Kevin V. Tram scite author profile

Some antiepileptic drugs have been shown to be clinically effective in the treatment of neuropathic pain. This study determined whether the new antiepileptic drug tiagabine, a GABA uptake inhibitor, is efficacious in mice in a broad range of nociceptive tests (hot-plate, formalin, and dynorphin-induced chronic allodynia) and compared tiagabine's potency with two other antiepileptic drugs, gabapentin and lamotrigine. Intraperitoneally administered tiagabine, but not lamotrigine, gabapentin, or i.t. tiagabine, produced dose-dependent antinoception in the hot-plate test. A 5-min pretreatment with tiagabine (2-29 nmol i.t.) dose-dependently inhibited both the acute and late phase formalin behaviors; pretreatment with lamotrigine (4 -265 nmol i.t.) inhibited only the late phase. In the formalin assay the GABA A antagonist bicuculline reversed the acute phase antinociception, whereas the GABA B antagonist saclofen reversed both the acute and late phase tiagabine-induced antinociception. Tiagabine administered i.p. but not i.t. dose-dependently reduced dynorphin-induced chronic allodynia for 120 min. Gabapentin and lamotrigine produced antinociception administered either i.t. or i.p. in a dose-dependent manner. Thus, we have shown that gabapentin and lamotrigine produced antinociception in two mouse models of pain, whereas tiagabine produced antinociception in all three mouse models of pain.

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A New Murine Model for Bronchiolitis Obliterans Post–Bone Marrow Transplant

Panoskaltsis‐Mortari¹,

Tram²,

Price³

et al. 2007

Am J Respir Crit Care Med

105

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Rationale: Bronchiolitis obliterans (BO) is a major problem in lung transplantation and is also part of the spectrum of late-onset pulmonary complications that can occur after hematopoietic stem cell transplant. Better mouse models are needed to study the onset of this disease so that therapeutic interventions can be developed. Objectives: Our goal was to develop a BO mouse model. Methods: Recipients were lethally conditioned and given a rescue dose of T-cell-depleted, allogeneic bone marrow (BM) supplemented with a sublethal dose of allogeneic T cells. Measurements and Main Results: At 2 months post-BM transplant, the lungs had extensive perivascular and peribronchiolar inflammation consisting of CD4 1 T cells, CD8 1 T cells, B cells, macrophages, neutrophils, and fibroblasts. In contrast to the acute model, histology showed airway obstruction consistent with BO. Epithelial cells of airways in the early stages of occlusion exhibited changes in expression of cytokeratins. Although the lung had severe allogeneic BM transplant-mediated disease, there was only mild to moderate graft-versus-host disease in liver, colon, skin, and spleen. High wet/ dry weight ratios and elevated hydroxyproline were seen, consistent with pulmonary edema and fibrosis. Mice with BO exhibited high airway resistance and low compliance. Increases in many inflammatory mediators in the lungs of mice that develop BO were seen early post-transplant and not later at the time of BO. Conclusions: This new mouse model will be useful for the study of BO associated with late post-hematopoietic stem cell transplant onset and chronic graft-versus-host disease, which also leads to poor outcome in the lung transplant setting.Keywords: bronchiolitis obliterans; mouse models; transplantation Bronchiolitis obliterans (BO) is a major obstacle that has limited the success of lung transplantation (1, 2). It is also part of the spectrum of late-onset pulmonary complications that can occur after hematopoietic stem cell transplant (HSCT) (3). The signature histopathologic finding in BO is the obliteration of the airway and airway epithelium by a fibroproliferative response (4-7). The formation of this lesion is generally believed to have two major components: airway epithelial injury, due to a directed alloimmune response, followed by fibroproliferation. This results in irreversible structural changes and impaired lung function. An increase in both CD8-and CD4-positive cells in BO lesions supports that this injury is immunologically mediated (8). The upregulation of major histocompatibility complex (MHC) class II antigens in lesions together with bronchoalveolar lavage lymphocytes demonstrating reactivity to donor-specific class I HLA antigens suggest that alloreactivity directed against the epithelial MHC antigens may be the inciting event (8). Within an affected lung, normal, inflamed, and fibrosed airways are histologically evident. This suggests a temporal and spatial continuum between injury and the fibroproliferative response.We previously established a mo...

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Identification of DPB1 Permissive Unrelated Donors Is Highly Likely

Tram

Stritesky

Wadsworth

et al. 2017

Biology of Blood and Marrow Transplantation

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HLA-DPB1 permissive matching based on T cell epitope (TCE) groups should be considered when selecting among equally matched HLA-A, -B, -C, -DRB1 unrelated hematopoietic stem cell donors to improve patient survival. Previous studies have defined 3 TCE groups based on functional assays of alloreactivity. Combinations of donor and recipient DPB1 alleles with low immunogenic potential identify permissive donors, who provide no increased risk of mortality compared with DPB1-matched donors. To determine the likelihood of identifying a DPB1 permissive-matched (includes both allele-matched and DPB1-permissive mismatched) unrelated donor for patients with high-resolution matches at 10/10 HLA-A, -B,- C, -DRB1, and -DQB1 in the Be The Match Registry, preliminary search requests from United States' transplant centers for 595 DPB1-typed patients were evaluated for existence of a DPB1 permissive-matched donor, identified either among already typed donors or by prospective DPB1 typing. The baseline DPB1 permissive match rate was 69% and improved to 80% after additional donor DPB1 typing (median, 4 donors per patient). When seeking a 10/10-matched, young (18- to 32-year-old) donor in the registry, the probability of finding a DPB1 permissive-matched donor started lower at 59% and improved to 70% after additional DPB1 testing. Our results show that most patients with a 10/10 match can find a DPB1 permissive-matched donor.

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Evidence for early fibrosis and increased airway resistance in bone marrow transplant recipient mice deficient in MMP12

England

Price

Tram

et al. 2011

American Journal of Physiology-Lung Cellular and Molecular Phys

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Idiopathic pneumonia syndrome (IPS) is a significant cause of morbidity and mortality post-bone marrow transplantation (BMT) in humans. In our established murine IPS model in which lethally conditioned recipients are given allogeneic bone marrow and splenocytes, recruitment of host monocytes occurs early post-BMT, followed by donor T cells concomitant with development of severe lung dysfunction. Because matrix metalloproteinase 12 (MMP12) is important for macrophage infiltration and injury in other mouse models of lung disease such as emphysema, lethally conditioned MMP12(-/-) mice were used as allogeneic recipients to determine whether MMP12 plays a similar role in potentiating lung injury in IPS. Surprisingly, MMP12(-/-) mice developed IPS and exhibited an accelerated allogeneic T cell-dependent decrease in compliance compared with wild-type (WT) recipients. MMP12(-/-), but not WT, mice also had allogeneic T cell-dependent elevated lung resistance post-BMT. Recruitment of monocytes and T cells into the lungs was not altered on day 7 post-BMT, but the lungs of MMP12(-/-) recipients had increased collagen deposition, a feature normally not seen in our IPS model. MMP12(-/-) mice had a compensatory increase in MMP2 in the lungs post-BMT, as well as increased β6-integrin compared with WT recipients, and only in the presence of allogeneic T cells. Levels of total transforming growth factor (TGF)-β1 protein in the lungs were elevated compared with WT recipients, consistent with the profibrotic function of β6-integrin as an activator of TGF-β. These data indicate that host-derived MMP12 may be important in limiting development of IPS by allowing proper remodeling of extracellular matrix and effective repair of BMT-related injury.

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Identification of a 10/10 matched donor for patients with an uncommon haplotype is unlikely

Olson

Gibbens

Tram

et al. 2017

HLA

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Kevin V. Tram

Comparison of Antiepileptic Drugs Tiagabine, Lamotrigine, and Gabapentin in Mouse Models of Acute, Prolonged, and Chronic Nociception

A New Murine Model for Bronchiolitis Obliterans Post–Bone Marrow Transplant

Identification of DPB1 Permissive Unrelated Donors Is Highly Likely

Evidence for early fibrosis and increased airway resistance in bone marrow transplant recipient mice deficient in MMP12

Identification of a 10/10 matched donor for patients with an uncommon haplotype is unlikely

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