statistic. Additional horses not affected by EDM were used for genetic comparison to identify regions unique to the case phenotype. The associated region on chromosome 3 contains only one gene encoding adhesion G protein–coupled receptor L3 (ADGRL3). Adhesion G protein–coupled receptor L3 is a member of the latrophilin subfamily of G protein–coupled receptors and may contribute to attention deficit/hyperactivity disorder in humans and hyperactive motor function in mice and zebrafish. Analysis of the predicted coding regions for Equine ADGRL3 in affected horses revealed a nonsynonymous single nucleotide polymorphism at Chr3:71,917,591 bp. Caspian and Caspian cross-relatives (n = 81) of the two initial cases and unrelated horses from similar breeds (n = 130, including Arabians, American Miniatures, and Shetlands) possessed this allele at 5% frequency, with no homozygotes observed within the non-Caspian breeds. This study suggests that a polymorphism in ADGRL3 could contribute to a genetic predisposition to Caspian horse EDM.

Published
2018

11. Comparative Oncogenomics Implicates the Neurofibromin 1 Gene (NF1) as a Breast Cancer Driver

Author

Fallon, B. L., Southard, T. L., Pfefferle, A. D., Schimenti, J. C., McNairn, A. J., Cerami, E. G., Wallace, M. D., Rinaldi, V. D., Perou, C. M., and Shen, L.

Abstract

Identifying genomic alterations driving breast cancer is complicated by tumor diversity and genetic heterogeneity. Relevant mouse models are powerful for untangling this problem because such heterogeneity can be controlled. Inbred Chaos3 mice exhibit high levels of genomic instability leading to mammary tumors that have tumor gene expression profiles closely resembling mature human mammary luminal cell signatures. We genomically characterized mammary adenocarcinomas from these mice to identify cancer-causing genomic events that overlap common alterations in human breast cancer. Chaos3 tumors underwent recurrent copy number alterations (CNAs), particularly deletion of the RAS inhibitor Neurofibromin 1 (Nf1) in nearly all cases. These overlap with human CNAs including NF1, which is deleted or mutated in 27.7% of all breast carcinomas. Chaos3 mammary tumor cells exhibit RAS hyperactivation and increased sensitivity to RAS pathway inhibitors. These results indicate that spontaneous NF1 loss can drive breast cancer. This should be informative for treatment of the significant fraction of patients whose tumors bear NF1 mutations.

Published
2012
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13. HUS1 regulates in vivo responses to genotoxic chemotherapies

Author

Balmus, G, primary, Lim, P X, additional, Oswald, A, additional, Hume, K R, additional, Cassano, A, additional, Pierre, J, additional, Hill, A, additional, Huang, W, additional, August, A, additional, Stokol, T, additional, Southard, T, additional, and Weiss, R S, additional

Published
2015
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16. DNA damage is a feature of feline injection-site sarcoma.

Author

Kang, S., Southard, T., and Hume, K. R.

Subjects
*DNA damage, *RADIOTHERAPY, *IMMUNOHISTOCHEMISTRY, *SARCOMA, *TISSUES, *CANCER
Abstract

Feline injection-site sarcoma ( FISS) is commonly treated with surgery and radiation therapy. Despite aggressive therapy, FISS has a high recurrence rate. The true benefit of adjuvant chemotherapy is not known. DNA damage response mechanisms help protect against genomic instability but can also promote chemoresistance. In order to determine whether DNA damage is a feature of FISS, we evaluated tumour tissues with γH2AX immunohistochemistry. H2AX is phosphorylated to form γH2AX following DNA double strand breaks. Seventeen FISS specimens were evaluated prospectively. DNA damage ranged from 2.18 to33.7%, with a median of 16.2%. Significant differences were noted between cats ( P < 0.0001). Mitotic index ranged from 0 to 57 with a median of 13 and did not correlate with γH2AX positivity ( P = 0.2). Further studies are needed to determine if γH2AX expression may predict chemosensitivity and have independent value as a prognostic factor. [ABSTRACT FROM AUTHOR]

Published
2017
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17. Parelaphostrongylus tenuis Cerebrospinal Nematodiasis in a Horse with Cervical Scoliosis and Meningomyelitis.

Author

Mittelman, N.S., Divers, T.J., Engiles, J.B., Gerhold, R., Ness, S., Scrivani, P.V., Southard, T., and Johnson, A.L.

Subjects
PARELAPHOSTRONGYLUS tenuis, HORSE diseases, SCOLIOSIS, POLYMERASE chain reaction, MYELITIS
Abstract

There are reports of horses with acute onset acquired cervical scoliosis and cutaneous analgesia. The underlying dorsal gray column myelitis that produces these neurologic signs has been only presumptively attributed to migration of Parelaphostrongylus tenuis within the spinal cord. Despite previous confirmation brain by polymerase chain reaction testing, of P. tenuis within the brain of horses by polymerase chain reaction testing, genetic testing has failed to definitively identify the presence of this parasite in cases of equine myelitis. This case report provides molecular confirmation via polymerase chain reaction of P. tenuis within the cervical spinal cord of a horse with scoliosis and cutaneous analgesia. [ABSTRACT FROM AUTHOR]

Published
2017
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22. Candidate Gene Analyses of Skeletal Variation in Malocclusion.

Author

da Fontoura, C. S. G., Miller, S. F., Wehby, G. L., Amendt, B. A., Holton, N. E., Southard, T. E., Allareddy, V., and Moreno Uribe, L. M.

Subjects
MALOCCLUSION, DNA analysis, CEPHALOMETRY, PRINCIPAL components analysis, PHENOTYPES, ODDS ratio, GENETIC polymorphisms, REGRESSION analysis
Abstract

This study evaluated associations between craniofacial candidate genes and skeletal variation in patients with malocclusion. Lateral cephalometric radiographs of 269 untreated adults with skeletal classes I, II, and III malocclusion were digitized with 14 landmarks. Two-dimensional coordinates were analyzed using Procrustes fit and principal component (PC) analysis to generate continuous malocclusion phenotypes. Skeletal class classifications (I, II, or III) were used as a categorical phenotype. Individuals were genotyped for 198 singlenucleotide polymorphisms (SNPs) in 71 craniofacial genes and loci. Phenotype-genotype associations were tested via multivariate linear regression for continuous phenotypes and multinomial logistic regression for skeletal malocclusion class. PC analysis resulted in 4 principal components (PCs) explaining 69% of the total skeletal facial variation. PC1 explained 32.7% of the variation and depicted vertical discrepancies ranging from skeletal deep to open bites. PC1 was associated with a SNP near PAX5 (P = 0.01). PC2 explained 21.7% and captured horizontal maxillomandibular discrepancies. PC2 was associated with SNPs upstream of SNAI3 (P = 0.0002) and MYO1H (P = 0.006). PC3 explained 8.2% and captured variation in ramus height, body length, and anterior cranial base orientation. PC3 was associated with TWIST1 (P = 0.000076). Finally, PC4 explained 6.6% and detected variation in condylar inclination as well as symphysis projection. PC4 was associated with PAX7 (P = 0.007). Furthermore, skeletal class II risk increased relative to class I with the minor alleles of SNPs in FGFR2 (odds ratio [OR] = 2.1, P = 0.004) and declined with SNPs in EDN1 (OR = 0.5, P = 0.007). Conversely, skeletal class III risk increased versus class I with SNPs in FGFR2 (OR 2.2, P = 0.005) and COL1A1 (OR = 2.1, P = 0.008) and declined with SNPs in TBX5 (OR = 0.5, P = 0.014). PAX5, SNAI3, MYO1H, TWIST1, and PAX7 are associated with craniofacial skeletal variation among patients with malocclusion, while FGFR2, EDN1, TBX5, and COL1A1 are associated with type of skeletal malocclusion. [ABSTRACT FROM AUTHOR]

Published
2015
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23. HUS1 regulates in vivoresponses to genotoxic chemotherapies

Author

Balmus, G, Lim, P X, Oswald, A, Hume, K R, Cassano, A, Pierre, J, Hill, A, Huang, W, August, A, Stokol, T, Southard, T, and Weiss, R S

Abstract

Cells are under constant attack from genotoxins and rely on a multifaceted DNA damage response (DDR) network to maintain genomic integrity. Central to the DDR are the ATM and ATR kinases, which respond primarily to double-strand DNA breaks (DSBs) and replication stress, respectively. Optimal ATR signaling requires the RAD9A-RAD1-HUS1 (9-1-1) complex, a toroidal clamp that is loaded at damage sites and scaffolds signaling and repair factors. Whereas complete ATR pathway inactivation causes embryonic lethality, partial Hus1impairment has been accomplished in adult mice using hypomorphic (Hus1neo) and null (Hus1Δ1) Hus1alleles, and here we use this system to define the tissue- and cell type-specific actions of the HUS1-mediated DDR in vivo. Hus1neo/Δ1mice showed hypersensitivity to agents that cause replication stress, including the crosslinking agent mitomycin C (MMC) and the replication inhibitor hydroxyurea, but not the DSB inducer ionizing radiation. Analysis of tissue morphology, genomic instability, cell proliferation and apoptosis revealed that MMC treatment caused severe damage in highly replicating tissues of mice with partial Hus1inactivation. The role of the 9-1-1 complex in responding to MMC was partially ATR-independent, as a HUS1 mutant that was proficient for ATR-induced checkpoint kinase 1 phosphorylation nevertheless conferred MMC hypersensitivity. To assess the interplay between the ATM and ATR pathways in responding to replication stress in vivo, we used Hus1/Atmdouble mutant mice. Whereas Hus1neo/neoand Atm−/−single mutant mice survived low-dose MMC similar to wild-type controls, Hus1neo/neoAtm−/−double mutants showed striking MMC hypersensitivity, consistent with a model in which MMC exposure in the context of Hus1dysfunction results in DSBs to which the ATM pathway normally responds. This improved understanding of the inter-dependency between two major DDR mechanisms during the response to a conventional chemotherapeutic illustrates how inhibition of checkpoint factors such as HUS1 may be effective for the treatment of ATM-deficient and other cancers.

Published
2016
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24. Spontaneous Unilateral Brainstem Infarction in Swiss Mice.

Author

Southard, T. and Brayton, C. F.

Subjects
INFARCTION, BRAIN stem diseases, LABORATORY mice, SEROLOGY, PRECANCEROUS conditions
Abstract

The article discusses a research study on Swiss mice with spontaneous unilateral brainstem infarction. Presented for necropsy service were eleven noninbred female mice with signs of acute vestibular syndrome after being euthanized with carbon dioxide and blood collected through cardiocentesis for serology. The study indicated that the vestibular signs on the 11 mice were secondary to lateral brainstem infarction and identified lesions in mice have similar Wallenberg lateral medullary syndrome features common in human brainstem infarcts.

Published
2011
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25. The Relationship Between the Density of the Alveolar Processes and that of Post-Cranial Bone.

Author

Southard, K. A., Southard, T. E., Schlechte, J. A., and Meis, P. A.

Subjects
ALVEOLAR process, DENTAL arch, BONE density, HUMAN body composition, MUSCULOSKELETAL system, MAXILLA, JAWS, MANDIBLE
Abstract

Skeletal mass declines in all populations with age, and the literature suggests that changes in oral bone may be linked to the status of the post-cranial (systemic) skeleton. However, there is a lack of information defining the relationship between alveolar process bone and the post-cranial skeleton in healthy individuals. The purpose of this study was to determine: (1) if the bone densities of the maxillary and mandibular alveolar processes are related to the bone density of the spine, hip, or radius in healthy women; and (2) if the alveolar process densities decline with age. Forty-one dentate Caucasian women aged 20 to 78 years underwent assessment of post-cranial (systemic) and alveolar process bone. D-speed vertical bitewing and periapical radiographs incorporating aluminum stepwedges, controlled exposure and processing conditions, and a density correction algorithm were used to make alveolar process density assessments with regions of interest (ROIs) apical to crestal bone and intrabony defects. Anteroposterior lumbar (LI to L4) and lateral lumbar (L2 to L4) spine, total hip (and subregions), and radius bone densities were determined by dual-energy x-ray absorptiometry (DEXA). Correlation analysis revealed significant relationships between maxillary alveolar process bone density and the density of the mandibular alveolar process (r = 0.57, p ≤ 0.001), anteroposterior lumbar spine (r = 0.53, p ≤ 0.001), lateral lumbar spine (r = 0.52, p ≤ 0.001), total hip (r = 0.39, p = 0.01), total radius (r = 0.39, p = 0.01), and age (r = -0.38, p =0.01). A two-tailed t test comparison revealed significantly greater maxillary alveolar process bone density in women younger than 50 years of age than in those 50 and older (p ≤ 0.01). We conclude that the density of maxillary alveolar process bone is significantly related to the density of the mandibular alveolar process, lumbar spine, hip, and radius in healthy women and that maxillary alveolar process bone density declines with age. [ABSTRACT FROM AUTHOR]

Published
2000
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26. Variation of Approximal Tooth Contact Tightness with Postural Change.

Author

SOUTHARD, T. E., SOUTHARD, K. A., and TOLLEY, E. A.

Subjects
DIASTEMA (Teeth), DENTAL occlusion, MALOCCLUSION, MAXILLARY expansion, RETROMAXILLARY space, JAW physiology, DENTAL research, TEETH abnormalities, POSTURE
Abstract

In order to investigate the role played by posture in determining posterior dental contact tightness, we measured contact tightness of maxillary and mandibular posterior teeth in ten adult subjects, while each was initially seated upright, after each had assumed a supine posture for two h, and finally after each had returned to an upright posture for two h. The technique used for measurement of contact tightness was based on frictional force concepts and consisted of the recording of the force required to withdraw a 0.038-mm-thick stainless-steel strip that had been slipped into each contact. A decreased mean tightness of all maxillary and mandibular contacts followed the change from an upright to a supine posture. The most significant decrease ( -32%) occurred at the mandibular first molar-second premolar contact, and the smallest decrease (- 10%) occurred at the mandibular first premolar-canine contact. An increased mean tightness of all maxillary and mandibular contacts followed a return to an upright posture. The most significant increase (20%) occurred at the maxillary first molar-second premolar contact, and the smallest increase (8%) occurred at the maxillary first premolar-canine contact. We conclude that posterior dental contact tightness, generally regarded by dentists as a static feature of occlusion, varies significantly as a function of posture. [ABSTRACT FROM AUTHOR]

Published
1990
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27. Naturally Occurring Parelaphostrongylus tenuis–Associated Choriomeningitis in a Guinea Pig With Neurologic Signs.

Author

Southard, T., Bender, H., Wade, S. E., Grunenwald, C., and Gerhold, R. W.

Subjects
GUINEA pigs, PARELAPHOSTRONGYLUS tenuis, LYMPHOCYTIC choriomeningitis, HINDLIMB, PARALYSIS, WHITE-tailed deer, POLYMERASE chain reaction, DISEASES
Abstract

An adult male guinea pig (Cavia porcellus) with a 1-month history of hind limb paresis, torticollis, and seizures was euthanized and submitted for necropsy. Gross examination was unremarkable, but histologic examination revealed multifocal eosinophilic and lymphoplasmacytic choriomeningitis and cross sections of nematode parasites within the leptomeninges of the midbrain and diencephalon. Morphologic features of the nematode were consistent with a metastrongyle, and the parasite was identified as Parelaphostrongylus tenuis by polymerase chain reaction testing and nucleotide sequencing. Further questioning of the owner revealed that the guinea pig was fed grass from a yard often grazed by white-tailed deer (Odocoileus virginianus). To the authors’ knowledge, this is the first report of a naturally occurring P. tenuis infection in a guinea pig. [ABSTRACT FROM PUBLISHER]

Published
2013
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31. Sleep in Kcna2 knockout mice

Author

Messing Albee, Chiu Shing-Yan, Southard Teresa, Vyazovskiy Vladyslav, Douglas Christopher L, Tononi Giulio, and Cirelli Chiara

Subjects
Biology (General), QH301-705.5
Abstract

Abstract Background Shaker codes for a Drosophila voltage-dependent potassium channel. Flies carrying Shaker null or hypomorphic mutations sleep 3–4 h/day instead of 8–14 h/day as their wild-type siblings do. Shaker-like channels are conserved across species but it is unknown whether they affect sleep in mammals. To address this issue, we studied sleep in Kcna2 knockout (KO) mice. Kcna2 codes for Kv1.2, the alpha subunit of a Shaker-like voltage-dependent potassium channel with high expression in the mammalian thalamocortical system. Results Continuous (24 h) electroencephalograph (EEG), electromyogram (EMG), and video recordings were used to measure sleep and waking in Kcna2 KO, heterozygous (HZ) and wild-type (WT) pups (P17) and HZ and WT adult mice (P67). Sleep stages were scored visually based on 4-s epochs. EEG power spectra (0–20 Hz) were calculated on consecutive 4-s epochs. KO pups die by P28 due to generalized seizures. At P17 seizures are either absent or very rare in KO pups (< 1% of the 24-h recording time), and abnormal EEG activity is only present during the seizure. KO pups have significantly less non-rapid eye movement (NREM) sleep (-23%) and significantly more waking (+21%) than HZ and WT siblings with no change in rapid eye movement (REM) sleep time. The decrease in NREM sleep is due to an increase in the number of waking episodes, with no change in number or duration of sleep episodes. Sleep patterns, daily amounts of sleep and waking, and the response to 6 h sleep deprivation are similar in HZ and WT adult mice. Conclusion Kv1.2, a mammalian homologue of Shaker, regulates neuronal excitability and affects NREM sleep.

Published
2007
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33. Evaluation of an ultrasound-guided freeze-core biopsy system for canine and feline brain tumors.

Author

Adams BS, Marino DJ, Loughin CA, Marino LJ, Southard T, Lesser ML, Akerman M, and Roynard P

Abstract

Objective: To determine if a single brain biopsy utilizing a freeze-core needle harvest system Cassi II under ultrasound guidance provides a diagnostic sample; to evaluate the technique's efficacy in procuring diagnostic samples in comparison with "open" surgical biopsies; and to describe intraoperative complications associated with the technique., Study Design: Experimental clinical study., Animals: Seventeen dogs and four cats with magnetic resonance imaging (MRI) diagnoses of readily surgically accessible intracranial masses., Methods: Immediately prior to surgical biopsy (SB), freeze-core biopsy (FCB) sample was obtained from each patient under ultrasound guidance., Results: Histopathology results from single FCB samples were found to be in 100% agreement with the SB samples. Freezing artifact was minimal and did not interfere with histopathologic interpretation. There were no intraoperative complications specifically attributable to the use of the FCB system., Conclusion: Based on the results of this small experimental study, the FCB system is expected to safely yield diagnostic quality intracranial masses biopsy specimens., Clinical Significance: This system has the potential of obtaining diagnostic biopsies of more deeply seated brain lesions (i.e., intra-axial tumors considered inaccessible or with large risks/difficulties by standard surgical means) which would provide a definitive diagnosis to guide appropriate therapy., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Adams, Marino, Loughin, Marino, Southard, Lesser, Akerman and Roynard.)

Published
2024
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34. A Gamma-adapted subunit vaccine induces broadly neutralizing antibodies against SARS-CoV-2 variants and protects mice from infection.

Author

Coria LM, Rodriguez JM, Demaria A, Bruno LA, Medrano MR, Castro CP, Castro EF, Del Priore SA, Hernando Insua AC, Kaufmann IG, Saposnik LM, Stone WB, Prado L, Notaro US, Amweg AN, Diaz PU, Avaro M, Ortega H, Ceballos A, Krum V, Zurvarra FM, Sidabra JE, Drehe I, Baqué JA, Li Causi M, De Nichilo AV, Payes CJ, Southard T, Vega JC, Auguste AJ, Álvarez DE, Flo JM, Pasquevich KA, and Cassataro J

Subjects
Animals, Mice, Humans, Broadly Neutralizing Antibodies, COVID-19 Vaccines, Vaccines, Subunit, Adjuvants, Immunologic, Epitopes, B-Lymphocyte, Antibodies, Viral, Antibodies, Neutralizing, Spike Glycoprotein, Coronavirus genetics, SARS-CoV-2, COVID-19 prevention & control
Abstract

In the context of continuous emergence of SARS-CoV-2 variants of concern (VOCs), one strategy to prevent the severe outcomes of COVID-19 is developing safe and effective broad-spectrum vaccines. Here, we present preclinical studies of a RBD vaccine derived from the Gamma SARS-CoV-2 variant adjuvanted with Alum. The Gamma-adapted RBD vaccine is more immunogenic than the Ancestral RBD vaccine in terms of inducing broader neutralizing antibodies. The Gamma RBD presents more immunogenic B-cell restricted epitopes and induces a higher proportion of specific-B cells and plasmablasts than the Ancestral RBD version. The Gamma-adapted vaccine induces antigen specific T cell immune responses and confers protection against Ancestral and Omicron BA.5 SARS-CoV-2 challenge in mice. Moreover, the Gamma RBD vaccine induces higher and broader neutralizing antibody activity than homologous booster vaccination in mice previously primed with different SARS-CoV-2 vaccine platforms. Our study indicates that the adjuvanted Gamma RBD vaccine is highly immunogenic and a broad-spectrum vaccine candidate., (© 2024. The Author(s).)

Published
2024
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35. Extreme plasticity of reproductive state in a female rodent.

Author

Freeman AR, Lee DN, Allen JJ, Blank B, Jeffery D, Lerer A, Singh B, Southard T, Cheong SH, and Ophir AG

Subjects
Animals, Female, Muridae, Estradiol, Biological Evolution, Reproduction, Estrogens
Abstract

Successful sexual reproduction relies on the coordination of multiple biological systems, yet traditional concepts of biological sex often ignore the natural plasticity in morphology and physiology underlying sex. Most female mammals develop a patent (i.e., opened) vaginal entrance (introitus) prenatally or postnatally before or during puberty, usually under the influence of estrogens, and remain patent for the remainder of their lifespan 1 . An exception is the southern African giant pouched rat (Cricetomys ansorgei), whose vaginal introitus remains sealed well into adulthood 2 . Here, we explore this phenomenon and report that the reproductive organs and the vaginal introitus can undergo astounding and reversible transformation. Non-patency is characterized by reduced uterine size and the presence of a sealed vaginal introitus. Furthermore, the female urine metabolome shows that patent and non-patent females profoundly differ in their urine content, a reflection of differences in physiology and metabolism. Surprisingly, patency state did not predict fecal estradiol or progesterone metabolite concentrations. Exploring the plasticity that exists in reproductive anatomy and physiology can uncover that traits long considered 'fixed' in adulthood can become plastic under specific evolutionary pressures. Moreover, the barriers to reproduction that such plasticity creates present unique challenges to maximizing reproductive potential., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published
2023
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36. Acute kidney injury in dogs following ingestion of cream of tartar and tamarinds and the connection to tartaric acid as the proposed toxic principle in grapes and raisins.

Author

Wegenast CA, Meadows ID, Anderson RE, Southard T, González Barrientos CR, and Wismer TA

Subjects
Dogs, Animals, Dental Calculus veterinary, Eating, Vitis, Tamarindus, Dog Diseases chemically induced, Acute Kidney Injury chemically induced, Acute Kidney Injury veterinary
Abstract

Objective: To (1) describe exposure history, clinical signs, treatment, and diagnostic findings in 4 dogs following ingestion of tamarinds, and in 2 dogs following ingestion of cream of tartar, and (2) discuss tartaric acid, the common denominator, as the proposed toxic principle in tamarinds and grapes., Series Summary: Reports in which dogs developed acute kidney injury following ingestion of cream of tartar or tamarinds were identified from the ASPCA Animal Poison Control Center electronic database. In these cases, decontamination was not performed, and treatments were delayed. Despite IV fluids and symptomatic and supportive care, 2 of the dogs became anuric and 1 became oliguric. Four dogs were euthanized, and the outcome is unknown for 2 of the dogs. Necropsies were performed on 3 of the dogs. Clinical signs, laboratory findings, and histopathologic lesions were similar to those reported in grape and raisin toxicosis., New or Unique Information Provided: Acute kidney injury may develop following ingestion of cream of tartar or tamarinds in dogs. Connecting these reports with findings in grape and raisin toxicosis and the sensitivity to tartaric acid in dogs, tartaric acid is identified as the likely toxic component in grapes and tamarinds., (© Veterinary Emergency and Critical Care Society 2022.)

Published
2022
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37. Investigation of SARS-CoV-2 infection and associated lesions in exotic and companion animals.

Author

Rotstein DS, Peloquin S, Proia K, Hart E, Lee J, Vyhnal KK, Sasaki E, Balamayooran G, Asin J, Southard T, Rothfeldt L, Venkat H, Mundschenk P, McDermott D, Crossley B, Ferro P, Gomez G, Henderson EH, Narayan P, Paulsen DB, Rekant S, Schroeder ME, Tell RM, Torchetti MK, Uzal FA, Carpenter A, and Ghai R

Subjects
Animals, Dogs, Pets, SARS-CoV-2, COVID-19 veterinary, Dog Diseases diagnosis, One Health
Abstract

Documented natural infections with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in exotic and companion animals following human exposures are uncommon. Those documented in animals are typically mild and self-limiting, and infected animals have only infrequently died or been euthanized. Through a coordinated One Health initiative, necropsies were conducted on 5 animals from different premises that were exposed to humans with laboratory-confirmed SARS-CoV-2 infection. The combination of epidemiologic evidence of exposure and confirmatory real-time reverse transcriptase-polymerase chain reaction testing confirmed infection in 3 cats and a tiger. A dog was a suspect case based on epidemiologic evidence of exposure but tested negative for SARS-CoV-2. Four animals had respiratory clinical signs that developed 2 to 12 days after exposure. The dog had bronchointerstitial pneumonia and the tiger had bronchopneumonia; both had syncytial-like cells with no detection of SARS-CoV-2. Individual findings in the 3 cats included metastatic mammary carcinoma, congenital renal disease, and myocardial disease. Based on the necropsy findings and a standardized algorithm, SARS-CoV-2 infection was not considered the cause of death in any of the cases. Continued surveillance and necropsy examination of animals with fatal outcomes will further our understanding of natural SARS-CoV-2 infection in animals and the potential role of the virus in development of lesions.

Published
2022
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39. Myocardial protein aggregates in pet guinea pigs.

Author

Southard T, Kelly K, and Armien AG

Subjects
Actins, Animals, Female, Guinea Pigs, Male, Myocardium, Retrospective Studies, Muscle, Skeletal, Protein Aggregates
Abstract

A retrospective study of guinea pigs submitted for necropsy revealed intracytoplasmic inclusions in the cardiomyocytes of 26 of 30 animals. The inclusions were found with approximately the same frequency in male and female guinea pigs and were slightly more common in older animals. In most cases, the animals did not have clinical signs or necropsy findings suggestive of heart failure, and the cause of death or reason for euthanasia was attributed to concurrent disease processes. However, the 4 guinea pigs with the highest inclusion body burden all had pulmonary edema, sometimes with intra-alveolar hemosiderin-laden macrophages, suggestive of heart failure. The inclusions were found in both the left and right ventricular myocardium, mainly in the papillary muscles, but were most common in the right ventricular free wall. No inclusions were detected in the atrial myocardium or in skeletal muscle. The inclusions did not stain with Congo red or periodic acid-Schiff. Electron microscopy revealed dense aggregates of disorganized myofilaments and microtubules that displaced and compressed the adjacent organelles. By immunohistochemistry, there was some scattered immunoreactivity for desmin and actin at the periphery of the inclusions and punctate actin reactivity within the aggregates. The inclusions did not react with antibodies to ubiquitin or cardiac myosin, but were variably reactive for alpha B crystallin, a small heat shock chaperone protein. The inclusions were interpreted as evidence of impaired proteostasis.

Published
2022
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40. Pharmacological and genetic perturbation establish SIRT5 as a promising target in breast cancer.

Author

Abril YLN, Fernandez IR, Hong JY, Chiang YL, Kutateladze DA, Zhao Q, Yang M, Hu J, Sadhukhan S, Li B, He B, Remick B, Bai JJ, Mullmann J, Wang F, Maymi V, Dhawan R, Auwerx J, Southard T, Cerione RA, Lin H, and Weiss RS

Subjects
Animals, Breast Neoplasms genetics, Breast Neoplasms pathology, Cell Line, Tumor, Enzyme Inhibitors pharmacology, Female, Heterografts, Humans, Isocitrate Dehydrogenase antagonists & inhibitors, Mice, Mice, Knockout, Oxidative Stress drug effects, Reactive Oxygen Species metabolism, Sirtuins antagonists & inhibitors, Breast Neoplasms drug therapy, Isocitrate Dehydrogenase genetics, Sirtuins genetics
Abstract

SIRT5 is a member of the sirtuin family of NAD + -dependent protein lysine deacylases implicated in a variety of physiological processes. SIRT5 removes negatively charged malonyl, succinyl, and glutaryl groups from lysine residues and thereby regulates multiple enzymes involved in cellular metabolism and other biological processes. SIRT5 is overexpressed in human breast cancers and other malignancies, but little is known about the therapeutic potential of SIRT5 inhibition for treating cancer. Here we report that genetic SIRT5 disruption in breast cancer cell lines and mouse models caused increased succinylation of IDH2 and other metabolic enzymes, increased oxidative stress, and impaired transformation and tumorigenesis. We, therefore, developed potent, selective, and cell-permeable small-molecule SIRT5 inhibitors. SIRT5 inhibition suppressed the transformed properties of cultured breast cancer cells and significantly reduced mammary tumor growth in vivo, in both genetically engineered and xenotransplant mouse models. Considering that Sirt5 knockout mice are generally normal, with only mild phenotypes observed, these data establish SIRT5 as a promising target for treating breast cancer. The new SIRT5 inhibitors provide useful probes for future investigations of SIRT5 and an avenue for targeting SIRT5 as a therapeutic strategy.

Published
2021
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41. Malunion of an In Utero Metacarpal Fracture in a Standardbred Mare Presenting for Dystocia.

Author

Lection J, Delvescovo B, Percival A, Wu T, Southard T, Diel de Amorim M, and Cheong SH

Subjects
Animals, Cesarean Section veterinary, Delivery, Obstetric veterinary, Female, Horses, Pregnancy, Dystocia etiology, Dystocia veterinary, Horse Diseases, Metacarpal Bones
Abstract

In utero fracture and malunion of long bones is a rare condition in horses. Most foals with in utero fractures are aborted, and the identification of a fetal in utero fracture in a mare with dystocia has not been reported. A 7-year-old multiparous Standardbred mare presented to a referral center for correction of dystocia. Assisted vaginal delivery and controlled vaginal delivery attempts were unsuccessful mainly because of contracted tendons impeding mutation. As the foal was alive, a cesarean section was elected. The foal was delivered but ultimately euthanized because of the congenital abnormalities. Computed tomography of the right forelimb of the foal along with gross examination and histologic evaluation of the right metacarpus revealed the malunion of a previous in utero fracture. While a few cases have been reported of in utero fracture, many of these were in abortuses and not in fetuses at term, making this case a new presentation and potential etiology for dystocia., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published
2021
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42. Equine Stereotaxtic Population Average Brain Atlas With Neuroanatomic Correlation.

Author

Johnson PJ, Janvier V, Luh WM, FitzMaurice M, Southard T, and Barry EF

Abstract

There is growing interest in the horse for behavioral, neuroanatomic and neuroscientific research due to its large and complex brain, cognitive abilities and long lifespan making it neurologically interesting and a potential large animal model for several neuropsychological diseases. Magnetic resonance imaging (MRI) is a powerful neuroscientific research tool that can be performed in vivo , with adapted equine facilities, or ex-vivo in the research setting. The brain atlas is a fundamental resource for neuroimaging research, and have been created for a multitude animal models, however, none currently exist for the equine brain. In this study, we document the creation of a high-resolution stereotaxic population average brain atlas of the equine. The atlas was generated from nine unfixed equine cadaver brains imaged within 4 h of euthanasia in a 3-tesla MRI. The atlas was generated using linear and non-linear registration methods and quality assessed using signal and contrast to noise calculations. Tissue segmentation maps (TSMs) for white matter (WM), gray matter (GM) and cerebrospinal fluid (CSF), were generated and manually segmented anatomic priors created for multiple subcortical brain structures. The resulting atlas was validated and correlated to gross anatomical specimens and is made freely available at as an online resource for researchers (https://doi.org/10.7298/cyrs-7b51.2). The mean volume metrics for the whole brain, GM and WM for the included subjects were documented and the effect of age and laterality assessed. Alterations in brain volume in relation to age were identified, though these variables were not found to be significantly correlated. All subjects had higher whole brain, GM and WM volumes on the right side, consistent with the well documented right forebrain dominance of horses. This atlas provides an important tool for automated processing in equine and translational neuroimaging research., (Copyright © 2019 Johnson, Janvier, Luh, FitzMaurice, Southard and Barry.)

Published
2019
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43. Littermate cats rescued from a shelter succumbed to acute, primary toxoplasmosis associated with TOXO DB genotype #4, generally circulating in wildlife.

Author

Crouch EEV, Mittel LD, Southard TL, Cerqueira-Cézar CK, Murata FHA, Kwok OCH, Su C, and Dubey JP

Subjects
Animals, Animals, Wild parasitology, Feces parasitology, Female, Litter Size, Liver parasitology, Lung parasitology, Male, Meat parasitology, Pregnancy, Raw Foods parasitology, Toxoplasmosis, Animal diagnosis, Cat Diseases parasitology, Cats parasitology, Genotype, Toxoplasma genetics, Toxoplasma pathogenicity, Toxoplasmosis, Animal mortality
Abstract

Cats are important in the epidemiology of Toxoplasma gondii infection because they are the only hosts that can excrete the environmentally resistant oocysts in the environment. Although exposure is common (approximately 30% of cats in the USA), clinical toxoplasmosis is relatively rare. Here, we report overwhelming disseminated toxoplasmosis in two litter mate 8-week-old kittens, thought to have acquired toxoplasmosis postnatally. Five domestic shorthair kittens, approximately 2-3 weeks of age, and the queen were found in upstate New York by a rescue group in spring of 2018. The kittens and queen were placed in a foster home for approximately 4-5 weeks and then transferred to a shelter. Two kittens died unexpectedly following a short illness. Postmortem examination of the two deceased kittens revealed overwhelming toxoplasmosis and the presence of entero-epithelial stages in small intestine, suggestive of recent ingestion of infected tissues. Antibodies to T. gondii were found in the deceased kittens and the queen but not in the three asymptomatic littermate kittens. No obvious cause of immunosuppression was demonstrated. Genetic typing of T. gondii from DNA extracted from liver and lungs of both kittens revealed Toxo DB #4 genotype, commonly found in wildlife. Owners and veterinarians should be aware of dangers of feeding raw meat to cats and contact with infected cat feces. Procedures to safely handle T. gondii infected feces in hospital setting are outlined., (Copyright © 2019. Published by Elsevier B.V.)

Published
2019
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44. Physical confinement induces malignant transformation in mammary epithelial cells.

Author

Lu YC, Chu T, Hall MS, Fu DJ, Shi Q, Chiu A, An D, Wang LH, Pardo Y, Southard T, Danko CG, Liphardt J, Nikitin AY, Wu M, Fischbach C, Coonrod S, and Ma M

Subjects
Acinar Cells pathology, Animals, Capsules, Carcinogenesis pathology, Extracellular Matrix metabolism, Female, Humans, Hydrogels chemistry, Insulin metabolism, Insulin-Like Growth Factor I metabolism, Mice, SCID, Sequence Analysis, RNA, Signal Transduction, Xenograft Model Antitumor Assays, Cell Transformation, Neoplastic pathology, Epithelial Cells pathology, Mammary Glands, Human pathology
Abstract

The physical microenvironment of tumor cells plays an important role in cancer initiation and progression. Here, we present evidence that confinement - a new physical parameter that is apart from matrix stiffness - can also induce malignant transformation in mammary epithelial cells. We discovered that MCF10A cells, a benign mammary cell line that forms growth-arrested polarized acini in Matrigel, transforms into cancer-like cells within the same Matrigel material following confinement in alginate shell hydrogel microcapsules. The confined cells exhibited a range of tumor-like behaviors, including uncontrolled cellular proliferation and invasion. Additionally, 4-6 weeks after transplantation into the mammary fad pads of immunocompromised mice, the confined cells formed large palpable masses that exhibited histological features similar to that of carcinomas. Taken together, our findings suggest that physical confinement represents a previously unrecognized mechanism for malignancy induction in mammary epithelial cells and also provide a new, microcapsule-based, high throughput model system for testing new breast cancer therapeutics., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published
2019
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45. Histological, electrophysiological and clinical effects of thermal radiofrequency therapy of the saphenous nerve and pulsed radiofrequency therapy of the sciatic nerve in dogs.

Author

Boesch JM, Campoy L, Southard T, Dewey C, Erb HN, Gleed RD, Martin-Flores M, Sakai DM, Sutton J, Williamson B, and Zatroch K

Subjects
Animals, Chronic Pain therapy, Dogs, Female, Osteoarthritis therapy, Pain Measurement veterinary, Sciatic Nerve anatomy & histology, Sciatic Nerve physiology, Single-Blind Method, Spinal Nerves anatomy & histology, Spinal Nerves physiology, Chronic Pain veterinary, Dog Diseases therapy, Osteoarthritis veterinary, Radiofrequency Therapy veterinary, Stifle innervation
Abstract

Objective: Thermal radiofrequency (TRF) of the saphenous nerve (a sensory nerve) combined with pulsed radiofrequency (PRF) of the sciatic nerve (a sensory and motor nerve) might relieve intractable stifle osteoarthritis (OA) pain in dogs. The objective was to determine if saphenous nerve TRF induces Wallerian degeneration and if sciatic nerve PRF induces degeneration or dysfunction., Study Design: Blinded, controlled, randomized, preclinical study., Animals: A group of six intact, female Beagle dogs aged 14-16 months., Methods: In each dog, one pelvic limb was assigned randomly to the control group and the other to the treatment group. Dogs were anesthetized and, using ultrasonography, radiofrequency electrodes were positioned adjacent to saphenous and sciatic nerves bilaterally; TRF and PRF were performed only in the treatment limb. Motor nerve conduction velocity (MNCV) was measured in both sciatic nerves 2 weeks later, and the dogs were euthanized. Hematoxylin and eosin-stained sections of saphenous and sciatic nerves were examined using light microscopy. Degeneration and inflammation were scored 0 (none) to 3 (severe). A one-tailed, paired Wilcoxon signed-rank test was used to test for differences in scores and MNCV between control and treatment nerves., Results: Degeneration and inflammation scores were higher in treatment saphenous nerves in 5/6 dogs [83%; 95% confidence interval (CI), 36%, 99%]; however, after Bonferroni correction only degeneration score was higher (p = 0.0313). Degeneration, inflammation or decreased MNCV were not observed in sciatic nerves (each outcome: 0/6 nerves, 0%; 95% CI, 0%, 48%). No dogs experienced postprocedural pain or neurological deficits., Conclusions and Clinical Relevance: The degeneration in TRF-treated saphenous nerves appears sufficient to impair transmission. Sciatic nerve PRF did not cause degeneration with attendant motor deficits, consistent with a proposed neuromodulatory mechanism. A clinical trial is needed to confirm the combined techniques produce analgesia without motor deficits in dogs with stifle OA., (Copyright © 2019 Association of Veterinary Anaesthetists and American College of Veterinary Anesthesia and Analgesia. Published by Elsevier Ltd. All rights reserved.)

Published
2019
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46. Salinomycin decreases feline sarcoma and carcinoma cell viability when combined with doxorubicin.

Author

Borlle L, Dergham A, Wund Z, Zumbo B, Southard T, and Hume KR

Subjects
Animals, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Carcinoma drug therapy, Cats, Cell Line, Tumor, Cell Survival drug effects, Doxorubicin toxicity, Drug Resistance, Neoplasm drug effects, Drug Synergism, In Vitro Techniques, Mice, Pyrans toxicity, Sarcoma drug therapy, Carcinoma veterinary, Doxorubicin pharmacology, Doxorubicin therapeutic use, Pyrans pharmacology, Pyrans therapeutic use, Sarcoma veterinary
Abstract

Background: Cancer is a significant health threat in cats. Chemoresistance is prevalent in solid tumors. The ionophore salinomycin has anti-cancer properties and may work synergistically with chemotherapeutics. The purpose of our study was to determine if salinomycin could decrease cancer cell viability when combined with doxorubicin in feline sarcoma and carcinoma cells., Results: We established two new feline injection-site sarcoma cell lines, B4 and C10, and confirmed their tumorigenic potential in athymic nude mice. B4 was more resistant to doxorubicin than C10. Dose-dependent effects were not observed until 92 μM in B4 cells (p = 0.0006) vs. 9.2 μM (p = 0.0004) in C10 cells. Dose-dependent effects of salinomycin were observed at 15 μM in B4 cells (p = 0.025) and at 10 μM in C10 cells (p = 0.020). Doxorubicin plus 5 μM salinomycin decreased viability of B4 cells compared to either agent alone, but only at supra-pharmacological doxorubicin concentrations. However, doxorubicin plus 5 μM salinomycin decreased viability of C10 cells compared to either agent alone at doxorubicin concentrations that can be achieved in vivo (1.84 and 4.6 μM, p < 0.004). In SCCF1 cells, dose-dependent effects of doxorubicin and salinomycin were observed at 9.2 (p = 0.036) and 2.5 (p = 0.0049) μM, respectively. When doxorubicin was combined with either 1, 2.5, or 5 μM of salinomycin in SCCF1 cells, dose-dependent effects of doxorubicin were observed at 9.2 (p = 0.0021), 4.6 (p = 0.0042), and 1.84 (p = 0.0021) μM, respectively. Combination index calculations for doxorubicin plus 2.5 and 5 μM salinomycin in SCCF1 cells were 0.4 and 0.6, respectively., Conclusions: We have developed two new feline sarcoma cell lines that can be used to study chemoresistance. We observed that salinomycin may potentiate (C10 cells) or work synergistically (SCCF1 cells) with doxorubicin in certain feline cancer cells. Further research is indicated to understand the mechanism of action of salinomycin in feline cancer cells as well as potential tolerability and toxicity in normal feline tissues.

Published
2019
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47. Biological indicators of chemoresistance: an ex vivo analysis of γH2AX and p53 expression in feline injection-site sarcomas.

Author

Bing Y, Wund Z, Abratte T, Borlle L, Kang S, Southard T, and Hume KR

Abstract

Background: The response of soft tissue sarcomas to cytotoxic chemotherapy is inconsistent. Biomarkers of chemoresistance or chemosensitivity are needed in order to identify appropriate patients for treatment. Given that many chemotherapeutics kill cells through direct DNA interactions, we hypothesized that upregulation of DNA damage response mechanisms would confer resistance to cytotoxic chemotherapy in sarcomas. To study this, we used spontaneously-occurring feline injection-site sarcomas (FISS)., Methods: γH2AX and p53 expression were determined in biopsy samples of FISS. γH2AX expression was determined via immunohistochemistry whereas p53 expression was determined via qRT-PCR. Cell lines derived from these sarcoma biopsies were then treated with carboplatin ( N  = 11) or doxorubicin ( N  = 5) and allowed to grow as colonies. Colony forming-ability of cells exposed to chemotherapy was compared to matched, untreated cells and expressed as percent survival relative to controls. ImageJ was used for quantification. A mixed model analysis was performed to determine if an association existed between relative survival of the treated cells and γH2AX or p53 expression in the original tumors. Cell lines were validated via vimentin expression or growth as subcutaneous sarcomas in nude mice., Results: An association was detected between γH2AX expression and relative survival in cells exposed to carboplatin ( P  = 0.0250). In the 11 FISS tumors evaluated, γH2AX expression ranged from 2.2 to 18.8% (mean, 13.3%). Cells from tumors with γH2AX expression higher than the sample population mean had fourfold greater relative survival after carboplatin exposure than cells from tumors with γH2AX expression less than the mean. There was no association between relative survival after carboplatin exposure and p53 expression ( P  = 0.1608), and there was no association between relative survival after doxorubicin exposure and either γH2AX ( P  = 0.6124) or p53 ( P  = 0.8645) expression. Four cell lines were validated via growth as sarcomas in nude mice. Vimentin expression was confirmed in the other 7 cell lines., Conclusions: γH2AX expression, but not wild type p53 , may potentially serve as a biomarker of resistance to platinum therapeutics in soft tissue sarcomas. To further investigate this finding, prospective, in vivo studies are indicated in animal models.

Published
2018
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48. Uterine carcinosarcoma (malignant mixed Müllerian tumor): case report in a goat and literature review.

Author

Cossic B, Hill JA, Cercone M, and Southard T

Subjects
Animals, Diagnosis, Differential, Female, Goat Diseases pathology, Goat Diseases surgery, Goats, Immunohistochemistry veterinary, Mixed Tumor, Mullerian diagnosis, Mixed Tumor, Mullerian pathology, Uterine Neoplasms diagnosis, Uterine Neoplasms pathology, Goat Diseases diagnosis, Mixed Tumor, Mullerian veterinary, Uterine Neoplasms veterinary
Abstract

Carcinosarcomas are biphasic malignant tumors composed of 2 distinct neoplastic cell populations, epithelial cells and mesenchymal cells. A 13-y-old, female, mixed-breed goat was presented with a 1-wk history of anuria and lethargy. Transabdominal ultrasonography showed an irregular and heterogeneous structure in the region of the bladder and uterus and changes in the echogenicity of both kidneys. Given the poor prognosis, euthanasia was elected. Autopsy revealed a large mass within the uterine cervix and confirmed the changes in the urinary tract. Histopathology and immunohistochemistry revealed a mixed, anti-cytokeratin AE1/AE3-positive epithelial, and vimentin-positive mesenchymal neoplasm consistent with a homologous carcinosarcoma, also called malignant mixed Müllerian tumor, with areas of double-labeling. We highlight the complexity of the diagnosis of uterine neoplasms in domestic animals and in goats in particular.

Published
2018
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49. Volumetric and linear measurements of lung tumor burden from non-gated micro-CT imaging correlate with histological analysis in a genetically engineered mouse model of non-small cell lung cancer.

Author

Gallastegui A, Cheung J, Southard T, and Hume KR

Subjects
Animals, Carcinoma, Non-Small-Cell Lung pathology, Female, Lung Neoplasms pathology, Male, Mice, Mice, Transgenic, Carcinoma, Non-Small-Cell Lung diagnostic imaging, Cone-Beam Computed Tomography, Lung Neoplasms diagnostic imaging, Tumor Burden
Abstract

In vivo micro-computed tomography (CT) imaging allows longitudinal studies of pulmonary neoplasms in genetically engineered mouse models. Respiratory gating increases the accuracy of lung tumor measurements but lengthens anesthesia time in animals that may be at increased risk for complications. We hypothesized that semiautomated, volumetric, and linear tumor measurements performed in micro-CT images from non-gated scans would have correlation with histological findings. Primary lung tumors were induced in eight FVB mice with two transgenes (FVB/N-Tg(tetO-Kras2)12Hev/J; FVB.Cg-Tg(Scgb1a1-rtTA)1Jaw/J). Non-gated micro-CT scans were performed and the lungs were subsequently harvested. In the acquired micro-CT scans, measurements of all identified tumors were determined using the following methods: semiautomated three-dimensional (3D) volume, ellipsoid volume, Response Evaluation Criteria in Solid Tumors (RECIST; sum of largest axial (i.e., transverse) diameter from five tumors), sum of largest axial diameters from all tumors (modified RECIST), and average axial diameter. For histological analysis, all five lung lobes were analyzed and the tumor area was summed from measurements made on five histological sections that were 300 µm apart from each other (covering a total depth of 1200 µm). All micro-CT measurement methods had very strong correlation with histological tumor burden (Pearson's correlation coefficient, 0.87 ( p = 0.0053) -0.98 ( p < 0.0001)). The only methods found to have different correlations were the semiautomated 3D method and the RECIST method (Williams' test for dependent overlapping correlations, p = 0.013). Our results suggest quantification of lung tumor burden from non-gated micro-CT imaging will reflect histological differences between mice and can therefore be used for between-group comparisons or when concerns about systemic health of research animals may limit lengthy anesthetic procedures.

Published
2018
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50. Childhood body mass index is associated with early dental development and eruption in a longitudinal sample from the Iowa Facial Growth Study.

Author

Nicholas CL, Kadavy K, Holton NE, Marshall T, Richter A, and Southard T

Subjects
Adolescent, Age Factors, Child, Child, Preschool, Female, Humans, Iowa, Longitudinal Studies, Male, Body Mass Index, Pediatric Obesity physiopathology, Tooth growth & development, Tooth Eruption physiology
Abstract

Introduction: Children with high body mass index (BMI) values have been demonstrated to have precocious dental development. Research has largely focused on cross-sectional data sets, leaving an incomplete understanding of the longitudinal relationship between BMI and dental maturation., Methods: We used a pure longitudinal growth series to examine the relationship between dental development and childhood BMI. Periapical radiographs from 77 children from the Iowa Growth Study were used to estimate dental development for those with high BMI values., Results: We confirmed prior studies in finding that children with higher BMI values were more likely to have advanced dental development for their ages (P <0.001). BMI at age 4 years was predictive for the timing of dental development at age 12 (P = 0.052). The precocity of the rate of dental development accelerated across growth. Overall dental development scores also correlated with the age of dental eruption for the mandibular canines and first premolars (P <0.001)., Conclusions: High BMI values at young ages predict advanced dental development at later times, suggesting a long-term effect of BMI on dental maturation and implying the need for earlier orthodontic interventions in obese children. These results corroborate those of previous studies, building further evidence that relatively early dental eruption is another consequence of childhood obesity., (Copyright © 2018 American Association of Orthodontists. Published by Elsevier Inc. All rights reserved.)

Published
2018
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