Your search keyword '"ganciclovir"' showing total 82 results

1. Evaluating a Targeted Cancer Therapy Approach Mediated by RNA

Author

Woess, Katharina, Sun, Yuchen, Morio, Hanae, Stierschneider, Anna, Kaufmann, Anna, Hainzl, Stefan, Trattner, Lisa, Kocher, Thomas, Tockner, Birgit, Leb-Reichl, Victoria, Steiner, Markus, Brachtl, Gabriele, South, Andrew P., Bauer, Johann W, Reichelt, Julia, Furihata, Tomomi, Wally, Verena, Koller, Ulrich, Piñón Hofbauer, Josefina, Guttmann-Gruber, Christina, Woess, Katharina, Sun, Yuchen, Morio, Hanae, Stierschneider, Anna, Kaufmann, Anna, Hainzl, Stefan, Trattner, Lisa, Kocher, Thomas, Tockner, Birgit, Leb-Reichl, Victoria, Steiner, Markus, Brachtl, Gabriele, South, Andrew P., Bauer, Johann W, Reichelt, Julia, Furihata, Tomomi, Wally, Verena, Koller, Ulrich, Piñón Hofbauer, Josefina, and Guttmann-Gruber, Christina

Abstract

Conventional anti-cancer therapies based on chemo- and/or radiotherapy represent highly effective means to kill cancer cells but lack tumor specificity and, therefore, result in a wide range of iatrogenic effects. A promising approach to overcome this obstacle is spliceosome-mediated RNA trans-splicing (SMaRT), which can be leveraged to target tumor cells while leaving normal cells unharmed. Notably, a previously established RNA trans-splicing molecule (RTM44) showed efficacy and specificity in exchanging the coding sequence of a cancer target gene (Ct-SLCO1B3) with the suicide gene HSV1-thymidine kinase in a colorectal cancer model, thereby rendering tumor cells sensitive to the prodrug ganciclovir (GCV). In the present work, we expand the application of this approach, using the same RTM44 in aggressive skin cancer arising in the rare genetic skin disease recessive dystrophic epidermolysis bullosa (RDEB). Stable expression of RTM44, but not a splicing-deficient control (NC), in RDEB-SCC cells resulted in expression of the expected fusion product at the mRNA and protein level. Importantly, systemic GCV treatment of mice bearing RTM44-expressing cancer cells resulted in a significant reduction in tumor volume and weight compared with controls. Thus, our results demonstrate the applicability of RTM44-mediated targeting of the cancer gene Ct-SLCO1B3 in a different malignancy.

Published

2022

2. Valganciclovir—Ganciclovir Use and Systematic Therapeutic Drug Monitoring. An Invitation to Antiviral Stewardship

Author

Galar, Alicia, Valerio, Maricela, Catalán, Pilar, García-González, Xandra, Burillo, Almudena, Fernández-Cruz, Ana, Zataráin, Eduardo, Sousa-Casasnovas, Iago, Anaya, Fernando, Rodríguez-Ferrero, María, Muñoz García, Patricia, Bouza, Emilio, Galar, Alicia, Valerio, Maricela, Catalán, Pilar, García-González, Xandra, Burillo, Almudena, Fernández-Cruz, Ana, Zataráin, Eduardo, Sousa-Casasnovas, Iago, Anaya, Fernando, Rodríguez-Ferrero, María, Muñoz García, Patricia, and Bouza, Emilio

Abstract

Valganciclovir (VGCV) and ganciclovir (GCV) doses must be adjusted according to indication, renal function and weight. No specific therapeutic exposure values have been established. We aimed to evaluate the adequacy of VGCV/GCV doses, to assess the interpatient variability in GCV serum levels, to identify predictive factors for this variability and to assess the clinical impact. This is a prospective study at a tertiary institution including hospitalized patients receiving VGCV/GCV prophylaxis or treatment. Adequacy of the antiviral dose was defined according to cytomegalovirus guidelines. Serum levels were determined using High-Performance Liquid Chromatography. Blood samples were drawn at least 3 days after antiviral initiation. Outcome was considered favorable if there was no evidence of cytomegalovirus infection during prophylaxis or when a clinical and microbiological resolution was attained within 21 days of treatment and no need for drug discontinuation due to toxicity. Seventy consecutive patients [74.3% male/median age: 59.2 years] were included. VGCV was used in 25 patients (35.7%) and GCV in 45 (64.3%). VGCV/GCV initial dosage was deemed adequate in 47/70 cases (67.1%), lower than recommended in 7/70 (10%) and higher in 16/70 (22.9%). Large inter-individual variability of serum levels was observed, with median trough levels of 2.3 mg/L and median peak levels of 7.8 mg/L. Inadequate dosing of VGCV/GCV and peak levels lower than 8.37 or greater than 11.86 mg/L were related to poor outcome. Further studies must be performed to confirm these results and to conclusively establish if VGCV/GCV therapeutic drug monitoring could be useful to improve outcomes in specific clinical situations., Instituto de Salud Carlos III (ISCIII)/FEDER, Depto. de Medicina, Fac. de Medicina, TRUE, pub

Published

2021

3. Gap junctions in human glioblastomas: implications for suicide gene therapy.

Author

Carrondo Cottin, Sylvine, Gould, Peter Vincent, Cantin, Léo, Caruso, Manuel, Carrondo Cottin, Sylvine, Gould, Peter Vincent, Cantin, Léo, and Caruso, Manuel

Abstract

Glioblastoma is a very aggressive astrocytic tumor and most patients have 1-year survival time after diagnosis. A promising therapeutic strategy is the local delivery of the herpes simplex virus thymidine kinase gene in the tumor bed followed by ganciclovir treatment. The presence of functional gap junctions is highly relevant for the success of suicide gene therapy. Connexins are expressed in practically all tissues and form gap junctions that allow intercellular communication. Connexin 43 (Cx43) is the major connexin member being expressed in astrocytes but its status in glioblastoma is not well defined. We have investigated by immunofluorescence the presence of Cx43 in 74 human glioblastoma samples; its expression was detected in 77% of the samples analyzed. We report here that glioblastoma is a heterogenous disease as regards Cx43 expression with presentations, in which Cx43 expression is unaltered, reduced or totally lost. A predominant Cx43 cytoplasmic localization was observed in four out of eight primary glioblastoma cultures that we have established. This aberrant localization reduced gap junctionnal intercellular communication by 50 to 75% as compared with primary cell cultures displaying gap junctional plaques. However, the bystander effect evaluated after lentiviral delivery of the herpes simplex virus thymidine kinase gene and ganciclovir treatment was detected in all Cx43-positive primary cell cultures, and it was independant of the Cx43 localization. These findings may have important clinical implications for the design of anticancer cytotoxic therapies that rely on the gap junction-mediated bystander effect for their success

Published

2021

4. Bystander effect in glioblastoma cells with a predominant cytoplasmic localization of connexin 43

Author

Carrondo Cottin, Sylvine, Ghani, Karim., Caruso, Manuel, Carrondo Cottin, Sylvine, Ghani, Karim., and Caruso, Manuel

Abstract

Herpes simplex virus thymidine kinase (TK) gene transfer followed by ganciclovir (GCV) administration is an approach investigated for glioblastoma treatment. The bystander effect (BE) enhances the cytotoxic effect of this strategy by allowing the diffusion of phosphorylated GCV from TK-expressing cells toward neighboring TK negative cells. This transfer of toxic metabolites is mainly mediated via gap junctions that are composed of connexins. Downregulation and/or cytoplasmic localization of connexins are common in tumors, and should be detrimental to the success of the TK/GCV strategy. In this study, we investigated the level of expression, the localization and the functionality of connexin43 (Cx43) in three glioblastoma cell lines. We showed that Cx43 was predominantly located in lysosomes and late endosomes, with only few gap junctions present at the cell surface. Surprisingly, the gap-junctional intercellular communication (GJIC) and the BE capacity were preserved, and in two of the cell lines analyzed, it was at least twice as high as compared to a control HeLa transfectant that expresses high levels of Cx43 at the cell membrane. Experiments performed in the presence of a-glycyrrhetinic acid or small interfering RNA confirmed that Cx43 was responsible for the GJIC and the BE. Our results indicate for the first time that the very limited numbers of gap junctions present in glioblastoma cells are highly functional. We thus conclude that the TK/GCV strategy is still a valuable therapeutic option to be developed for the treatment of glioblastoma patients.

Published

2021

5. NUDT15 polymorphism influences the metabolism and therapeutic effects of acyclovir and ganciclovir

Author

Nishii, Rina, Mizuno, Takanori, Rehling, Daniel, Smith, Colton, Clark, Brandi L., Zhao, Xujie, Brown, Scott A., Smart, Brandon, Moriyama, Takaya, Yamada, Yuji, Ichinohe, Tatsuo, Onizuka, Makoto, Atsuta, Yoshiko, Yang, Lei, Yang, Wenjian, Thomas, Paul G., Stenmark, Pål, Kato, Motohiro, Yang, Jun J., Nishii, Rina, Mizuno, Takanori, Rehling, Daniel, Smith, Colton, Clark, Brandi L., Zhao, Xujie, Brown, Scott A., Smart, Brandon, Moriyama, Takaya, Yamada, Yuji, Ichinohe, Tatsuo, Onizuka, Makoto, Atsuta, Yoshiko, Yang, Lei, Yang, Wenjian, Thomas, Paul G., Stenmark, Pål, Kato, Motohiro, and Yang, Jun J.

Abstract

Nucleobase and nucleoside analogs (NNA) are widely used as anti-viral and anti-cancer agents, and NNA phosphorylation is essential for the activity of this class of drugs. Recently, diphosphatase NUDT15 was linked to thiopurine metabolism with NUDT15 polymorphism associated with drug toxicity in patients. Profiling NNA drugs, we identify acyclovir (ACV) and ganciclovir (GCV) as two new NNAs metabolized by NUDT15. NUDT15 hydrolyzes ACV and GCV triphosphate metabolites, reducing their effects against cytomegalovirus (CMV) in vitro. Loss of NUDT15 potentiates cytotoxicity of ACV and GCV in host cells. In hematopoietic stem cell transplant patients, the risk of CMV viremia following ACV prophylaxis is associated with NUDT15 genotype (P = 0.015). Donor NUDT15 deficiency is linked to graft failure in patients receiving CMV-seropositive stem cells (P = 0.047). In conclusion, NUDT15 is an important metabolizing enzyme for ACV and GCV, and NUDT15 variation contributes to inter-patient variability in their therapeutic effects.

Published

2021

6. NUDT15-mediated hydrolysis limits the efficacy of anti-HCMV drug ganciclovir

Author

Zhang, Si Min, Rehling, Daniel, Jemth, Ann-Sofie, Throup, Adam, Landázuri, Natalia, Almlöf, Ingrid, Göttmann, Mona, Valerie, Nicholas C. K., Borhade, Sanjay R., Wakchaure, Prasad, Page, Brent D. G., Desroses, Matthieu, Homan, Evert J., Scobie, Martin, Rudd, Sean G., Warpman Berglund, Ulrika, Söderberg-Nauclér, Cecilia, Stenmark, Pål, Helleday, Thomas, Zhang, Si Min, Rehling, Daniel, Jemth, Ann-Sofie, Throup, Adam, Landázuri, Natalia, Almlöf, Ingrid, Göttmann, Mona, Valerie, Nicholas C. K., Borhade, Sanjay R., Wakchaure, Prasad, Page, Brent D. G., Desroses, Matthieu, Homan, Evert J., Scobie, Martin, Rudd, Sean G., Warpman Berglund, Ulrika, Söderberg-Nauclér, Cecilia, Stenmark, Pål, and Helleday, Thomas

Abstract

Ganciclovir (GCV) is the first-line therapy against human cytomegalovirus (HCMV), a widespread infection that is particularly dangerous for immunodeficient individuals. Closely resembling deoxyguanosine triphosphate, the tri-phosphorylated metabolite of GCV (GCV-TP) is preferentially incorporated by the viral DNA polymerase, thereby terminating chain extension and, eventually, viral replication. However, the treatment outcome of GCV varies greatly among individuals, therefore warranting better understanding of its metabolism. Here we show that NUDT15, a Nudix hydrolase known to metabolize thiopurine triphosphates, can similarly hydrolyze GCV-TP through biochemical studies and co-crystallization of the NUDT15/GCV-TP complex. More critically, GCV efficacy was potentiated in HCMV-infected cells following NUDT15 depletion by RNAi or inhibition by an in-house-developed, nanomolar NUDT15 inhibitor, TH8321, suggesting that pharmacological targeting of NUDT15 is a possible avenue to improve existing anti-HCMV regimens. Collectively, the data further implicate NUDT15 as a broad-spectrum metabolic regulator of nucleoside analog therapeutics, such as thiopurines and GCV.

Published

2021

7. Bystander effect in glioblastoma cells with a predominant cytoplasmic localization of connexin 43

Author

Carrondo Cottin, Sylvine, Ghani, Karim, Caruso, Manuel, Carrondo Cottin, Sylvine, Ghani, Karim, and Caruso, Manuel

Abstract

Herpes simplex virus thymidine kinase (TK) gene transfer followed by ganciclovir (GCV) administration is an approach investigated for glioblastoma treatment. The bystander effect (BE) enhances the cytotoxic effect of this strategy by allowing the diffusion of phosphorylated GCV from TK-expressing cells toward neighboring TK negative cells. This transfer of toxic metabolites is mainly mediated via gap junctions that are composed of connexins. Downregulation and/or cytoplasmic localization of connexins are common in tumors, and should be detrimental to the success of the TK/GCV strategy. In this study, we investigated the level of expression, the localization and the functionality of connexin43 (Cx43) in three glioblastoma cell lines. We showed that Cx43 was predominantly located in lysosomes and late endosomes, with only few gap junctions present at the cell surface. Surprisingly, the gap-junctional intercellular communication (GJIC) and the BE capacity were preserved, and in two of the cell lines analyzed, it was at least twice as high as compared to a control HeLa transfectant that expresses high levels of Cx43 at the cell membrane. Experiments performed in the presence of a-glycyrrhetinic acid or small interfering RNA confirmed that Cx43 was responsible for the GJIC and the BE. Our results indicate for the first time that the very limited numbers of gap junctions present in glioblastoma cells are highly functional. We thus conclude that the TK/GCV strategy is still a valuable therapeutic option to be developed for the treatment of glioblastoma patients.

Published

2021

8. Gap junctions in human glioblastomas: implications for suicide gene therapy.

Author

Carrondo Cottin, Sylvine, Gould, Peter Vincent, Cantin, Léo, Caruso, Manuel, Carrondo Cottin, Sylvine, Gould, Peter Vincent, Cantin, Léo, and Caruso, Manuel

Abstract

Glioblastoma is a very aggressive astrocytic tumor and most patients have 1-year survival time after diagnosis. A promising therapeutic strategy is the local delivery of the herpes simplex virus thymidine kinase gene in the tumor bed followed by ganciclovir treatment. The presence of functional gap junctions is highly relevant for the success of suicide gene therapy. Connexins are expressed in practically all tissues and form gap junctions that allow intercellular communication. Connexin 43 (Cx43) is the major connexin member being expressed in astrocytes but its status in glioblastoma is not well defined. We have investigated by immunofluorescence the presence of Cx43 in 74 human glioblastoma samples; its expression was detected in 77% of the samples analyzed. We report here that glioblastoma is a heterogenous disease as regards Cx43 expression with presentations, in which Cx43 expression is unaltered, reduced or totally lost. A predominant Cx43 cytoplasmic localization was observed in four out of eight primary glioblastoma cultures that we have established. This aberrant localization reduced gap junctionnal intercellular communication by 50 to 75% as compared with primary cell cultures displaying gap junctional plaques. However, the bystander effect evaluated after lentiviral delivery of the herpes simplex virus thymidine kinase gene and ganciclovir treatment was detected in all Cx43-positive primary cell cultures, and it was independant of the Cx43 localization. These findings may have important clinical implications for the design of anticancer cytotoxic therapies that rely on the gap junction-mediated bystander effect for their success

Published

2021

9. Early cytomegalovirus DNAemia and antiviral dose adjustment in high vs intermediate risk kidney transplant recipients.

Author

Schaenman, Joanna, Schaenman, Joanna, Phonphok, Korntip, Spanuchart, Ittikorn, Duong, Tin, Sievers, Theodore M, Lum, Erik, Reed, Elaine F, Bunnapradist, Suphamai, Schaenman, Joanna, Schaenman, Joanna, Phonphok, Korntip, Spanuchart, Ittikorn, Duong, Tin, Sievers, Theodore M, Lum, Erik, Reed, Elaine F, and Bunnapradist, Suphamai

Abstract

BackgroundCytomegalovirus (CMV) infection continues to negatively affect outcomes for solid organ transplant recipients, despite the advent of strategies for preemptive surveillance and prophylaxis. The impact is especially great for CMV seronegative recipients of donor seropositive organs, who typically lack the ability to control CMV infection at the time of transplantation.MethodsWe reviewed episodes of CMV DNAemia in a modern cohort of kidney transplant recipients over a 3-year period at a high-volume transplant center to investigate the frequency of DNAemia during antiviral prophylaxis.ResultsDespite receipt of antiviral prophylaxis per current guidelines, 75 cases of CMV DNAemia were observed in the first 100 days after transplantation. For high risk patients, median time to DNAemia was 75 days after transplantation, and the majority of patients had experienced dose-reduction of valganciclovir due to renal insufficiency. Review of CMV seropositive intermediate risk patients demonstrated DNAemia occurring earlier after transplantation compared with high risk patients with a median time of 64 days (P = .029). The impact of valganciclovir dose adjustment was less notable in the intermediate risk group.ConclusionsGuidelines recommend beginning routine surveillance for CMV after the completion of antiviral prophylaxis. Our findings suggest that closer monitoring may be beneficial, especially for high risk patients at risk for DNAemia. Patients requiring dose adjustment of valganciclovir due to renal insufficiency may be at increased risk for CMV DNAemia. Improved methods for CMV prophylaxis and evaluation of immunologic risk for CMV DNAemia and disease are needed to improve patient outcomes after kidney transplantation.

Published

2021

10. Early removal of senescent cells protects retinal ganglion cells loss in experimental ocular hypertension.

Author

Rocha, Lorena Raquel, Rocha, Lorena Raquel, Nguyen Huu, Viet Anh, Palomino La Torre, Claudia, Xu, Qianlan, Jabari, Mary, Krawczyk, Michal, Weinreb, Robert N, Skowronska-Krawczyk, Dorota, Rocha, Lorena Raquel, Rocha, Lorena Raquel, Nguyen Huu, Viet Anh, Palomino La Torre, Claudia, Xu, Qianlan, Jabari, Mary, Krawczyk, Michal, Weinreb, Robert N, and Skowronska-Krawczyk, Dorota

Abstract

Experimental ocular hypertension induces senescence of retinal ganglion cells (RGCs) that mimics events occurring in human glaucoma. Senescence-related chromatin remodeling leads to profound transcriptional changes including the upregulation of a subset of genes that encode multiple proteins collectively referred to as the senescence-associated secretory phenotype (SASP). Emerging evidence suggests that the presence of these proinflammatory and matrix-degrading molecules has deleterious effects in a variety of tissues. In the current study, we demonstrated in a transgenic mouse model that early removal of senescent cells induced upon elevated intraocular pressure (IOP) protects unaffected RGCs from senescence and apoptosis. Visual evoked potential (VEP) analysis demonstrated that remaining RGCs are functional and that the treatment protected visual functions. Finally, removal of endogenous senescent retinal cells after IOP elevation by a treatment with senolytic drug dasatinib prevented loss of retinal functions and cellular structure. Senolytic drugs may have the potential to mitigate the deleterious impact of elevated IOP on RGC survival in glaucoma and other optic neuropathies.

Published

2020

11. Detection of lentiviral suicide gene therapy in C6 rat glioma using hyperpolarised [1-13C]pyruvate

Author

Nivajärvi, Riikka, Olsson, Venla, Hyppönen, Viivi, Bowen, Sean, Leinonen, Hanna M., Lesch, Hanna P., Ardenkjær-Larsen, Jan Henrik, Gröhn, Olli H.J., Ylä-Herttuala, Seppo, Kettunen, Mikko I., Nivajärvi, Riikka, Olsson, Venla, Hyppönen, Viivi, Bowen, Sean, Leinonen, Hanna M., Lesch, Hanna P., Ardenkjær-Larsen, Jan Henrik, Gröhn, Olli H.J., Ylä-Herttuala, Seppo, and Kettunen, Mikko I.

Abstract

Hyperpolarised [1-13C]pyruvate MRI has shown promise in monitoring therapeutic efficacy in a number of cancers including glioma. In this study, we assessed the pyruvate response to the lentiviral suicide gene therapy of herpes simplex virus-1 thymidine kinase with the prodrug ganciclovir (HSV-TK/GCV) in C6 rat glioma and compared it with traditional MR therapy markers. Female Wistar rats were inoculated with 106 C6 glioma cells. Treated animals received intratumoural lentiviral HSV-TK gene transfers on days 7 and 8 followed by 2-week GCV therapy starting on day 10. Animals were repeatedly imaged during therapy using volumetric MRI, diffusion and relaxation mapping, as well as metabolic [1-13C]pyruvate MRS imaging. Survival (measured as time before animals reached a humane endpoint and were euthanised) was assessed up to day 30 posttherapy. HSV-TK/GCV gene therapy lengthened the median survival time from 12 to 25 days. This was accompanied by an apparent tumour growth arrest, but no changes in diffusion or relaxation parameters in treated animals. The metabolic response was more evident in the case-by-case analysis than in the group-level analysis. Treated animals also showed a 37 ± 15% decrease (P < 0.05, n = 5) in lactate-to-pyruvate ratio between therapy weeks, whereas a 44 ± 18% increase (P < 0.05, n = 6) was observed in control animals. Hyperpolarised [1-13C]pyruvate MRI can offer complementary metabolic information to traditional MR methods to give a more comprehensive picture of the slowly developing gene therapy response. This may benefit the detection of the successful therapy response in patients.

Published

2020

12. In vitro co-infection by cytomegalovirus improves the antiviral activity of ganciclovir against human adenovirus

Author

Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Red Española de Investigación en Patología Infecciosa, European Commission, Spanish Adenovirus Network, Aguilar Guisado, Manuela, Marrugal-Lorenzo, José Antonio, Berastegui-Cabrera, Judith, Merino Díaz, Laura, Pachón, Jerónimo, Sánchez-Céspedes, Javier, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Red Española de Investigación en Patología Infecciosa, European Commission, Spanish Adenovirus Network, Aguilar Guisado, Manuela, Marrugal-Lorenzo, José Antonio, Berastegui-Cabrera, Judith, Merino Díaz, Laura, Pachón, Jerónimo, and Sánchez-Céspedes, Javier

Abstract

Human adenovirus (HAdV) infection has an important clinical impact in the immunosuppressed population and is associated with high morbidity and mortality rates. The lack of a specific, safe and effective antiviral treatment against HAdV makes necessary the search for new therapeutic options. The aim of this study was to evaluate the in vitro activity of ganciclovir (GCV) against HAdV in co-infection by human cytomegalovirus (HCMV) and HAdV in cellular cultures. Quantitative real-time polymerase chain reaction (qPCR) was used to measure HAdV and HCMV DNA replication efficiency in monocultures and in co-infection situations in the presence of both cidofovir (CDV) and GCV. The effects of GCV and CDV were also evaluated in a burst assay (used to measure the production of virus particles) for both viruses, alone and in combination. GCV decreased by 1-log the HAdV DNA replication efficiency in co-infection with HCMV compared with its activity in HAdV monoculture. The burst assay showed that the reductions in virus yield in the presence of GCV were higher for HCMV and co-infection than for HAdV in monoculture (145.2±35.5- vs. 116.4±27.3- vs. 23.0±10.0-fold, respectively, P<0.05). The improved anti-HAdV activity of GCV during co-infection may be because of the more efficient phosphorylation of GCV by the HCMV protein kinase, UL97. Patients treated with GCV as pre-emptive therapy for HCMV infection may be considered as low-risk for developing HAdV infections; however, further evaluations are required to confirm these results.

Published

2020

13. A double masked randomised 4-week, placebo-controlled study in the USA, Thailand and Taiwan to compare the efficacy of oral valganciclovir and topical 2% ganciclovir in the treatment of cytomegalovirus anterior uveitis: study protocol.

Author

Takhar, Jaskirat S, Takhar, Jaskirat S, Joye, Ashlin S, Somkijrungroj, Thanapong, Laovirojjanakul, Wipada, Lin, Chang-Ping, Lietman, Thomas M, Porco, Travis C, Keenan, Jeremy D, Gebreegziabher, Elisabeth A, Seitzman, Gerami D, Rose-Nussbaumer, Jennifer, Doan, Thuy A, Acharya, Nisha R, Gonzales, John A, Takhar, Jaskirat S, Takhar, Jaskirat S, Joye, Ashlin S, Somkijrungroj, Thanapong, Laovirojjanakul, Wipada, Lin, Chang-Ping, Lietman, Thomas M, Porco, Travis C, Keenan, Jeremy D, Gebreegziabher, Elisabeth A, Seitzman, Gerami D, Rose-Nussbaumer, Jennifer, Doan, Thuy A, Acharya, Nisha R, and Gonzales, John A

Abstract

IntroductionCytomegalovirus (CMV) anterior uveitis is a recognised cause of anterior uveitis in immunocompetent patients and is preventable cause of vision loss. Ocular sequelae include corneal endothelial damage which can cause corneal oedema and failure, as well as glaucoma. Recurrences of inflammation are common and therefore patients are often exposed to long-term therapy. Oral therapy is available in the form of valganciclovir, although with the caveat of systemic side effects such as bone marrow suppression and renal failure necessitating regular interval laboratory monitoring. Recent reports have demonstrated that topical 2% ganciclovir solution may offer promising treatment outcomes in patients with CMV anterior uveitis with superior safety, cost-effectiveness and convenience profiles. An investigation into the relative equipoise of these therapies is warranted for these reasons.Methods and analysisThe Systemic and Topical Control of Cytomegalovirus Anterior uveitis: Treatment Outcomes (STACCATO) trial is designed as a multicentre, block randomised by site, double-masked, placebo-controlled trial comparing the efficacy of oral valganciclovir, 2% topical ganciclovir and placebo in treating PCR-proven CMV anterior uveitis. Participant clinical evaluation will occur at three study time points by a masked study ophthalmologist over a 28-day period to assess resolution of ocular inflammation (secondary outcome). A control group will provide additional information about the possible impact that the infected host's immune response may play in controlling local viral replication. The primary analysis is an analysis of covariance (three arms) correcting for baseline to compare quantitative CMV viral load in the anterior chamber (AC) aqueous fluid before and 7 days after treatment.Ethics and disseminationThe University of California San Francisco Committee on Human Research and the Khon Kaen University Institutional Review Board have given ethical approval. The result

Published

2019

14. Targeting senescent cells alleviates obesity-induced metabolic dysfunction.

Author

Palmer, Allyson K, Palmer, Allyson K, Xu, Ming, Zhu, Yi, Pirtskhalava, Tamar, Weivoda, Megan M, Hachfeld, Christine M, Prata, Larissa G, van Dijk, Theo H, Verkade, Esther, Casaclang-Verzosa, Grace, Johnson, Kurt O, Cubro, Hajrunisa, Doornebal, Ewald J, Ogrodnik, Mikolaj, Jurk, Diana, Jensen, Michael D, Chini, Eduardo N, Miller, Jordan D, Matveyenko, Aleksey, Stout, Michael B, Schafer, Marissa J, White, Thomas A, Hickson, LaTonya J, Demaria, Marco, Garovic, Vesna, Grande, Joseph, Arriaga, Edgar A, Kuipers, Folkert, von Zglinicki, Thomas, LeBrasseur, Nathan K, Campisi, Judith, Tchkonia, Tamar, Kirkland, James L, Palmer, Allyson K, Palmer, Allyson K, Xu, Ming, Zhu, Yi, Pirtskhalava, Tamar, Weivoda, Megan M, Hachfeld, Christine M, Prata, Larissa G, van Dijk, Theo H, Verkade, Esther, Casaclang-Verzosa, Grace, Johnson, Kurt O, Cubro, Hajrunisa, Doornebal, Ewald J, Ogrodnik, Mikolaj, Jurk, Diana, Jensen, Michael D, Chini, Eduardo N, Miller, Jordan D, Matveyenko, Aleksey, Stout, Michael B, Schafer, Marissa J, White, Thomas A, Hickson, LaTonya J, Demaria, Marco, Garovic, Vesna, Grande, Joseph, Arriaga, Edgar A, Kuipers, Folkert, von Zglinicki, Thomas, LeBrasseur, Nathan K, Campisi, Judith, Tchkonia, Tamar, and Kirkland, James L

Abstract

Adipose tissue inflammation and dysfunction are associated with obesity-related insulin resistance and diabetes, but mechanisms underlying this relationship are unclear. Although senescent cells accumulate in adipose tissue of obese humans and rodents, a direct pathogenic role for these cells in the development of diabetes remains to be demonstrated. Here, we show that reducing senescent cell burden in obese mice, either by activating drug-inducible "suicide" genes driven by the p16Ink4a promoter or by treatment with senolytic agents, alleviates metabolic and adipose tissue dysfunction. These senolytic interventions improved glucose tolerance, enhanced insulin sensitivity, lowered circulating inflammatory mediators, and promoted adipogenesis in obese mice. Elimination of senescent cells also prevented the migration of transplanted monocytes into intra-abdominal adipose tissue and reduced the number of macrophages in this tissue. In addition, microalbuminuria, renal podocyte function, and cardiac diastolic function improved with senolytic therapy. Our results implicate cellular senescence as a causal factor in obesity-related inflammation and metabolic derangements and show that emerging senolytic agents hold promise for treating obesity-related metabolic dysfunction and its complications.

Published

2019

15. Systemic clearance of p16INK4a -positive senescent cells mitigates age-associated intervertebral disc degeneration.

Author

Patil, Prashanti, Patil, Prashanti, Dong, Qing, Wang, Dong, Chang, Jianhui, Wiley, Christopher, Demaria, Marco, Lee, Joon, Kang, James, Niedernhofer, Laura J, Robbins, Paul D, Sowa, Gwendolyn, Campisi, Judith, Zhou, Daohong, Vo, Nam, Patil, Prashanti, Patil, Prashanti, Dong, Qing, Wang, Dong, Chang, Jianhui, Wiley, Christopher, Demaria, Marco, Lee, Joon, Kang, James, Niedernhofer, Laura J, Robbins, Paul D, Sowa, Gwendolyn, Campisi, Judith, Zhou, Daohong, and Vo, Nam

Abstract

RationaleAge-related changes in the intervertebral discs are the predominant contributors to back pain, a common physical and functional impairment experienced by older persons. Cellular senescence, a process wherein cells undergo growth arrest and chronically secrete numerous inflammatory molecules and proteases, has been reported to cause decline in the health and function of multiple tissues with age. Although senescent cells have been reported to increase in intervertebral degeneration (IDD), it is not known whether they are causative in age-related IDD.ObjectiveThe study aimed to elucidate whether a causal relationship exists between cellular senescence and age-related IDD.Methods and resultsTo examine the impact of senescent cells on age-associated IDD, we used p16-3MR transgenic mice, which enables the selective removal of p16Ink4a -positive senescent cells by the drug ganciclovir. Disc cellularity, aggrecan content and fragmentation alongside expression of inflammatory cytokine (IL-6) and matrix proteases (ADAMTS4 and MMP13) in discs of p16-3MR mice treated with GCV and untreated controls were assessed. In aged mice, reducing the per cent of senescent cells decreased disc aggrecan proteolytic degradation and increased overall proteoglycan matrix content along with improved histological disc features. Additionally, reduction of senescent cells lowered the levels of MMP13, which is purported to promote disc degenerative changes during aging.ConclusionsThe findings of this study suggest that systemic reduction in the number of senescent cells ameliorates multiple age-associated changes within the disc tissue. Cellular senescence could therefore serve as a therapeutic target to restore the health of disc tissue that deteriorates with age.

Published

2019

16. Systemic clearance of p16INK4a -positive senescent cells mitigates age-associated intervertebral disc degeneration.

Author

Patil, Prashanti, Patil, Prashanti, Dong, Qing, Wang, Dong, Chang, Jianhui, Wiley, Christopher, Demaria, Marco, Lee, Joon, Kang, James, Niedernhofer, Laura J, Robbins, Paul D, Sowa, Gwendolyn, Campisi, Judith, Zhou, Daohong, Vo, Nam, Patil, Prashanti, Patil, Prashanti, Dong, Qing, Wang, Dong, Chang, Jianhui, Wiley, Christopher, Demaria, Marco, Lee, Joon, Kang, James, Niedernhofer, Laura J, Robbins, Paul D, Sowa, Gwendolyn, Campisi, Judith, Zhou, Daohong, and Vo, Nam

Abstract

RationaleAge-related changes in the intervertebral discs are the predominant contributors to back pain, a common physical and functional impairment experienced by older persons. Cellular senescence, a process wherein cells undergo growth arrest and chronically secrete numerous inflammatory molecules and proteases, has been reported to cause decline in the health and function of multiple tissues with age. Although senescent cells have been reported to increase in intervertebral degeneration (IDD), it is not known whether they are causative in age-related IDD.ObjectiveThe study aimed to elucidate whether a causal relationship exists between cellular senescence and age-related IDD.Methods and resultsTo examine the impact of senescent cells on age-associated IDD, we used p16-3MR transgenic mice, which enables the selective removal of p16Ink4a -positive senescent cells by the drug ganciclovir. Disc cellularity, aggrecan content and fragmentation alongside expression of inflammatory cytokine (IL-6) and matrix proteases (ADAMTS4 and MMP13) in discs of p16-3MR mice treated with GCV and untreated controls were assessed. In aged mice, reducing the per cent of senescent cells decreased disc aggrecan proteolytic degradation and increased overall proteoglycan matrix content along with improved histological disc features. Additionally, reduction of senescent cells lowered the levels of MMP13, which is purported to promote disc degenerative changes during aging.ConclusionsThe findings of this study suggest that systemic reduction in the number of senescent cells ameliorates multiple age-associated changes within the disc tissue. Cellular senescence could therefore serve as a therapeutic target to restore the health of disc tissue that deteriorates with age.

Published

2019

17. Targeting senescent cells alleviates obesity-induced metabolic dysfunction.

Author

Palmer, Allyson K, Palmer, Allyson K, Xu, Ming, Zhu, Yi, Pirtskhalava, Tamar, Weivoda, Megan M, Hachfeld, Christine M, Prata, Larissa G, van Dijk, Theo H, Verkade, Esther, Casaclang-Verzosa, Grace, Johnson, Kurt O, Cubro, Hajrunisa, Doornebal, Ewald J, Ogrodnik, Mikolaj, Jurk, Diana, Jensen, Michael D, Chini, Eduardo N, Miller, Jordan D, Matveyenko, Aleksey, Stout, Michael B, Schafer, Marissa J, White, Thomas A, Hickson, LaTonya J, Demaria, Marco, Garovic, Vesna, Grande, Joseph, Arriaga, Edgar A, Kuipers, Folkert, von Zglinicki, Thomas, LeBrasseur, Nathan K, Campisi, Judith, Tchkonia, Tamar, Kirkland, James L, Palmer, Allyson K, Palmer, Allyson K, Xu, Ming, Zhu, Yi, Pirtskhalava, Tamar, Weivoda, Megan M, Hachfeld, Christine M, Prata, Larissa G, van Dijk, Theo H, Verkade, Esther, Casaclang-Verzosa, Grace, Johnson, Kurt O, Cubro, Hajrunisa, Doornebal, Ewald J, Ogrodnik, Mikolaj, Jurk, Diana, Jensen, Michael D, Chini, Eduardo N, Miller, Jordan D, Matveyenko, Aleksey, Stout, Michael B, Schafer, Marissa J, White, Thomas A, Hickson, LaTonya J, Demaria, Marco, Garovic, Vesna, Grande, Joseph, Arriaga, Edgar A, Kuipers, Folkert, von Zglinicki, Thomas, LeBrasseur, Nathan K, Campisi, Judith, Tchkonia, Tamar, and Kirkland, James L

Abstract

Adipose tissue inflammation and dysfunction are associated with obesity-related insulin resistance and diabetes, but mechanisms underlying this relationship are unclear. Although senescent cells accumulate in adipose tissue of obese humans and rodents, a direct pathogenic role for these cells in the development of diabetes remains to be demonstrated. Here, we show that reducing senescent cell burden in obese mice, either by activating drug-inducible "suicide" genes driven by the p16Ink4a promoter or by treatment with senolytic agents, alleviates metabolic and adipose tissue dysfunction. These senolytic interventions improved glucose tolerance, enhanced insulin sensitivity, lowered circulating inflammatory mediators, and promoted adipogenesis in obese mice. Elimination of senescent cells also prevented the migration of transplanted monocytes into intra-abdominal adipose tissue and reduced the number of macrophages in this tissue. In addition, microalbuminuria, renal podocyte function, and cardiac diastolic function improved with senolytic therapy. Our results implicate cellular senescence as a causal factor in obesity-related inflammation and metabolic derangements and show that emerging senolytic agents hold promise for treating obesity-related metabolic dysfunction and its complications.

Published

2019

18. A double masked randomised 4-week, placebo-controlled study in the USA, Thailand and Taiwan to compare the efficacy of oral valganciclovir and topical 2% ganciclovir in the treatment of cytomegalovirus anterior uveitis: study protocol.

Author

Takhar, Jaskirat S, Takhar, Jaskirat S, Joye, Ashlin S, Somkijrungroj, Thanapong, Laovirojjanakul, Wipada, Lin, Chang-Ping, Lietman, Thomas M, Porco, Travis C, Keenan, Jeremy D, Gebreegziabher, Elisabeth A, Seitzman, Gerami D, Rose-Nussbaumer, Jennifer, Doan, Thuy A, Acharya, Nisha R, Gonzales, John A, Takhar, Jaskirat S, Takhar, Jaskirat S, Joye, Ashlin S, Somkijrungroj, Thanapong, Laovirojjanakul, Wipada, Lin, Chang-Ping, Lietman, Thomas M, Porco, Travis C, Keenan, Jeremy D, Gebreegziabher, Elisabeth A, Seitzman, Gerami D, Rose-Nussbaumer, Jennifer, Doan, Thuy A, Acharya, Nisha R, and Gonzales, John A

Abstract

IntroductionCytomegalovirus (CMV) anterior uveitis is a recognised cause of anterior uveitis in immunocompetent patients and is preventable cause of vision loss. Ocular sequelae include corneal endothelial damage which can cause corneal oedema and failure, as well as glaucoma. Recurrences of inflammation are common and therefore patients are often exposed to long-term therapy. Oral therapy is available in the form of valganciclovir, although with the caveat of systemic side effects such as bone marrow suppression and renal failure necessitating regular interval laboratory monitoring. Recent reports have demonstrated that topical 2% ganciclovir solution may offer promising treatment outcomes in patients with CMV anterior uveitis with superior safety, cost-effectiveness and convenience profiles. An investigation into the relative equipoise of these therapies is warranted for these reasons.Methods and analysisThe Systemic and Topical Control of Cytomegalovirus Anterior uveitis: Treatment Outcomes (STACCATO) trial is designed as a multicentre, block randomised by site, double-masked, placebo-controlled trial comparing the efficacy of oral valganciclovir, 2% topical ganciclovir and placebo in treating PCR-proven CMV anterior uveitis. Participant clinical evaluation will occur at three study time points by a masked study ophthalmologist over a 28-day period to assess resolution of ocular inflammation (secondary outcome). A control group will provide additional information about the possible impact that the infected host's immune response may play in controlling local viral replication. The primary analysis is an analysis of covariance (three arms) correcting for baseline to compare quantitative CMV viral load in the anterior chamber (AC) aqueous fluid before and 7 days after treatment.Ethics and disseminationThe University of California San Francisco Committee on Human Research and the Khon Kaen University Institutional Review Board have given ethical approval. The result

Published

2019

19. Cell Death Induction of Thymidine Kinase Gene Transfer Followed by Ganciclovir Treatment in Oral Squamous Cell Carcinoma Cell Lines

Author

Kuratate, Itaru, Osaki, Mitsuhiko, Ryoke, Kazuo, Kuratate, Itaru, Osaki, Mitsuhiko, and Ryoke, Kazuo

Abstract

The tumoricidal effect of herpes simplex virus thymidine kinase (HSV-tk) gene transfer followed by ganciclovir (GCV) treatment has been demonstrated in relation to the bystander effect. We examined the mode of cell death after GCV treatment in three human oral squamous cell carcinoma (SCC) cell lines that had been infected with adenovirus possessing HSV-tk gene. Oral SCC cell lines displayed high susceptibility to HSV-tk/GCV treatment despite low transduction. Evidence suggests that apoptosis was not found by internucleosomal DNA fragmentation, cell cycle kinetics or gene expressions indicative of apoptosis. However, we observed different levels of expression of annexin V-positive/propidium iodide-negative cells in all the cell lines and occasional TUNEL-positive cells in one cell line. To address these controversial findings, we further confirmed the morphological phenotypes of cell death with semi-thin and ultra-thin sections, which revealed that the cells undergoing death were consistent with necrosis, i.e. swelling of cytoplasm and intracellular organs with membrane disruption. Furthermore, no apoptotic bodies were detected within cytoplasm of apparently intact cells. A nonapoptotic mechanism may play a central role in the HSV-tk/GCV-induced cell death in oral SCC cell lines.

Published

2018

20. Cutaneous ulcers in ganciclovir-resistant cytomegalovirus infection.

Author

Wang C., Mar A., Wang C., and Mar A.

Abstract

Cytomegalovirus (CMV) infection represents a major cause of morbidity and mortality in immunocompromised hosts. The disease spectrum of CMV infection can range from asymptomatic or a mild mononucleosis syndrome to significant tissue-invasive disease especially hepatitis, colitis, pneumonitis and retinitis. Cutaneous CMV infection is rare, however it may herald resistant or disseminated disease. We describe a case of a 67 year-old male renal transplant recipient that suffered both recurrent CMV-related ulcers around his genitalia and right leg, as well as a Marjolin ulcer. He subsequently developed retinitis and a viraemia that was resistant to ganciclovir. Treatment with foscarnet improved ocular and cutaneous disease, however ultimately withdrawal of immunosuppression was required.

Published

2018

21. Cutaneous ulcers in ganciclovir-resistant cytomegalovirus infection.

Author

Wang C., Mar A., Wang C., and Mar A.

Abstract

Cytomegalovirus (CMV) infection represents a major cause of morbidity and mortality in immunocompromised hosts. The disease spectrum of CMV infection can range from asymptomatic or a mild mononucleosis syndrome to significant tissue-invasive disease especially hepatitis, colitis, pneumonitis and retinitis. Cutaneous CMV infection is rare, however it may herald resistant or disseminated disease. We describe a case of a 67 year-old male renal transplant recipient that suffered both recurrent CMV-related ulcers around his genitalia and right leg, as well as a Marjolin ulcer. He subsequently developed retinitis and a viraemia that was resistant to ganciclovir. Treatment with foscarnet improved ocular and cutaneous disease, however ultimately withdrawal of immunosuppression was required.

Published

2018

22. Perfil clínico de la infección congénita por Citomegalovirus

Author

Yousseph, Yarelis, Carnevale, Mayli, Yousseph, Yarelis, and Carnevale, Mayli

Abstract

Cytomegalovirus (CMV) infection is considered the most common cause of viral infection in pregnant women, the fetus and newborn. With the aim of describing the clinical profile of congenital cytomegalovirus infection in patients admitted in the Servicio Desconcentrado Hospital Pediátrico Dr. Agustín Zubillaga during the 2012-2016 period, we conducted a retrospective study selecting 33 clinical histories to review; 60.6% of patients had congenital CMV infection while 39.3% had TORCH syndrome. 63.6% of patients were < 7 days at the moment of diagnosis, predominantly male (63.6%), with a gestational age < 36 weeks (69.7%) and a birth weight between 2501-3000 grs (51.5%). The average age of diagnosis was 17.9 ± 10.4 days; 96.9% of patients had jaundice, petechial rash (42.4%), enteritis and hepatosplenomegaly (27.2%, respectively). Hyperbilirubinemia was found in 96,9% of patients, leukocytosis in 72,7%, thrombocytopenia in 81.8% and high glutamic oxalacetic and pyruvic transaminase levels in 78.7% and 42.4% of cases. 96.9% of cases reported positive blood PCR, 18.1% positive PCR in urine and 3% positive IgM. Only 12.1% of patients received human immunoglobulin and 6% received ganciclovir. The average hospital stay was 25.2 ± 12.5 days and 90.9% of patients responded satisfactorily. This study provides relevant information on the clinical profile of congenital CMV infection in order to help improve the management of this type of cases in our hospital., La infección por Citomegalovirus (CMV) se considera la infección viral más frecuente en la gestante, el feto y el recién nacido. Con el objetivo de describir el perfil clínico de la infección congénita por Citomegalovirus en pacientes que ingresaron al Servicio Desconcentrado Hospital Pediátrico Dr. Agustín Zubillaga durante el lapso 2012-2016, se realizó un estudio retrospectivo seleccionando un total de 33 historias clínicas para su evaluación; 60,6% de pacientes presentaron infección congénita por CMV mientras que 39,3% fueron diagnosticados con síndrome de TORCH. El mayor porcentaje de pacientes tenían una edad menor a 7 días (63,6%), con predominio del sexo masculino (63,6%), edad gestacional menor de 36 semanas (69,7%) y un peso al nacer entre 2501-3000 grs (51,5%). La edad promedio del diagnóstico fue de 17,9 ± 10,4 días. El 96,9% de los pacientes presentaron ictericia, petequias (42,4%), enteritis y hepatoesplenomegalia (27,2%, respectivamente). Entre los resultados paraclínicos, 96,9% de los pacientes presentó hiperbilirrubinemia, leucocitosis (72,7%), trombocitopenia (81,8%), aumento de las transaminasas glutámico oxalacética y pirúvica (78,7% y 42,4%, respectivamente). El 96,9% de los pacientes reportaron PCR positivo en sangre, mientras que en 18,1% de los casos el PCR fue positivo en orina y 3% presentaron IgM positiva. Sólo 12,1% de los pacientes recibieron inmunoglobulina humana y 6% recibieron ganciclovir. El tiempo de evolución promedio fue de 25,2 ± 12,5 días y 90,9% de los pacientes evolucionaron satisfactoriamente. En conclusión, este estudio aporta información relevante sobre el perfil clínico de la infección congénita por CMV con el fin de contribuir a mejorar la atención de este tipo de casos en nuestro centro de salud.

Published

2018

23. Queratitis por herpes simple: revisión de literatura

Author

García Acevedo, Federico and García Acevedo, Federico

Abstract

Introducción: La queratitis herpética es una de las causas de ceguera infecciosa más común de los países desarrollados. A pesar de que no se ha podido determinar el impacto real, el impacto global se calcula en aproximadamente 1 a 1,5 millones de casos.Objetivo: Describir los hallazgos en la literatura actual sobre queratitis herpética.Método: Revisión de la literatura científica entre 2008 y 2018 en queratitis herpética sobre aspectos inherentes al virus y la patología corneal. Se tomaron en cuenta artículos de revisión y artículos originales relacionados con la epidemiología, fisiopatología, clínica, diagnóstico y tratamiento a través de Pubmed usando los siguientes términos MeSH: Herpes simplex virus, herpes simplex keratitis, HSV, keratitis, acyclovir, ganciclovir, corneal vascularisation.Resultados: En la búsqueda de la literatura se encontraron 20 artículos donde se evidencia que en los países en vía de desarrollo hay muy pocos estudios sobre la incidencia y prevalencia de la enfermedad en la población y que nos regimos por datos epidemiológicos de los países desarrollados para la toma de decisiones clínicas. Se describe la fisiopatología y respuesta inmune de la infección por el Herpes virus a nivel celular y molecular lo que permite entender la presentación clínica y curso de la infección. Igualmente se describen pruebas diagnósticas y abordajes terapéuticos clásicos y recientes.Conclusión: A través de la revisión de la literatura encontramos que la queratitis herpética sigue teniendo una gran incidencia en la población mundial, pero gracias a los tratamientos nuevos y existentes se puede disminuir de manera importante la morbilidad en estos pacientes.

Published

2018

24. Pre-clinical development of gene modification of haematopoietic stem cells with chimeric antigen receptors for cancer immunotherapy.

Author

Larson, Sarah M, Larson, Sarah M, Truscott, Laurel C, Chiou, Tzu-Ting, Patel, Amie, Kao, Roy, Tu, Andy, Tyagi, Tulika, Lu, Xiang, Elashoff, David, De Oliveira, Satiro N, Larson, Sarah M, Larson, Sarah M, Truscott, Laurel C, Chiou, Tzu-Ting, Patel, Amie, Kao, Roy, Tu, Andy, Tyagi, Tulika, Lu, Xiang, Elashoff, David, and De Oliveira, Satiro N

Abstract

Patients with refractory or recurrent B-lineage hematologic malignancies have less than 50% of chance of cure despite intensive therapy and innovative approaches are needed. We hypothesize that gene modification of haematopoietic stem cells (HSC) with an anti-CD19 chimeric antigen receptor (CAR) will produce a multi-lineage, persistent immunotherapy against B-lineage malignancies that can be controlled by the HSVsr39TK suicide gene. High-titer third-generation self-inactivating lentiviral constructs were developed to deliver a second-generation CD19-specific CAR and the herpes simplex virus thymidine kinase HSVsr39TK to provide a suicide gene to allow ablation of gene-modified cells if necessary. Human HSC were transduced with such lentiviral vectors and evaluated for function of both CAR and HSVsr39TK. Satisfactory transduction efficiency was achieved; the addition of the suicide gene did not impair CAR expression or antigen-specific cytotoxicity, and determined marked cytotoxicity to ganciclovir. NSG mice transplanted with gene-modified human HSC showed CAR expression not significantly different between transduced cells with or without HSVsr39TK, and expression of anti-CD19 CAR conferred anti-tumor survival advantage. Treatment with ganciclovir led to significant ablation of gene-modified cells in mouse tissues. Haematopoietic stem cell transplantation is frequently part of the standard of care for patients with relapsed and refractory B cell malignancies; following HSC collection, a portion of the cells could be modified to express the CD19-specific CAR and give rise to a persistent, multi-cell lineage, HLA-independent immunotherapy, enhancing the graft-versus-malignancy activity.

Published

2017

25. Local clearance of senescent cells attenuates the development of post-traumatic osteoarthritis and creates a pro-regenerative environment.

Author

Jeon, Ok Hee, Jeon, Ok Hee, Kim, Chaekyu, Laberge, Remi-Martin, Demaria, Marco, Rathod, Sona, Vasserot, Alain P, Chung, Jae Wook, Kim, Do Hun, Poon, Yan, David, Nathaniel, Baker, Darren J, van Deursen, Jan M, Campisi, Judith, Elisseeff, Jennifer H, Jeon, Ok Hee, Jeon, Ok Hee, Kim, Chaekyu, Laberge, Remi-Martin, Demaria, Marco, Rathod, Sona, Vasserot, Alain P, Chung, Jae Wook, Kim, Do Hun, Poon, Yan, David, Nathaniel, Baker, Darren J, van Deursen, Jan M, Campisi, Judith, and Elisseeff, Jennifer H

Abstract

Senescent cells (SnCs) accumulate in many vertebrate tissues with age and contribute to age-related pathologies, presumably through their secretion of factors contributing to the senescence-associated secretory phenotype (SASP). Removal of SnCs delays several pathologies and increases healthy lifespan. Aging and trauma are risk factors for the development of osteoarthritis (OA), a chronic disease characterized by degeneration of articular cartilage leading to pain and physical disability. Senescent chondrocytes are found in cartilage tissue isolated from patients undergoing joint replacement surgery, yet their role in disease pathogenesis is unknown. To test the idea that SnCs might play a causative role in OA, we used the p16-3MR transgenic mouse, which harbors a p16INK4a (Cdkn2a) promoter driving the expression of a fusion protein containing synthetic Renilla luciferase and monomeric red fluorescent protein domains, as well as a truncated form of herpes simplex virus 1 thymidine kinase (HSV-TK). This mouse strain allowed us to selectively follow and remove SnCs after anterior cruciate ligament transection (ACLT). We found that SnCs accumulated in the articular cartilage and synovium after ACLT, and selective elimination of these cells attenuated the development of post-traumatic OA, reduced pain and increased cartilage development. Intra-articular injection of a senolytic molecule that selectively killed SnCs validated these results in transgenic, non-transgenic and aged mice. Selective removal of the SnCs from in vitro cultures of chondrocytes isolated from patients with OA undergoing total knee replacement decreased expression of senescent and inflammatory markers while also increasing expression of cartilage tissue extracellular matrix proteins. Collectively, these findings support the use of SnCs as a therapeutic target for treating degenerative joint disease.

Published

2017

26. Pre-clinical development of gene modification of haematopoietic stem cells with chimeric antigen receptors for cancer immunotherapy.

Author

Larson, Sarah M, Larson, Sarah M, Truscott, Laurel C, Chiou, Tzu-Ting, Patel, Amie, Kao, Roy, Tu, Andy, Tyagi, Tulika, Lu, Xiang, Elashoff, David, De Oliveira, Satiro N, Larson, Sarah M, Larson, Sarah M, Truscott, Laurel C, Chiou, Tzu-Ting, Patel, Amie, Kao, Roy, Tu, Andy, Tyagi, Tulika, Lu, Xiang, Elashoff, David, and De Oliveira, Satiro N

Abstract

Patients with refractory or recurrent B-lineage hematologic malignancies have less than 50% of chance of cure despite intensive therapy and innovative approaches are needed. We hypothesize that gene modification of haematopoietic stem cells (HSC) with an anti-CD19 chimeric antigen receptor (CAR) will produce a multi-lineage, persistent immunotherapy against B-lineage malignancies that can be controlled by the HSVsr39TK suicide gene. High-titer third-generation self-inactivating lentiviral constructs were developed to deliver a second-generation CD19-specific CAR and the herpes simplex virus thymidine kinase HSVsr39TK to provide a suicide gene to allow ablation of gene-modified cells if necessary. Human HSC were transduced with such lentiviral vectors and evaluated for function of both CAR and HSVsr39TK. Satisfactory transduction efficiency was achieved; the addition of the suicide gene did not impair CAR expression or antigen-specific cytotoxicity, and determined marked cytotoxicity to ganciclovir. NSG mice transplanted with gene-modified human HSC showed CAR expression not significantly different between transduced cells with or without HSVsr39TK, and expression of anti-CD19 CAR conferred anti-tumor survival advantage. Treatment with ganciclovir led to significant ablation of gene-modified cells in mouse tissues. Haematopoietic stem cell transplantation is frequently part of the standard of care for patients with relapsed and refractory B cell malignancies; following HSC collection, a portion of the cells could be modified to express the CD19-specific CAR and give rise to a persistent, multi-cell lineage, HLA-independent immunotherapy, enhancing the graft-versus-malignancy activity.

Published

2017

27. Local clearance of senescent cells attenuates the development of post-traumatic osteoarthritis and creates a pro-regenerative environment.

Author

Jeon, Ok Hee, Jeon, Ok Hee, Kim, Chaekyu, Laberge, Remi-Martin, Demaria, Marco, Rathod, Sona, Vasserot, Alain P, Chung, Jae Wook, Kim, Do Hun, Poon, Yan, David, Nathaniel, Baker, Darren J, van Deursen, Jan M, Campisi, Judith, Elisseeff, Jennifer H, Jeon, Ok Hee, Jeon, Ok Hee, Kim, Chaekyu, Laberge, Remi-Martin, Demaria, Marco, Rathod, Sona, Vasserot, Alain P, Chung, Jae Wook, Kim, Do Hun, Poon, Yan, David, Nathaniel, Baker, Darren J, van Deursen, Jan M, Campisi, Judith, and Elisseeff, Jennifer H

Abstract

Senescent cells (SnCs) accumulate in many vertebrate tissues with age and contribute to age-related pathologies, presumably through their secretion of factors contributing to the senescence-associated secretory phenotype (SASP). Removal of SnCs delays several pathologies and increases healthy lifespan. Aging and trauma are risk factors for the development of osteoarthritis (OA), a chronic disease characterized by degeneration of articular cartilage leading to pain and physical disability. Senescent chondrocytes are found in cartilage tissue isolated from patients undergoing joint replacement surgery, yet their role in disease pathogenesis is unknown. To test the idea that SnCs might play a causative role in OA, we used the p16-3MR transgenic mouse, which harbors a p16INK4a (Cdkn2a) promoter driving the expression of a fusion protein containing synthetic Renilla luciferase and monomeric red fluorescent protein domains, as well as a truncated form of herpes simplex virus 1 thymidine kinase (HSV-TK). This mouse strain allowed us to selectively follow and remove SnCs after anterior cruciate ligament transection (ACLT). We found that SnCs accumulated in the articular cartilage and synovium after ACLT, and selective elimination of these cells attenuated the development of post-traumatic OA, reduced pain and increased cartilage development. Intra-articular injection of a senolytic molecule that selectively killed SnCs validated these results in transgenic, non-transgenic and aged mice. Selective removal of the SnCs from in vitro cultures of chondrocytes isolated from patients with OA undergoing total knee replacement decreased expression of senescent and inflammatory markers while also increasing expression of cartilage tissue extracellular matrix proteins. Collectively, these findings support the use of SnCs as a therapeutic target for treating degenerative joint disease.

Published

2017

28. Effectiveness of Preemptive Therapy for Cytomegalovirus Disease in Pediatric Liver Transplantation

Author

Nicastro, E, Giovannozzi, S, Stroppa, P, Casotti, V, Callegaro, A, Tebaldi, A, Farina, C, Colledan, M, D'Antiga, L, Nicastro E, Giovannozzi S, Stroppa P, Casotti V, Callegaro AP, Tebaldi A, Farina C, Colledan M, D'Antiga L, Nicastro, E, Giovannozzi, S, Stroppa, P, Casotti, V, Callegaro, A, Tebaldi, A, Farina, C, Colledan, M, D'Antiga, L, Nicastro E, Giovannozzi S, Stroppa P, Casotti V, Callegaro AP, Tebaldi A, Farina C, Colledan M, and D'Antiga L

Abstract

Background Most pediatric liver transplantation (LT) centers administer long courses of prophylaxis against cytomegalovirus (CMV) without evidence of benefit and with significant drug exposure and costs. We aimed at evaluating overall outcomes, direct and putative indirect effects of CMV, possible impact of viremia and risk factors for CMV infection in pediatric LT recipients managed with ganciclovir-based preemptive therapy (PET). Methods The records of all the children who underwent LT between 2008 and 2014 were retrospectively analyzed. Results One hundred children were included. Three children had CMV disease; no CMV-related death or graft loss was recorded. The only identified risk factor for CMV infection was the donor/recipient serostatus (odds ratio, 17.23; 95% confidence interval, 1.88-157.87; P = 0.012), while viremia per se did not worsen LT outcomes, such as the incidence of acute rejection, Epstein-Barr virus infection, sepsis, biliary and vascular complications, nor graft dysfunction/loss or death at 3 and 5 years after LT. When compared with a historical cohort of children receiving ganciclovir prophylaxis, PET did not differ from prophylaxis for any of the selected outcomes, but was rather associated with lower antiviral drug exposure (6.4 ± 13 days vs 38.6 ± 14 days, P < 0.0001) and cost per patient (2.2 ± 3.9 k€ vs 6.6 ± 8.2 k€, P = 0.001). Conclusions PET is effective in controlling CMV in children receiving LT, with lower costs and lower exposure to antivirals.

Published

2017

29. Clearance of senescent cells by ABT263 rejuvenates aged hematopoietic stem cells in mice.

Author

Chang, Jianhui, Chang, Jianhui, Wang, Yingying, Shao, Lijian, Laberge, Remi-Martin, Demaria, Marco, Campisi, Judith, Janakiraman, Krishnamurthy, Sharpless, Norman E, Ding, Sheng, Feng, Wei, Luo, Yi, Wang, Xiaoyan, Aykin-Burns, Nukhet, Krager, Kimberly, Ponnappan, Usha, Hauer-Jensen, Martin, Meng, Aimin, Zhou, Daohong, Chang, Jianhui, Chang, Jianhui, Wang, Yingying, Shao, Lijian, Laberge, Remi-Martin, Demaria, Marco, Campisi, Judith, Janakiraman, Krishnamurthy, Sharpless, Norman E, Ding, Sheng, Feng, Wei, Luo, Yi, Wang, Xiaoyan, Aykin-Burns, Nukhet, Krager, Kimberly, Ponnappan, Usha, Hauer-Jensen, Martin, Meng, Aimin, and Zhou, Daohong

Abstract

Senescent cells (SCs) accumulate with age and after genotoxic stress, such as total-body irradiation (TBI). Clearance of SCs in a progeroid mouse model using a transgenic approach delays several age-associated disorders, suggesting that SCs play a causative role in certain age-related pathologies. Thus, a 'senolytic' pharmacological agent that can selectively kill SCs holds promise for rejuvenating tissue stem cells and extending health span. To test this idea, we screened a collection of compounds and identified ABT263 (a specific inhibitor of the anti-apoptotic proteins BCL-2 and BCL-xL) as a potent senolytic drug. We show that ABT263 selectively kills SCs in culture in a cell type- and species-independent manner by inducing apoptosis. Oral administration of ABT263 to either sublethally irradiated or normally aged mice effectively depleted SCs, including senescent bone marrow hematopoietic stem cells (HSCs) and senescent muscle stem cells (MuSCs). Notably, this depletion mitigated TBI-induced premature aging of the hematopoietic system and rejuvenated the aged HSCs and MuSCs in normally aged mice. Our results demonstrate that selective clearance of SCs by a pharmacological agent is beneficial in part through its rejuvenation of aged tissue stem cells. Thus, senolytic drugs may represent a new class of radiation mitigators and anti-aging agents.

Published

2016

30. A prototype antifungal contact lens

Author

Ciolino, Joseph B., Hudson, Sarah P., Mobbs, Ashley N., Hoare, Todd R., Iwata, Naomi G., Fink, Gerald R., Kohane, Daniel S., Ciolino, Joseph B., Hudson, Sarah P., Mobbs, Ashley N., Hoare, Todd R., Iwata, Naomi G., Fink, Gerald R., and Kohane, Daniel S.

Abstract

peer-reviewed, PURPOSE. To design a contact lens to treat and prevent fungal ocular infections.METHODS. Curved contact lenses were created by encapsulating econazole-impregnated poly(lactic-co-glycolic) acid (PLGA) films in poly(hydroxyethyl methacrylate) (pHEMA) by ultraviolet photopolymerization. Release studies were conducted in phosphate-buffered saline at 37 degrees C with continuous shaking. The contact lenses and their release media were tested in an antifungal assay against Candida albicans. Cross sections of the pre- and postrelease contact lenses were characterized by scanning electron microscopy and by Raman spectroscopy.RESULTS. Econazole-eluting contact lenses provided extended antifungal activity against Candida albicans fungi. Fungicidal activity varied in duration and effectiveness depending on the mass of the econazole-PLGA film encapsulated in the contact lens.CONCLUSIONS. An econazole-eluting contact lens could be used as a treatment for fungal ocular infections. (Invest Ophthalmol Vis Sci. 2011;52:6286-6291) DOI:10.1167/iovs.10-6935, PUBLISHED, peer-reviewed

Published

2016

31. Clearance of senescent cells by ABT263 rejuvenates aged hematopoietic stem cells in mice.

Author

Chang, Jianhui, Chang, Jianhui, Wang, Yingying, Shao, Lijian, Laberge, Remi-Martin, Demaria, Marco, Campisi, Judith, Janakiraman, Krishnamurthy, Sharpless, Norman E, Ding, Sheng, Feng, Wei, Luo, Yi, Wang, Xiaoyan, Aykin-Burns, Nukhet, Krager, Kimberly, Ponnappan, Usha, Hauer-Jensen, Martin, Meng, Aimin, Zhou, Daohong, Chang, Jianhui, Chang, Jianhui, Wang, Yingying, Shao, Lijian, Laberge, Remi-Martin, Demaria, Marco, Campisi, Judith, Janakiraman, Krishnamurthy, Sharpless, Norman E, Ding, Sheng, Feng, Wei, Luo, Yi, Wang, Xiaoyan, Aykin-Burns, Nukhet, Krager, Kimberly, Ponnappan, Usha, Hauer-Jensen, Martin, Meng, Aimin, and Zhou, Daohong

Abstract

Senescent cells (SCs) accumulate with age and after genotoxic stress, such as total-body irradiation (TBI). Clearance of SCs in a progeroid mouse model using a transgenic approach delays several age-associated disorders, suggesting that SCs play a causative role in certain age-related pathologies. Thus, a 'senolytic' pharmacological agent that can selectively kill SCs holds promise for rejuvenating tissue stem cells and extending health span. To test this idea, we screened a collection of compounds and identified ABT263 (a specific inhibitor of the anti-apoptotic proteins BCL-2 and BCL-xL) as a potent senolytic drug. We show that ABT263 selectively kills SCs in culture in a cell type- and species-independent manner by inducing apoptosis. Oral administration of ABT263 to either sublethally irradiated or normally aged mice effectively depleted SCs, including senescent bone marrow hematopoietic stem cells (HSCs) and senescent muscle stem cells (MuSCs). Notably, this depletion mitigated TBI-induced premature aging of the hematopoietic system and rejuvenated the aged HSCs and MuSCs in normally aged mice. Our results demonstrate that selective clearance of SCs by a pharmacological agent is beneficial in part through its rejuvenation of aged tissue stem cells. Thus, senolytic drugs may represent a new class of radiation mitigators and anti-aging agents.

Published

2016

32. Citomegalovirus en el embarazo

Author

Chaverri Guillen, Gilbert and Chaverri Guillen, Gilbert

Abstract

Congenital infection with cytomegalovirus (CMV) represents the leading cause of maternal fetal infection, also is the leading cause of childhood deafness worldwide. Infected women can present a large number of events or asymptomatic. Most newborns and infants are asymptomatic at birth, but can present late sequelae such as mental retardation, learning disabilities, cerebral palsy, epilepsy, partial or total deafness or blindness and visual deficits. Mother diagnosis is based on the presence of antibodies in blood and fetal diagnosis is based on detection of immunocomplexes in amniotic fluid. Treatment during pregnancy has been used antiviral drugs such as ganciclovir and valganciclovir orally., La infección congénita por el citomegalovirus (CMV) representa la principal causa de infección materna fetal y es la principal causa de sordera infantil a nivel mundial. Las mujeres infectadas pueden presentar un gran número de manifestaciones o ser asintomáticas. La mayoría de recién nacidos y lactantes se encuentran asintomáticos al nacer, pero pueden presentar secuelas tardías como retardo mental, discapacidades en el aprendizaje, parálisis cerebral, epilepsia, sordera total o parcial y déficit visual o ceguera. El diagnóstico de la madre se basa en la presencia de anticuerpos en sangre y el diagnóstico fetal se basa en la detección de inmunocomplejos en líquido amniótico. El tratamiento durante el embarazo se ha utilizado antivirales como el ganciclovir y su forma oral valganciclovir.

Published

2016

33. Fatal lactic acidosis possibly related to ganciclovir therapy in a renal transplant patient?

Author

UCL - SSS/IREC/MEDA - Pôle de médecine aiguë, UCL - SSS/IREC/NEFR-Pôle de Néphrologie, UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de soins intensifs, UCL - (SLuc) Service de néphrologie, UCL - (SLuc) Service de biochimie médicale, Wittebole, Xavier, Morelle, Johann, Vincent, Marie-Françoise, Hantson, Philippe, UCL - SSS/IREC/MEDA - Pôle de médecine aiguë, UCL - SSS/IREC/NEFR-Pôle de Néphrologie, UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de soins intensifs, UCL - (SLuc) Service de néphrologie, UCL - (SLuc) Service de biochimie médicale, Wittebole, Xavier, Morelle, Johann, Vincent, Marie-Françoise, and Hantson, Philippe

Abstract

Ganciclovir is widely prescribed in renal transplant patients for the prevention or treatment of herpes and cytomegalovirus (CMV) infections. Side-effects are usually represented by hematological disorders, and particularly leucopenia. We report a case of severe and fatal lactic acidosis developing in a 76-year-old renal transplant woman, a few days after ganciclovir has been introduced to treat CMV pneumonia. Usual etiologies of lactic acidosis were ruled out. A high lactate/pyruvate molecular ratio was suggestive of a respiratory chain dysfunction. With the analogy to nucleoside analogues-related lactic acidosis, we suggest that ganciclovir may exceptionally be responsible for respiratory chain dysfunction and subsequent lactic acidosis, and we discuss potential risk factors in our patient.

Published

2015

34. Outflow tract ablation using a conditionally cytotoxic feline immunodeficiency viral vector.

Author

Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep S, Tseng, Harry, Kim, James D, Schuman, Joel S, Weinreb, Robert N, Loewen, Nils A, Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep S, Tseng, Harry, Kim, James D, Schuman, Joel S, Weinreb, Robert N, and Loewen, Nils A

Abstract

PurposeTo create an in vivo model of vector-mediated trabecular meshwork (TM) ablation and replacement.MethodsWe generated a conditionally cytotoxic, trackable vector, HSVtkiG, that expressed herpes simplex virus 1 thymidine kinase (HSVtk) and enhanced green fluorescent protein (eGFP). We optimized HSVtkiG ablation in vitro with ganciclovir (GCV) in comparison to eGFP control vector GINSIN and investigated the mechanism. Right eyes of 24 rats were then injected intracamerally with either HSVtkiG or GINSIN, before intraperitoneal GCV was administered 1 week later. Intraocular pressure, central corneal thickness (CCT), and slit-lamp exams were assessed for 8 weeks. Transduction and ablation were followed by gonioscopic visualization of eGFP. Histology was obtained with TM cell counts and immunohistochemistry markers of inflammation.ResultsTransduction and ablation parameters were established in vitro. Apoptosis was the cause of cell death. In vivo, transduction was seen gonioscopically to be targeted to the TM, followed by disappearance of eGFP marker fluorescence in HSVtkiG-transduced cells after injection of GCV. Ablation resulted in an IOP decrease of 25% in HSVtkiG-injected eyes 2 days after GCV but not in GINSIN or noninjected control eyes (P < 0.05). Trabecular meshwork cellularity was decreased at the time of lowest IOP and recovered thereafter, while CCT remained unchanged. Inflammation was absent.ConclusionsA vector-based system for inducible ablation of cells of the outflow tract was developed. Trabecular meshwork ablation lowered IOP, and recovery of cellularity and IOP followed. This model may be useful to study pressure regulation by the TM, its stem cells, and migration patterns.

Published

2014

35. Renal (and herpetic) re-transplantation.

Author

Robertson A., Hughes P.D., Setyapranata S., Wiggins K.J., Holt S.G., Mulley W.R., Kerr P.G., Landgren A.J., Young A., Opdam H., Robertson A., Hughes P.D., Setyapranata S., Wiggins K.J., Holt S.G., Mulley W.R., Kerr P.G., Landgren A.J., Young A., and Opdam H.

Abstract

Aim: Case report of renal re-transplantation, reported only once previously. Report: A middle aged recipient received a kidney transplant from a deceased multi-organ donor. After initially doing well, the patient suffered cardiac arrest several days post-operatively and sustained hypoxic brain injury and was declared brain dead. Following the family's consent, the allograft kidney was retrieved and re-transplanted into a man with end-stage renal failure secondary to reflux nephropathy. The lungs were used in a separate recipient but the liver was not transplanted due to suspicion of fatty changes based on macroscopic appearance. Histological analysis of the liver more than 24 hours after transplantation of the other organs revealed coagulative parenchymal necrosis with nuclear inclusions and moderate parenchymal cholestasis, suggestive of herpes viral hepatitis. Examination of the renal implantation biopsy showed histiocytes with enlarged nuclei containing viral inclusions in the capsular fibrous tissue, with positive immunostaining for herpes simplex virus (HSV). Valaciclovir was started immediately after obtaining histological evidence of donor HSV infection and this was subsequently converted to intravenous ganciclovir. Our recipient had pre-formed IgG antibodies to HSV-1 and HSV-2, and was IgM negative pretransplant. HSV viraemia was detected day 5 post-transplant with a viral load of 7688 copies/mL by polymerase chain reaction (PCR) assay. He completed a 30-day course of intravenous ganciclovir before switching to valganciclovir as standard cytomegalovirus prophylaxis. The HSV PCR became undetectable on day 7 of IV ganciclovir and has remained undetectable. The patient remains well with an estimated glomerular filtration rate of 61 mL/min/1.73 m2 and further investigation of the apparent viral transmission is underway. Conclusion(s): We report good short term results of renal re-transplantation and HSV transmission by transplantation.

Published

2014

36. Renal (and herpetic) re-transplantation.

Author

Robertson A., Hughes P.D., Setyapranata S., Wiggins K.J., Holt S.G., Mulley W.R., Kerr P.G., Landgren A.J., Young A., Opdam H., Robertson A., Hughes P.D., Setyapranata S., Wiggins K.J., Holt S.G., Mulley W.R., Kerr P.G., Landgren A.J., Young A., and Opdam H.

Abstract

Aim: Case report of renal re-transplantation, reported only once previously. Report: A middle aged recipient received a kidney transplant from a deceased multi-organ donor. After initially doing well, the patient suffered cardiac arrest several days post-operatively and sustained hypoxic brain injury and was declared brain dead. Following the family's consent, the allograft kidney was retrieved and re-transplanted into a man with end-stage renal failure secondary to reflux nephropathy. The lungs were used in a separate recipient but the liver was not transplanted due to suspicion of fatty changes based on macroscopic appearance. Histological analysis of the liver more than 24 hours after transplantation of the other organs revealed coagulative parenchymal necrosis with nuclear inclusions and moderate parenchymal cholestasis, suggestive of herpes viral hepatitis. Examination of the renal implantation biopsy showed histiocytes with enlarged nuclei containing viral inclusions in the capsular fibrous tissue, with positive immunostaining for herpes simplex virus (HSV). Valaciclovir was started immediately after obtaining histological evidence of donor HSV infection and this was subsequently converted to intravenous ganciclovir. Our recipient had pre-formed IgG antibodies to HSV-1 and HSV-2, and was IgM negative pretransplant. HSV viraemia was detected day 5 post-transplant with a viral load of 7688 copies/mL by polymerase chain reaction (PCR) assay. He completed a 30-day course of intravenous ganciclovir before switching to valganciclovir as standard cytomegalovirus prophylaxis. The HSV PCR became undetectable on day 7 of IV ganciclovir and has remained undetectable. The patient remains well with an estimated glomerular filtration rate of 61 mL/min/1.73 m2 and further investigation of the apparent viral transmission is underway. Conclusion(s): We report good short term results of renal re-transplantation and HSV transmission by transplantation.

Published

2014

37. Outflow tract ablation using a conditionally cytotoxic feline immunodeficiency viral vector.

Author

Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep S, Tseng, Harry, Kim, James D, Schuman, Joel S, Weinreb, Robert N, Loewen, Nils A, Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep S, Tseng, Harry, Kim, James D, Schuman, Joel S, Weinreb, Robert N, and Loewen, Nils A

Abstract

PurposeTo create an in vivo model of vector-mediated trabecular meshwork (TM) ablation and replacement.MethodsWe generated a conditionally cytotoxic, trackable vector, HSVtkiG, that expressed herpes simplex virus 1 thymidine kinase (HSVtk) and enhanced green fluorescent protein (eGFP). We optimized HSVtkiG ablation in vitro with ganciclovir (GCV) in comparison to eGFP control vector GINSIN and investigated the mechanism. Right eyes of 24 rats were then injected intracamerally with either HSVtkiG or GINSIN, before intraperitoneal GCV was administered 1 week later. Intraocular pressure, central corneal thickness (CCT), and slit-lamp exams were assessed for 8 weeks. Transduction and ablation were followed by gonioscopic visualization of eGFP. Histology was obtained with TM cell counts and immunohistochemistry markers of inflammation.ResultsTransduction and ablation parameters were established in vitro. Apoptosis was the cause of cell death. In vivo, transduction was seen gonioscopically to be targeted to the TM, followed by disappearance of eGFP marker fluorescence in HSVtkiG-transduced cells after injection of GCV. Ablation resulted in an IOP decrease of 25% in HSVtkiG-injected eyes 2 days after GCV but not in GINSIN or noninjected control eyes (P < 0.05). Trabecular meshwork cellularity was decreased at the time of lowest IOP and recovered thereafter, while CCT remained unchanged. Inflammation was absent.ConclusionsA vector-based system for inducible ablation of cells of the outflow tract was developed. Trabecular meshwork ablation lowered IOP, and recovery of cellularity and IOP followed. This model may be useful to study pressure regulation by the TM, its stem cells, and migration patterns.

Published

2014

38. Outflow tract ablation using a conditionally cytotoxic feline immunodeficiency viral vector.

Author

Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep, Tseng, Harry, Kim, James, Schuman, Joel, Loewen, Nils, Weinreb, Robert, Zhang, Ze, Zhang, Ze, Dhaliwal, Amardeep, Tseng, Harry, Kim, James, Schuman, Joel, Loewen, Nils, and Weinreb, Robert

Abstract

PURPOSE: To create an in vivo model of vector-mediated trabecular meshwork (TM) ablation and replacement. METHODS: We generated a conditionally cytotoxic, trackable vector, HSVtkiG, that expressed herpes simplex virus 1 thymidine kinase (HSVtk) and enhanced green fluorescent protein (eGFP). We optimized HSVtkiG ablation in vitro with ganciclovir (GCV) in comparison to eGFP control vector GINSIN and investigated the mechanism. Right eyes of 24 rats were then injected intracamerally with either HSVtkiG or GINSIN, before intraperitoneal GCV was administered 1 week later. Intraocular pressure, central corneal thickness (CCT), and slit-lamp exams were assessed for 8 weeks. Transduction and ablation were followed by gonioscopic visualization of eGFP. Histology was obtained with TM cell counts and immunohistochemistry markers of inflammation. RESULTS: Transduction and ablation parameters were established in vitro. Apoptosis was the cause of cell death. In vivo, transduction was seen gonioscopically to be targeted to the TM, followed by disappearance of eGFP marker fluorescence in HSVtkiG-transduced cells after injection of GCV. Ablation resulted in an IOP decrease of 25% in HSVtkiG-injected eyes 2 days after GCV but not in GINSIN or noninjected control eyes (P < 0.05). Trabecular meshwork cellularity was decreased at the time of lowest IOP and recovered thereafter, while CCT remained unchanged. Inflammation was absent. CONCLUSIONS: A vector-based system for inducible ablation of cells of the outflow tract was developed. Trabecular meshwork ablation lowered IOP, and recovery of cellularity and IOP followed. This model may be useful to study pressure regulation by the TM, its stem cells, and migration patterns.

Published

2014

39. Severe acute colitis and CMV-cause or effect in a tertiary hospital population.

Author

Moore G., Goldberg R., Shelton E., Marsh P., Moore G., Goldberg R., Shelton E., and Marsh P.

Abstract

Background: Colonic cytomegalovirus (CMV) reactivation is increased in severe acute colitis (ASC) patients, and has variably been associated with use of systemic corticosteroids, azathioprine and steroid-refractory disease. The diagnosis of CMV in ASC remains a challenge, however prompt recognition of CMV reactivation in important, because it is associated with increased morbidity and mortality and requires antiviral therapy. We sought to assess the frequency of CMV in our ASC patients and their outcomes. Method(s): Patients admitted with a diagnosis of Inflammatory Bowel Disease (IBD) between Jan 2011 and April 2013 and had tissue biopsies were obtained retrospectively from a pathology database and their records reviewed. Patients with Crohn's Disease (CD), Ulcerative Colitis (UC) and IBD - unspecified (IBD-U) were included. Data was analysed using Mann Whitney and Chi squared testing. Result(s): There were a total of 68 patients with 104 episodes. Mean age was 44 (+/-19) years, 33 (49% were female), and the diagnoses at the time were UC in 34 (51%), CD in 22 (33%) and IBD-U in 11 (16%). Prior to admission, 58 (56%) received prednisolone at a mean dose of 26 mg (+/-15) and 58 (56%) were on a thiopurine, and 5 (5%) were on methotrexate. Rescue therapy was given in 21 (20%) patients with 20 receiving infliximab and 1 cyclosporine. Colectomy was performed within 30 days in 9 (13%) of patients. The mean length of stay was 13 days. CMV inclusion bodies were found in 7 (6%) of cases, immunohistochemistry was performed in 40 (38%) of cases, it was positive in 3 (3%) cases - all positive IHC cases had inclusion bodies found. CMV tissue PCR was performed in 2 cases and positive in 1. CMV serologies was tested in 21 (20%) cases and of these 5 (9%) were IgM positive. CMV PCR was performed in 19 (18%) of cases, and was positive in 8 (7%) of cases. Eight (16%) patients received CMV antiviral treatment (gancyclovir or valgancyclovir), 7 (88%) of whom had UC or IBD-U and 1 had CD

Published

2013

40. Severe acute colitis and CMV-cause or effect in a tertiary hospital population.

Author

Moore G., Goldberg R., Shelton E., Marsh P., Moore G., Goldberg R., Shelton E., and Marsh P.

Abstract

Background: Colonic cytomegalovirus (CMV) reactivation is increased in severe acute colitis (ASC) patients, and has variably been associated with use of systemic corticosteroids, azathioprine and steroid-refractory disease. The diagnosis of CMV in ASC remains a challenge, however prompt recognition of CMV reactivation in important, because it is associated with increased morbidity and mortality and requires antiviral therapy. We sought to assess the frequency of CMV in our ASC patients and their outcomes. Method(s): Patients admitted with a diagnosis of Inflammatory Bowel Disease (IBD) between Jan 2011 and April 2013 and had tissue biopsies were obtained retrospectively from a pathology database and their records reviewed. Patients with Crohn's Disease (CD), Ulcerative Colitis (UC) and IBD - unspecified (IBD-U) were included. Data was analysed using Mann Whitney and Chi squared testing. Result(s): There were a total of 68 patients with 104 episodes. Mean age was 44 (+/-19) years, 33 (49% were female), and the diagnoses at the time were UC in 34 (51%), CD in 22 (33%) and IBD-U in 11 (16%). Prior to admission, 58 (56%) received prednisolone at a mean dose of 26 mg (+/-15) and 58 (56%) were on a thiopurine, and 5 (5%) were on methotrexate. Rescue therapy was given in 21 (20%) patients with 20 receiving infliximab and 1 cyclosporine. Colectomy was performed within 30 days in 9 (13%) of patients. The mean length of stay was 13 days. CMV inclusion bodies were found in 7 (6%) of cases, immunohistochemistry was performed in 40 (38%) of cases, it was positive in 3 (3%) cases - all positive IHC cases had inclusion bodies found. CMV tissue PCR was performed in 2 cases and positive in 1. CMV serologies was tested in 21 (20%) cases and of these 5 (9%) were IgM positive. CMV PCR was performed in 19 (18%) of cases, and was positive in 8 (7%) of cases. Eight (16%) patients received CMV antiviral treatment (gancyclovir or valgancyclovir), 7 (88%) of whom had UC or IBD-U and 1 had CD

Published

2013

41. A novel murine model to deplete hepatic stellate cells uncovers their role in amplifying liver damage in mice.

Author

Puche, Juan E, Puche, Juan E, Lee, Youngmin A, Jiao, Jingjing, Aloman, Costica, Fiel, Maria I, Muñoz, Ursula, Kraus, Thomas, Lee, Tingfang, Yee, Hal F, Friedman, Scott L, Puche, Juan E, Puche, Juan E, Lee, Youngmin A, Jiao, Jingjing, Aloman, Costica, Fiel, Maria I, Muñoz, Ursula, Kraus, Thomas, Lee, Tingfang, Yee, Hal F, and Friedman, Scott L

Abstract

UnlabelledWe have developed a novel model for depleting mouse hepatic stellate cells (HSCs) that has allowed us to clarify their contributions to hepatic injury and fibrosis. Transgenic (Tg) mice expressing the herpes simplex virus thymidine kinase gene (HSV-Tk) driven by the mouse GFAP promoter were used to render proliferating HSCs susceptible to killing in response to ganciclovir (GCV). Effects of GCV were explored in primary HSCs and in vivo. Panlobular damage was provoked to maximize HSC depletion by combining CCl(4) (centrilobular injury) with allyl alcohol (AA) (periportal injury), as well as in a bile duct ligation (BDL) model. Cell depletion in situ was quantified using dual immunofluorescence (IF) for desmin and GFAP. In primary HSCs isolated from both untreated wild-type (WT) and Tg mice, GCV induced cell death in ≈ 50% of HSCs from Tg, but not WT, mice. In TG mice treated with CCl(4) +AA+GCV, there was a significant decrease in GFAP and desmin-positive cells, compared to WT mice (≈ 65% reduction; P < 0.01), which was accompanied by a decrease in the expression of HSC-activation markers (alpha smooth muscle actin, beta platelet-derived growth factor receptor, and collagen I). Similar results were observed after BDL. Associated with HSC depletion in both fibrosis models, there was marked attenuation of fibrosis and liver injury, as indicated by Sirius Red/Fast Green, hematoxylin and eosin quantification, and serum alanine/aspartate aminotransferase. Hepatic expression of interleukin-10 and interferon-gamma was increased after HSC depletion. No toxicity of GCV in either WT or Tg mice accounted for the differences in injury.ConclusionActivated HSCs significantly amplify the response to liver injury, further expanding this cell type's repertoire in orchestrating hepatic injury and repair.

Published

2013

42. Thymidine kinase-mediated shut down of bone morphogenetic protein-4 expression allows regulated bone production

Author

Lombardo, Barbara, Rocco, Teresa, Esposito, Maria T, Cantilena, Bruno, Gargiulo, Sara, Greco, Adelaide, Montanaro, Donatella, Brunetti, Arturo, Pastore, Lucio, Lombardo, Barbara, Rocco, Teresa, Esposito, Maria T, Cantilena, Bruno, Gargiulo, Sara, Greco, Adelaide, Montanaro, Donatella, Brunetti, Arturo, and Pastore, Lucio

Abstract

Bone morphogenetic Proteins (BMPs) are growth factors also involved in ossification and chondrogenesis that have generated interest for their efficiency in inducing bone neo-synthesis. BMPs expression in engineered cells has been successful in stimulating osteoblastic differentiation and ectopic and orthotopic bone formation in vivo. We have previously shown that an adenoviral vector expressing bone morphogenetic protein type-4 (BMP-4) is able to efficiently drive bone formation in a rabbit model of discontinuous bone lesions. However, unregulated secretion of BMPs has also been implicated in bone overproduction and exostosis. We have constructed a replication-defective first generation adenoviral (FG-Ad) vector containing a cassette for the expression of BMP-4 associated with the Herpes Simplex virus thymidine kinase (TK) gene (FG-B4TK) in order to shut down BMP-4 expression and, therefore, regulate bone production. TK expression does not interfere with BMP-4 ability to induce ectopic bone formation in athymic nude mice. Administration of ganciclovir blocks ectopic bone production in quadriceps muscle transduced with the FG-B4TK with no effect on the contralateral muscle transduced with a vector expressing only BMP-4. Histological findings confirmed the pro-apoptotic activity of TK and the reduction of mineralized areas in the quadriceps transduced with FG-B4TK in mice treated with ganciclovir. We have generated a system to block BMP-4 secretion by inducing apoptosis in transduced cells therefore blocking unwanted bone formation. This system is an additional tool to generate regulated amount of bone in discontinuous bone lesions and can be easily coupled with biomaterials capable of recruiting cells and generating a local bioreactor.

Published

2013

43. The time course of development and impact from viral resistance against ganciclovir in cytomegalovirus infection

Author

Cunha-Bang, C da, Kirkby, N, Sønderholm, M, Sørensen, S S, Sengeløv, H, Iversen, M, Rasmussen, A, Gustafsson, F, Frederiksen, C M, Kjaer, J, Lepri, A Cozzi, Lundgren, J D, Cunha-Bang, C da, Kirkby, N, Sønderholm, M, Sørensen, S S, Sengeløv, H, Iversen, M, Rasmussen, A, Gustafsson, F, Frederiksen, C M, Kjaer, J, Lepri, A Cozzi, and Lundgren, J D

Abstract

(Val)ganciclovir is used to treat cytomegalovirus (CMV) infection following solid organ (SOT) or hematopoietic stem cell (HSCT) transplantation. Treatment failures occur, but the contribution from 39 known ganciclovir-related mutations (GRMs) in the CMV-UL97 gene remains controversial. We propose a categorization of these GRMs potentially useful when interpreting sequence analyses in clinical settings. The UL97 gene was sequenced from first/recurrent CMV infections among consecutive SOT or HSCT recipients during 2004-2009. GRMs were categorized as: Signature GRM (sGRM) if in vitro ganciclovir IC(50) ratio for mutated versus wild-type virus >2 (n = 24); polymorphic GRM (pGRM) if ratio

Published

2013

44. The time course of development and impact from viral resistance against ganciclovir in cytomegalovirus infection

Author

Cunha-Bang, C da, Kirkby, N, Sønderholm, M, Sørensen, S S, Sengeløv, H, Iversen, M, Rasmussen, A, Gustafsson, F, Frederiksen, C M, Kjaer, J, Lepri, A Cozzi, Lundgren, J D, Cunha-Bang, C da, Kirkby, N, Sønderholm, M, Sørensen, S S, Sengeløv, H, Iversen, M, Rasmussen, A, Gustafsson, F, Frederiksen, C M, Kjaer, J, Lepri, A Cozzi, and Lundgren, J D

Abstract

(Val)ganciclovir is used to treat cytomegalovirus (CMV) infection following solid organ (SOT) or hematopoietic stem cell (HSCT) transplantation. Treatment failures occur, but the contribution from 39 known ganciclovir-related mutations (GRMs) in the CMV-UL97 gene remains controversial. We propose a categorization of these GRMs potentially useful when interpreting sequence analyses in clinical settings. The UL97 gene was sequenced from first/recurrent CMV infections among consecutive SOT or HSCT recipients during 2004-2009. GRMs were categorized as: Signature GRM (sGRM) if in vitro ganciclovir IC(50) ratio for mutated versus wild-type virus >2 (n = 24); polymorphic GRM (pGRM) if ratio

Published

2013

45. Cytomegalovirus disease and infection in lung transplant recipients in the setting of planned indefinite valganciclovir prophylaxis.

Author

Wiita, AP, Wiita, AP, Roubinian, N, Khan, Y, Chin-Hong, PV, Singer, JP, Golden, JA, Miller, S, Wiita, AP, Wiita, AP, Roubinian, N, Khan, Y, Chin-Hong, PV, Singer, JP, Golden, JA, and Miller, S

Abstract

BackgroundThe optimal method of both predicting and preventing cytomegalovirus (CMV) disease in lung transplant recipients remains unclear. In particular, the most appropriate duration of CMV prophylaxis post transplant is unresolved. We report herein our experience with a planned indefinite regimen of valganciclovir prophylaxis and monitoring of quantitative CMV load in bronchoalveolar lavage (BAL) fluid.MethodsWe performed a single-center observational study with both prospective and retrospective components. The included patients (n = 128) received a planned regimen of indefinite valganciclovir prophylaxis post transplant, regardless of donor (D)/recipient (R) CMV serostatus. Real-time polymerase chain reaction assay for detection of CMV in BAL was prospectively performed over a 1-year period. Clinical data were reviewed retrospectively; median follow-up was 24.8 months (range 1-93 months).ResultsSixty-five patients (50.6%) discontinued valganciclovir prophylaxis, either temporarily or permanently, with a primary cause of mild leukopenia. Six cases of CMV disease were identified (4.7%), with no significant difference between those who were on continuous prophylaxis or not (4.6% vs. 4.9%; P = non-significant [ns]). However, those who discontinued prophylaxis showed an increased incidence of laboratory-detected CMV infection (40.7% vs. 12.7%; P = 0.001). High-risk D+/R- patients did not demonstrate a significantly increased incidence of CMV disease (8.1% vs. 3.3% other serotypes; P = ns). Three patients (2.3%) developed valganciclovir-resistant CMV disease. Molecular detection of CMV in BAL fluid was significantly more sensitive than shell vial culture. However, BAL CMV viral load was not predictive of subsequent disease development.ConclusionsExtended valganciclovir prophylaxis for all lung transplant recipients led to a low incidence of CMV disease and resistance. In such low-incidence populations, routine quantitation of CMV in BAL did not confer significant cli

Published

2012

46. Active retinitis in an infant with postnatally acquired cytomegalovirus infection.

Author

Bambino Gesù Children’s Hospital – (Italy) Rome - Department of Medical and Surgical Neonatology, Piersigilli, Fiammetta, Catena, Gino, De Gasperis, Marco Rossi, Lozzi, Simona, Auriti, Cinzia, Bambino Gesù Children’s Hospital – (Italy) Rome - Department of Medical and Surgical Neonatology, Piersigilli, Fiammetta, Catena, Gino, De Gasperis, Marco Rossi, Lozzi, Simona, and Auriti, Cinzia

Abstract

Congenital cytomegalovirus (CMV) is frequently associated with active retinitis. In contrast, in the immunocompetent neonate with postnatally acquired CMV infection retinitis is rarely present and usually does not progress. We describe the case of an infant with postnatal CMV infection and active retinitis diagnosed at 20 days of life. Owing to the rapid progression of the retinitis, therapy with intravenous ganciclovir was performed, with prompt regression of the retinitis. Therapy was then continued with oral valganciclovir for one further week. Although very unusual, CMV retinitis has to be taken into consideration in neonates with early postnatally acquired CMV infection, as an early diagnosis and treatment may be crucial to avoid visual impairment.

Published

2012

47. Cytomegalovirus disease and infection in lung transplant recipients in the setting of planned indefinite valganciclovir prophylaxis.

Author

Wiita, AP, Wiita, AP, Roubinian, N, Khan, Y, Chin-Hong, PV, Singer, JP, Golden, JA, Miller, S, Wiita, AP, Wiita, AP, Roubinian, N, Khan, Y, Chin-Hong, PV, Singer, JP, Golden, JA, and Miller, S

Abstract

BackgroundThe optimal method of both predicting and preventing cytomegalovirus (CMV) disease in lung transplant recipients remains unclear. In particular, the most appropriate duration of CMV prophylaxis post transplant is unresolved. We report herein our experience with a planned indefinite regimen of valganciclovir prophylaxis and monitoring of quantitative CMV load in bronchoalveolar lavage (BAL) fluid.MethodsWe performed a single-center observational study with both prospective and retrospective components. The included patients (n = 128) received a planned regimen of indefinite valganciclovir prophylaxis post transplant, regardless of donor (D)/recipient (R) CMV serostatus. Real-time polymerase chain reaction assay for detection of CMV in BAL was prospectively performed over a 1-year period. Clinical data were reviewed retrospectively; median follow-up was 24.8 months (range 1-93 months).ResultsSixty-five patients (50.6%) discontinued valganciclovir prophylaxis, either temporarily or permanently, with a primary cause of mild leukopenia. Six cases of CMV disease were identified (4.7%), with no significant difference between those who were on continuous prophylaxis or not (4.6% vs. 4.9%; P = non-significant [ns]). However, those who discontinued prophylaxis showed an increased incidence of laboratory-detected CMV infection (40.7% vs. 12.7%; P = 0.001). High-risk D+/R- patients did not demonstrate a significantly increased incidence of CMV disease (8.1% vs. 3.3% other serotypes; P = ns). Three patients (2.3%) developed valganciclovir-resistant CMV disease. Molecular detection of CMV in BAL fluid was significantly more sensitive than shell vial culture. However, BAL CMV viral load was not predictive of subsequent disease development.ConclusionsExtended valganciclovir prophylaxis for all lung transplant recipients led to a low incidence of CMV disease and resistance. In such low-incidence populations, routine quantitation of CMV in BAL did not confer significant cli

Published

2012

48. Effect and safety of granulocyte-monocyte adsorption apheresis for patients with ulcerative colitis positive for cytomegalovirus in comparison with immunosuppressants.

Author

10588875, 60362498, 30402910, 90737884, 30188487, Yoshino, Takuya, Nakase, Hiroshi, Matsuura, Minoru, Matsumura, Kayoko, Honzawa, Yusuke, Fukuchi, Takumi, Watanabe, Kenji, Murano, Mitsuyuki, Tsujikawa, Tomoyuki, Fukunaga, Ken, Matsumoto, Takayuki, Chiba, Tsutomu, 10588875, 60362498, 30402910, 90737884, 30188487, Yoshino, Takuya, Nakase, Hiroshi, Matsuura, Minoru, Matsumura, Kayoko, Honzawa, Yusuke, Fukuchi, Takumi, Watanabe, Kenji, Murano, Mitsuyuki, Tsujikawa, Tomoyuki, Fukunaga, Ken, Matsumoto, Takayuki, and Chiba, Tsutomu

Abstract

Background: Cytomegalovirus (CMV) infection exacerbates ulcerative colitis (UC) refractory to immunosuppressive therapies (IMT). However, the underlying UC remained active in some UC patients, despite the fact that CMV-DNA in colonic mucosa became negative after antiviral therapy. Therefore, new therapeutic strategies for UC patients concomitant with CMV infection in mucosa are required. Aims: The aim of this study was to evaluate the effect and safety of granulocyte-monocyte adsorption apheresis (GMA) in UC patients positive for CMV infection after antiviral therapy. Methods: From October 2003 to December 2008, 64 patients with UC refractory to IMT, including steroids and immunomodulators, were enrolled in this retrospective, observational, multicenter study, which was reviewed and approved by the Institutional Review Board of Kyoto University. CMV infection was investigated by 3 methods (histologic examination, CMV antigenemia, and polymerase chain reaction). We investigated the clinical outcomes of GMA and IMT after 2 weeks of treatment with ganciclovir. Results: Thirty-one (48.4%) of 64 patients with UC refractory to IMT were positive for CMV. Of the 31 patients, 4 (12.9%) underwent colectomy. Twenty-seven patients (87.1%) underwent antiviral therapy. Of those 27 patients, 7 achieved remission following antiviral therapy alone. Of the remaining 20 patients who did not achieve remission despite the disappearance of CMV-DNA, 11 and 9 patients were treated with additional GMA (GMA group) and IMT (IMT group), respectively. Of 11 patients (GMA group), 9 achieved remission and 2 underwent colectomy. Out of the remaining 9 patients (IMT group), 4 achieved remission and 5 underwent colectomy. CMV-DNA was not detected in 11 patients after GMA, but it was detected again in all 5 patients of the IMT group who underwent colectomy. The total colectomy rate in UC patients positive for CMV was 35.5% (11/31). In addition, colectomy-free survival in the CMV relapse (+) group was

Published

2011

49. Regarding: Humar et al. The efficacy and safety of 200 days valganciclovir cytomegalovirus prophylaxis in high-risk kidney transplant recipients. Am J Transplant 2010;10:1228–1237

Author

da Cunha-Bang, C, Iversen, M, Mortensen, S A, Rasmussen, A, Sengeløv, H, Sørensen, S S, Lundgren, J, da Cunha-Bang, C, Iversen, M, Mortensen, S A, Rasmussen, A, Sengeløv, H, Sørensen, S S, and Lundgren, J

Published

2011

50. Regarding: Humar et al. The efficacy and safety of 200 days valganciclovir cytomegalovirus prophylaxis in high-risk kidney transplant recipients. Am J Transplant 2010;10:1228–1237

Author

da Cunha-Bang, C, Iversen, M, Mortensen, S A, Rasmussen, A, Sengeløv, H, Sørensen, S S, Lundgren, J, da Cunha-Bang, C, Iversen, M, Mortensen, S A, Rasmussen, A, Sengeløv, H, Sørensen, S S, and Lundgren, J

Published

2011