Your search keyword '"David J. Lockhart"' showing total 124 results

1. Oral Migalastat HCl Leads to Greater Systemic Exposure and Tissue Levels of Active α-Galactosidase A in Fabry Patients when Co-Administered with Infused Agalsidase.

Author

David G Warnock, Daniel G Bichet, Myrl Holida, Ozlem Goker-Alpan, Kathy Nicholls, Mark Thomas, Francois Eyskens, Suma Shankar, Mathews Adera, Sheela Sitaraman, Richie Khanna, John J Flanagan, Brandon A Wustman, Jay Barth, Carrolee Barlow, Kenneth J Valenzano, David J Lockhart, Pol Boudes, and Franklin K Johnson

Subjects

Medicine, Science

Abstract

Migalastat HCl (AT1001, 1-Deoxygalactonojirimycin) is an investigational pharmacological chaperone for the treatment of α-galactosidase A (α-Gal A) deficiency, which leads to Fabry disease, an X-linked, lysosomal storage disorder. The currently approved, biologics-based therapy for Fabry disease is enzyme replacement therapy (ERT) with either agalsidase alfa (Replagal) or agalsidase beta (Fabrazyme). Based on preclinical data, migalastat HCl in combination with agalsidase is expected to result in the pharmacokinetic (PK) enhancement of agalsidase in plasma by increasing the systemic exposure of active agalsidase, thereby leading to increased cellular levels in disease-relevant tissues. This Phase 2a study design consisted of an open-label, fixed-treatment sequence that evaluated the effects of single oral doses of 150 mg or 450 mg migalastat HCl on the PK and tissue levels of intravenously infused agalsidase (0.2, 0.5, or 1.0 mg/kg) in male Fabry patients. As expected, intravenous administration of agalsidase alone resulted in increased α-Gal A activity in plasma, skin, and peripheral blood mononuclear cells (PBMCs) compared to baseline. Following co-administration of migalastat HCl and agalsidase, α-Gal A activity in plasma was further significantly increased 1.2- to 5.1-fold compared to agalsidase administration alone, in 22 of 23 patients (95.6%). Importantly, similar increases in skin and PBMC α-Gal A activity were seen following co-administration of migalastat HCl and agalsidase. The effects were not related to the administered migalastat HCl dose, as the 150 mg dose of migalastat HCl increased α-Gal A activity to the same extent as the 450 mg dose. Conversely, agalsidase had no effect on the plasma PK of migalastat. No migalastat HCl-related adverse events or drug-related tolerability issues were identified.ClinicalTrials.gov NCT01196871.

Published

2015

2. The pharmacological chaperone AT2220 increases the specific activity and lysosomal delivery of mutant acid alpha-glucosidase, and promotes glycogen reduction in a transgenic mouse model of Pompe disease.

Author

Richie Khanna, Allan C Powe, Yi Lun, Rebecca Soska, Jessie Feng, Rohini Dhulipala, Michelle Frascella, Anadina Garcia, Lee J Pellegrino, Su Xu, Nastry Brignol, Matthew J Toth, Hung V Do, David J Lockhart, Brandon A Wustman, and Kenneth J Valenzano

Subjects

Medicine, Science

Abstract

Pompe disease is an inherited lysosomal storage disorder that results from a deficiency in acid α-glucosidase (GAA) activity due to mutations in the GAA gene. Pompe disease is characterized by accumulation of lysosomal glycogen primarily in heart and skeletal muscles, which leads to progressive muscle weakness. We have shown previously that the small molecule pharmacological chaperone AT2220 (1-deoxynojirimycin hydrochloride, duvoglustat hydrochloride) binds and stabilizes wild-type as well as multiple mutant forms of GAA, and can lead to higher cellular levels of GAA. In this study, we examined the effect of AT2220 on mutant GAA, in vitro and in vivo, with a primary focus on the endoplasmic reticulum (ER)-retained P545L mutant form of human GAA (P545L GAA). AT2220 increased the specific activity of P545L GAA toward both natural (glycogen) and artificial substrates in vitro. Incubation with AT2220 also increased the ER export, lysosomal delivery, proteolytic processing, and stability of P545L GAA. In a new transgenic mouse model of Pompe disease that expresses human P545L on a Gaa knockout background (Tg/KO) and is characterized by reduced GAA activity and elevated glycogen levels in disease-relevant tissues, daily oral administration of AT2220 for 4 weeks resulted in significant and dose-dependent increases in mature lysosomal GAA isoforms and GAA activity in heart and skeletal muscles. Importantly, oral administration of AT2220 also resulted in significant glycogen reduction in disease-relevant tissues. Compared to daily administration, less-frequent AT2220 administration, including repeated cycles of 4 or 5 days with AT2220 followed by 3 or 2 days without drug, respectively, resulted in even greater glycogen reductions. Collectively, these data indicate that AT2220 increases the specific activity, trafficking, and lysosomal stability of P545L GAA, leads to increased levels of mature GAA in lysosomes, and promotes glycogen reduction in situ. As such, AT2220 may warrant further evaluation as a treatment for Pompe disease.

Published

2014

3. Migalastat HCl reduces globotriaosylsphingosine (lyso-Gb3) in Fabry transgenic mice and in the plasma of Fabry patients.

Author

Brandy Young-Gqamana, Nastry Brignol, Hui-Hwa Chang, Richie Khanna, Rebecca Soska, Maria Fuller, Sheela A Sitaraman, Dominique P Germain, Roberto Giugliani, Derralynn A Hughes, Atul Mehta, Kathy Nicholls, Pol Boudes, David J Lockhart, Kenneth J Valenzano, and Elfrida R Benjamin

Subjects

Medicine, Science

Abstract

Fabry disease (FD) results from mutations in the gene (GLA) that encodes the lysosomal enzyme α-galactosidase A (α-Gal A), and involves pathological accumulation of globotriaosylceramide (GL-3) and globotriaosylsphingosine (lyso-Gb3). Migalastat hydrochloride (GR181413A) is a pharmacological chaperone that selectively binds, stabilizes, and increases cellular levels of α-Gal A. Oral administration of migalastat HCl reduces tissue GL-3 in Fabry transgenic mice, and in urine and kidneys of some FD patients. A liquid chromatography-tandem mass spectrometry method was developed to measure lyso-Gb3 in mouse tissues and human plasma. Oral administration of migalastat HCl to transgenic mice reduced elevated lyso-Gb3 levels up to 64%, 59%, and 81% in kidney, heart, and skin, respectively, generally equal to or greater than observed for GL-3. Furthermore, baseline plasma lyso-Gb3 levels were markedly elevated in six male FD patients enrolled in Phase 2 studies. Oral administration of migalastat HCl (150 mg QOD) reduced urine GL-3 and plasma lyso-Gb3 in three subjects (range: 15% to 46% within 48 weeks of treatment). In contrast, three showed no reductions in either substrate. These results suggest that measurement of tissue and/or plasma lyso-Gb3 is feasible and may be warranted in future studies of migalastat HCl or other new potential therapies for FD.

Published

2013

4. The pharmacological chaperone AT2220 increases recombinant human acid α-glucosidase uptake and glycogen reduction in a mouse model of Pompe disease.

Author

Richie Khanna, John J Flanagan, Jessie Feng, Rebecca Soska, Michelle Frascella, Lee J Pellegrino, Yi Lun, Darlene Guillen, David J Lockhart, and Kenneth J Valenzano

Subjects

Medicine, Science

Abstract

Pompe disease is an inherited lysosomal storage disease that results from a deficiency in the enzyme acid α-glucosidase (GAA), and is characterized by progressive accumulation of lysosomal glycogen primarily in heart and skeletal muscles. Recombinant human GAA (rhGAA) is the only approved enzyme replacement therapy (ERT) available for the treatment of Pompe disease. Although rhGAA has been shown to slow disease progression and improve some of the pathophysiogical manifestations, the infused enzyme tends to be unstable at neutral pH and body temperature, shows low uptake into some key target tissues, and may elicit immune responses that adversely affect tolerability and efficacy. We hypothesized that co-administration of the orally-available, small molecule pharmacological chaperone AT2220 (1-deoxynojirimycin hydrochloride, duvoglustat hydrochloride) may improve the pharmacological properties of rhGAA via binding and stabilization. AT2220 co-incubation prevented rhGAA denaturation and loss of activity in vitro at neutral pH and 37°C in both buffer and blood. In addition, oral pre-administration of AT2220 to rats led to a greater than two-fold increase in the circulating half-life of intravenous rhGAA. Importantly, co-administration of AT2220 and rhGAA to GAA knock-out (KO) mice resulted in significantly greater rhGAA levels in plasma, and greater uptake and glycogen reduction in heart and skeletal muscles, compared to administration of rhGAA alone. Collectively, these preclinical data highlight the potentially beneficial effects of AT2220 on rhGAA in vitro and in vivo. As such, a Phase 2 clinical study has been initiated to investigate the effects of co-administered AT2220 on rhGAA in Pompe patients.

Published

2012

5. The validation of pharmacogenetics for the identification of Fabry patients to be treated with migalastat

Author

Jay A. Barth, Benjamin Bronfin, David J. Lockhart, William R. Wilcox, Robert J. Desnick, Daniel G. Bichet, Dominique P. Germain, Xiaoyang Wu, John Kirk, Raphael Schiffmann, Hadis Williams, Roberto Giugliani, Julie Yu, Sarah Bond, Elfrida R. Benjamin, Kenneth J. Valenzano, Farhana Pruthi, Carrolee Barlow, Derralynn Hughes, Maria Cecilia Della Valle, Evan Katz, and Jeff Castelli

Subjects

Male, 0301 basic medicine, Oncology, medicine.medical_specialty, 1-Deoxynojirimycin, Validation Studies as Topic, Pharmacology, Cell Line, 03 medical and health sciences, Clinical Trials, Phase II as Topic, Predictive Value of Tests, Migalastat, Internal medicine, Leukocytes, medicine, Humans, Original Research Article, Genetics (clinical), Fabry disease, business.industry, personalized medicine, Enzyme replacement therapy, medicine.disease, pharmacological chaperone, HEK293 Cells, 030104 developmental biology, Clinical Trials, Phase III as Topic, alpha-Galactosidase, Mutation, Biological Assay, Female, lysosomal storage disorder, business, Pharmacogenetics, enzyme replacement therapy

Abstract

Purpose: Fabry disease is an X-linked lysosomal storage disorder caused by mutations in the α-galactosidase A gene. Migalastat, a pharmacological chaperone, binds to specific mutant forms of α-galactosidase A to restore lysosomal activity. Methods: A pharmacogenetic assay was used to identify the α-galactosidase A mutant forms amenable to migalastat. Six hundred Fabry disease–causing mutations were expressed in HEK-293 (HEK) cells; increases in α-galactosidase A activity were measured by a good laboratory practice (GLP)-validated assay (GLP HEK/Migalastat Amenability Assay). The predictive value of the assay was assessed based on pharmacodynamic responses to migalastat in phase II and III clinical studies. Results: Comparison of the GLP HEK assay results in in vivo white blood cell α-galactosidase A responses to migalastat in male patients showed high sensitivity, specificity, and positive and negative predictive values (≥0.875). GLP HEK assay results were also predictive of decreases in kidney globotriaosylceramide in males and plasma globotriaosylsphingosine in males and females. The clinical study subset of amenable mutations (n = 51) was representative of all 268 amenable mutations identified by the GLP HEK assay. Conclusion: The GLP HEK assay is a clinically validated method of identifying male and female Fabry patients for treatment with migalastat. Genet Med 19 4, 430–438.

Published

2017

6. Oral pharmacological chaperone migalastat compared with enzyme replacement therapy in Fabry disease: 18-month results from the randomised phase III ATTRACT study

Author

David J. Lockhart, Ana Jovanovic, Toya Ohashi, Elfrida R. Benjamin, Norio Sakai, Raphael Schiffmann, David M. Koeller, Gere Sunder-Plassmann, Dominique P. Germain, Jeffrey P. Castelli, Elizabeth Ludington, Charles Marques Lourenço, Kathleen Nicholls, Mark Thomas, Ozlem Goker-Alpan, Robin H. Lachmann, David Dimmock, Ulla Feldt-Rasmussen, Jay A. Barth, Carrolee Barlow, François Eyskens, Patrick Deegan, Eric Hachulla, Nina Skuban, William R. Wilcox, Daniel G. Bichet, John Kirk, Iacopo Olivotto, Suma P. Shankar, Gerard Vockley, Takashi Hamazaki, Franklin K. Johnson, Derralynn Hughes, Pol Boudes, Christopher Viereck, Ichiei Narita, Khan Nedd, and Julie Yu

Subjects

Male, 0301 basic medicine, Cardiomyopathy, 030204 cardiovascular system & hematology, Medical and Health Sciences, 0302 clinical medicine, Migalastat, Pharmacological chaperone, Genetics (clinical), Genetics & Heredity, Kidney, biology, Enzyme replacement therapy, Middle Aged, Biological Sciences, Treatment Outcome, medicine.anatomical_structure, Administration, Female, lysosomal storage disorder, medicine.drug, Oral, Adult, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, 1-Deoxynojirimycin, Adolescent, Urology, Renal function, lyso-Gb3, 03 medical and health sciences, Genetics, medicine, Humans, Enzyme Replacement Therapy, Aged, Fabry disease, Alpha-galactosidase, business.industry, nutritional and metabolic diseases, medicine.disease, enzyme replacement therapy, Administration, Oral, Fabry Disease, Lysosomes, Molecular Chaperones, alpha-Galactosidase, 030104 developmental biology, biology.protein, Human medicine, business

Abstract

Background Fabry disease is an X-linked lysosomal storage disorder caused by GLA mutations, resulting in α-galactosidase (α-Gal) deficiency and accumulation of lysosomal substrates. Migalastat, an oral pharmacological chaperone being developed as an alternative to intravenous enzyme replacement therapy (ERT), stabilises specific mutant ( amenable ) forms of α-Gal to facilitate normal lysosomal trafficking. Methods The main objective of the 18-month, randomised, active-controlled ATTRACT study was to assess the effects of migalastat on renal function in patients with Fabry disease previously treated with ERT. Effects on heart, disease substrate, patient-reported outcomes (PROs) and safety were also assessed. Results Fifty-seven adults (56% female) receiving ERT (88% had multiorgan disease) were randomised (1.5:1), based on a preliminary cell-based assay of responsiveness to migalastat, to receive 18 months open-label migalastat or remain on ERT. Four patients had non-amenable mutant forms of α-Gal based on the validated cell-based assay conducted after treatment initiation and were excluded from primary efficacy analyses only. Migalastat and ERT had similar effects on renal function. Left ventricular mass index decreased significantly with migalastat treatment (−6.6 g/m 2 (−11.0 to −2.2)); there was no significant change with ERT. Predefined renal, cardiac or cerebrovascular events occurred in 29% and 44% of patients in the migalastat and ERT groups, respectively. Plasma globotriaosylsphingosine remained low and stable following the switch from ERT to migalastat. PROs were comparable between groups. Migalastat was generally safe and well tolerated. Conclusions Migalastat offers promise as a first-in-class oral monotherapy alternative treatment to intravenous ERT for patients with Fabry disease and amenable mutations. Trial registration number: NCT00925301; Pre-results.

Published

2016

7. Coformulation of a Novel Human α-Galactosidase A With the Pharmacological Chaperone AT1001 Leads to Improved Substrate Reduction in Fabry Mice

Author

Kate Chang, Amol Ketkar, Nicola Robertson, Masahito Miyamoto, Kenneth J. Valenzano, Yi Lun, Nastry Brignol, Su Xu, Kazutoshi Mihara, Rebecca Soska, Jessie Feng, Hidehito Yasukawa, Robert Boyd, Michelle Frascella, Carole Shardlow, Rick Hamler, Susie Fowles, Alison Churchill, Richie Khanna, David J. Lockhart, Anadina Garcia, Tohru Hirato, Elfrida R. Benjamin, Adriane Schilling, and Sean Sullivan

Subjects

Cell type, Globotriaosylceramide, Pharmacology, law.invention, Substrate Specificity, chemistry.chemical_compound, Mice, law, Drug Discovery, medicine, Genetics, Animals, Humans, Enzyme Replacement Therapy, Molecular Biology, chemistry.chemical_classification, Enzyme replacement therapy, Fibroblasts, medicine.disease, Fabry disease, In vitro, Pharmacological chaperone, Disease Models, Animal, Drug Combinations, Enzyme, Biochemistry, chemistry, alpha-Galactosidase, Mutation, Recombinant DNA, Fabry Disease, Molecular Medicine, Original Article, Oligopeptides, medicine.drug, Molecular Chaperones

Abstract

Fabry disease is an X-linked lysosomal storage disorder caused by mutations in the gene that encodes α-galactosidase A and is characterized by pathological accumulation of globotriaosylceramide and globotriaosylsphingosine. Earlier, the authors demonstrated that oral coadministration of the pharmacological chaperone AT1001 (migalastat HCl; 1-deoxygalactonojirimycin HCl) prior to intravenous administration of enzyme replacement therapy improved the pharmacological properties of the enzyme. In this study, the authors investigated the effects of coformulating AT1001 with a proprietary recombinant human α-galactosidase A (ATB100) into a single intravenous formulation. AT1001 increased the physical stability and reduced aggregation of ATB100 at neutral pH in vitro, and increased the potency for ATB100-mediated globotriaosylceramide reduction in cultured Fabry fibroblasts. In Fabry mice, AT1001 coformulation increased the total exposure of active enzyme, and increased ATB100 levels in cardiomyocytes, cardiac vascular endothelial cells, renal distal tubular epithelial cells, and glomerular cells, cell types that do not show substantial uptake with enzyme replacement therapy alone. Notably, AT1001 coformulation also leads to greater tissue globotriaosylceramide reduction when compared with ATB100 alone, which was positively correlated with reductions in plasma globotriaosylsphingosine. Collectively, these data indicate that intravenous administration of ATB100 coformulated with AT1001 may provide an improved therapy for Fabry disease and thus warrants further investigation.

Published

2015

8. Duvoglustat HCl Increases Systemic and Tissue Exposure of Active Acid α-Glucosidase in Pompe Patients Co-administered with Alglucosidase α

Author

Sheela Sitaraman, Todd Levine, Carrolee Barlow, Mark Roberts, Barry J. Byrne, Tahseen Mozaffar, Priya S. Kishnani, Pascal Laforêt, Richie Khanna, Jessie Feng, Mark A. Tarnopolsky, David J. Lockhart, Majed Dasouki, Matthews Adera, Ozlem Goker-Alpan, Franklin K. Johnson, Mazen M. Dimachkie, K. Sivakumar, Pol Boudes, Kenneth J. Valenzano, Erika Finanger, Muhammad Ali Pervaiz, K. Guter, Elfrida R. Benjamin, John J. Flanagan, Richard Lazauskas, and Jay A. Barth

Subjects

0301 basic medicine, Adult, Male, 1-Deoxynojirimycin, Administration, Oral, Pharmacology, Drug Administration Schedule, law.invention, 03 medical and health sciences, chemistry.chemical_compound, Pharmacokinetics, law, Drug Discovery, medicine, Genetics, Humans, Enzyme Replacement Therapy, Adverse effect, Infusions, Intravenous, Muscle, Skeletal, Alglucosidase alfa, Molecular Biology, Glycogen, Glycogen Storage Disease Type II, Pompe disease, Drug Synergism, alpha-Glucosidases, Enzyme replacement therapy, Middle Aged, pharmacological chaperone, Pharmacological chaperone, 030104 developmental biology, Treatment Outcome, Biochemistry, chemistry, Tolerability, Recombinant DNA, Molecular Medicine, Drug Therapy, Combination, Female, Original Article, Patient Safety, Lysosomes, pharmacokinetics, medicine.drug

Abstract

Duvoglustat HCl (AT2220, 1-deoxynojirimycin) is an investigational pharmacological chaperone for the treatment of acid α-glucosidase (GAA) deficiency, which leads to the lysosomal storage disorder Pompe disease, which is characterized by progressive accumulation of lysosomal glycogen primarily in heart and skeletal muscles. The current standard of care is enzyme replacement therapy with recombinant human GAA (alglucosidase alfa [AA], Genzyme). Based on preclinical data, oral co-administration of duvoglustat HCl with AA increases exposure of active levels in plasma and skeletal muscles, leading to greater substrate reduction in muscle. This phase 2a study consisted of an open-label, fixed-treatment sequence that evaluated the effect of single oral doses of 50 mg, 100 mg, 250 mg, or 600 mg duvoglustat HCl on the pharmacokinetics and tissue levels of intravenously infused AA (20 mg/kg) in Pompe patients. AA alone resulted in increases in total GAA activity and protein in plasma compared to baseline. Following co-administration with duvoglustat HCl, total GAA activity and protein in plasma were further increased 1.2- to 2.8-fold compared to AA alone in all 25 Pompe patients; importantly, muscle GAA activity was increased for all co-administration treatments from day 3 biopsy specimens. No duvoglustat-related adverse events or drug-related tolerability issues were identified., Pharmacological chaperones stabilize enzyme replacement in circulation, providing increased uptake of properly folded enzyme into tissues. In a phase 2a study, Kishnani et al. demonstrate a 2-fold increase in plasma and increased uptake in muscle of active recombinant human GAA following co-administration with duvoglustat HCl in patients with late onset Pompe disease.

Published

2017

9. A GCase Chaperone Improves Motor Function in a Mouse Model of Synucleinopathy

Author

David J. Lockhart, Sindalana Hean, Lee Pellegrino, Sheila M. Fleming, Melanie B. Watson, Farzad Mortazavi, Franziska Richter, Caitlin K. Mulligan, Brian Ranes, Chunni Zhu, Richie Khanna, John J. Flanagan, Sean W. Clark, Pedrom C. Sioshansi, Krystal De La Rosa, Vincent Lemesre, Brandon Wustman, and Marie-Françoise Chesselet

Subjects

Male, Parkinson's disease, Chaperone, Neurodegenerative, Pharmacology, Mice, chemistry.chemical_compound, Motor behavior, 2.1 Biological and endogenous factors, Pharmacology (medical), Aetiology, Tartrates, Acid-beta-glucosidase, biology, beta-Glucosidase, Dopaminergic, Brain, Parkinson Disease, Pharmacology and Pharmaceutical Sciences, Substantia Nigra, Pharmacological chaperone, Protein Transport, 5.1 Pharmaceuticals, Neurological, alpha-Synuclein, Public Health and Health Services, Original Article, Development of treatments and therapeutic interventions, Imino Pyranoses, medicine.drug, Substantia nigra, Motor Activity, Mouse model, Alpha-synuclein, Protein Aggregates, medicine, Animals, Humans, Synucleinopathies, Neurology & Neurosurgery, Animal, Dopaminergic Neurons, Prevention, Neurosciences, medicine.disease, Brain Disorders, Disease Models, Animal, nervous system, chemistry, Chaperone (protein), Disease Models, biology.protein, Acid-β-glucosidase, Neurology (clinical), Glucocerebrosidase, Neuroscience

Abstract

Mutation of the lysosomal hydrolase acid-β-glucosidase (GCase), which leads to reduced GCase activity, is one of the most frequent genetic risk factors for Parkinson's disease (PD) and promotes α-synuclein accumulation in the brain, a hallmark of PD and other synucleinopathies. Whether targeting GCase pharmacologically is a valid therapeutic strategy for sporadic PD in the absence of GCase mutation is unknown. We have investigated whether increasing the stability, trafficking, and activity of wild-type GCase could be beneficial in synucleinopathies by administering the pharmacological chaperone AT2101 (afegostat-tartrate, isofagomine) to mice that overexpress human wild-type α-synuclein (Thy1-aSyn mice). AT2101 administered orally for 4 months to Thy1-aSyn mice improved motor and nonmotor function, abolished microglial inflammatory response in the substantia nigra, reduced α-synuclein immunoreactivity in nigral dopaminergic neurons, and reduced the number of small α-synuclein aggregates, while increasing the number of large α-synuclein aggregates. These data support the further investigation of pharmacological chaperones that target GCase as a therapeutic approach for sporadic PD and other synucleinopathies, even in the absence of glucocerebrosidase mutations.

Published

2014

10. Treatment of Fabry's Disease with the Pharmacologic Chaperone Migalastat

Author

Joel Charrow, Dominique P. Germain, Maryam Banikazemi, Kathleen Nicholls, Carrolee Barlow, Majed Dasouki, Raphael Schiffmann, Ana Jovanovic, Khan Nedd, Nicola Longo, Suma P. Shankar, Jay A. Barth, Usama A Sharaf El Din, John Kirk, Christopher Viereck, Jeff Castelli, Derralynn Hughes, Charles Marques Lourenço, Ozlem Goker-Alpan, Roberto Giugliani, Ahmad Tuffaha, Claudio Feliciani, Stephen Waldek, Franklin K. Johnson, Elfrida R. Benjamin, C. Ronald Scott, David J. Lockhart, P Giraldo, Julie Yu, Daniel G. Bichet, Drago Bratkovic, Hernan Amartino, Nina Skuban, Seymour Packman, Elizabeth Ludington, Roser Torra, David N. Finegold, Ulla Feldt-Rasmussen, William R. Wilcox, and Fatih Süheyl Ezgü

Subjects

0301 basic medicine, Adult, Diarrhea, Male, medicine.medical_specialty, 1-Deoxynojirimycin, Adolescent, Heart Ventricles, Globotriaosylceramide, Pharmacology, Kidney, Nephropathy, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Double-Blind Method, Internal medicine, Migalastat, medicine, Humans, Aged, Ultrasonography, Alpha-galactosidase, biology, business.industry, Trihexosylceramides, General Medicine, Enzyme replacement therapy, Middle Aged, medicine.disease, Fabry's disease, Fabry disease, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, alpha-Galactosidase, Mutation, biology.protein, Fabry Disease, Female, Hypertrophy, Left Ventricular, business, 030217 neurology & neurosurgery, Glomerular Filtration Rate

Abstract

BACKGROUND Fabry's disease, an X-linked disorder of lysosomal alpha-galactosidase deficiency, leads to substrate accumulation in multiple organs. Migalastat, an oral pharmacologic chaperone, stabilizes specific mutant forms of alpha-galactosidase, increasing enzyme trafficking to lysosomes. METHODS The initial assay of mutant alpha-galactosidase forms that we used to categorize 67 patients with Fabry's disease for randomization to 6 months of double-blind migalastat or placebo (stage 1), followed by open-label migalastat from 6 to 12 months (stage 2) plus an additional year, had certain limitations. Before unblinding, a new, validated assay showed that 50 of the 67 participants had mutant alpha-galactosidase forms suitable for targeting by migalastat. The primary end point was the percentage of patients who had a response (>= 50% reduction in the number of globotriaosylceramide inclusions per kidney interstitial capillary) at 6 months. We assessed safety along with disease substrates and renal, cardiovascular, and patient-reported outcomes. RESULTS The primary end-point analysis, involving patients with mutant alpha-galactosidase forms that were suitable or not suitable for migalastat therapy, did not show a significant treatment effect: 13 of 32 patients (41%) who received migalastat and 9 of 32 patients (28%) who received placebo had a response at 6 months (P = 0.30). Among patients with suitable mutant alpha-galactosidase who received migalastat for up to 24 months, the annualized changes from baseline in the estimated glomerular filtration rate (GFR) and measured GFR were -0.30 +/- 0.66 and -1.51 +/- 1.33 ml per minute per 1.73 m(2) of body-surface area, respectively. The left-ventricular-mass index decreased significantly from baseline (-7.7 g per square meter; 95% confidence interval [CI], -15.4 to -0.01), particularly when left ventricular hypertrophy was present (-18.6 g per square meter; 95% CI, -38.2 to 1.0). The severity of diarrhea, reflux, and indigestion decreased. CONCLUSIONS Among all randomly assigned patients (with mutant alpha-galactosidase forms that were suitable or not suitable for migalastat therapy), the percentage of patients who had a response at 6 months did not differ significantly between the migalastat group and the placebo group. (Funded by Amicus Therapeutics; ClinicalTrials.gov numbers, NCT00925301 [study AT1001-011] and NCT01458119 [study AT1001-041].)

Published

2016

11. Co-administration With the Pharmacological Chaperone AT1001 Increases Recombinant Human α-Galactosidase A Tissue Uptake and Improves Substrate Reduction in Fabry Mice

Author

Yi Lun, John J. Flanagan, Nastry Brignol, Michelle Frascella, David J. Lockhart, Darlene Guillen, Adriane Schilling, Jessie Feng, Kenneth J. Valenzano, Brandy L. Young, Richie Khanna, Elfrida R. Benjamin, Lee Pellegrino, Brian Ranes, Leo B. Dungan, and Rebecca Soska

Subjects

Blotting, Western, Globotriaosylceramide, Fluorescent Antibody Technique, Pharmacology, law.invention, Mice, chemistry.chemical_compound, law, Drug Discovery, medicine, Genetics, Animals, Humans, Enzyme Replacement Therapy, Molecular Biology, Alpha-galactosidase, biology, Trihexosylceramides, Enzyme replacement therapy, medicine.disease, Fabry disease, Molecular biology, Recombinant Proteins, In vitro, Rats, Pharmacological chaperone, chemistry, alpha-Galactosidase, Knockout mouse, biology.protein, Recombinant DNA, Fabry Disease, Molecular Medicine, Original Article, Oligopeptides, medicine.drug

Abstract

Fabry disease is an X-linked lysosomal storage disorder (LSD) caused by mutations in the gene (GLA) that encodes the lysosomal hydrolase α-galactosidase A (α-Gal A), and is characterized by pathological accumulation of the substrate, globotriaosylceramide (GL-3). Regular infusion of recombinant human α-Gal A (rhα-Gal A), termed enzyme replacement therapy (ERT), is the primary treatment for Fabry disease. However, rhα-Gal A has low physical stability, a short circulating half-life, and variable uptake into different disease-relevant tissues. We hypothesized that coadministration of the orally available, small molecule pharmacological chaperone AT1001 (GR181413A, 1-deoxygalactonojirimycin, migalastat hydrochloride) may improve the pharmacological properties of rhα-Gal A via binding and stabilization. AT1001 prevented rhα-Gal A denaturation and activity loss in vitro at neutral pH and 37 °C. Coincubation of Fabry fibroblasts with rhα-Gal A and AT1001 resulted in up to fourfold higher cellular α-Gal A and ~30% greater GL-3 reduction compared to rhα-Gal A alone. Furthermore, coadministration of AT1001 to rats increased the circulating half-life of rhα-Gal A by >2.5-fold, and in GLA knockout mice resulted in up to fivefold higher α-Gal A levels and fourfold greater GL-3 reduction than rhα-Gal A alone. Collectively, these data highlight the potentially beneficial effects of AT1001 on rhα-Gal A, thus warranting clinical investigation.

Published

2012

12. A Pharmacogenetic Approach to Identify Mutant Forms of α-Galactosidase A that Respond to a Pharmacological Chaperone for Fabry Disease

Author

Pol Boudes, Raphael Schiffmann, David J. Lockhart, Elfrida R. Benjamin, Kirsten Mascioli, Kenneth J. Valenzano, Maria Cecilia Della Valle, Evan Katz, Xiaoyang Wu, John J. Flanagan, and Jeffrey P. Castelli

Subjects

Male, 1-Deoxynojirimycin, Protein Conformation, Cell, Mutant, Biology, Peripheral blood mononuclear cell, Migalastat, α-Galactosidase A, Genetics, medicine, Humans, Point Mutation, Genetics (clinical), Alpha-galactosidase, AT1001, HEK 293 cells, medicine.disease, Fabry disease, Molecular biology, pharmacological chaperone, Pharmacological chaperone, Enzyme Activation, medicine.anatomical_structure, HEK293 Cells, Fabry, Gene Expression Regulation, alpha-Galactosidase, biology.protein, Leukocytes, Mononuclear, Fabry Disease, Biological Assay, Mutant Proteins, medicine.drug, Research Article

Abstract

Fabry disease is caused by mutations in the gene (GLA) that encodes α-galactosidase A (α-Gal A). The iminosugar AT1001 (GR181413A, migalastat hydrochloride, 1-deoxygalactonojirimycin) is a pharmacological chaperone that selectively binds and stabilizes α-Gal A, increasing total cellular levels and activity for some mutant forms (defined as “responsive”). In this study, we developed a cell-based assay in cultured HEK-293 cells to identify mutant forms of α-Gal A that are responsive to AT1001. Concentration-dependent increases in α-Gal A activity in response to AT1001 were shown for 49 (60%) of 81 mutant forms. The responses of α-Gal A mutant forms were generally consistent with the responses observed in male Fabry patient-derived lymphoblasts. Importantly, the HEK-293 cell responses of 19 α-Gal A mutant forms to a clinically achievable concentration of AT1001 (10 µM) were generally consistent with observed increases in α-Gal A activity in peripheral blood mononuclear cells from male Fabry patients orally administered AT1001 during Phase 2 clinical studies. This indicates that the cell-based responses can identify mutant forms of α-Gal A that are likely to respond to AT1001 in vivo. Thus, the HEK-293 cell-based assay may be a useful aid in the identification of Fabry patients with AT1001-responsive mutant forms. Hum Mutat 32:1–13, 2011. © 2011 Wiley-Liss, Inc.

Published

2011

13. The pharmacological chaperone isofagomine increases the activity of the Gaucher disease L444P mutant form of β-glucosidase

Author

Hadis Nafar, Brigitte Rigat, Allan C. Powe, Jessie Feng, Yi Lun, Elfrida R. Benjamin, Richie Khanna, Adriane Schilling, David J. Lockhart, Lee Pellegrino, Brian Ranes, Raphael Schiffmann, Kenneth J. Valenzano, Brandon Wustman, Don J. Mahuran, David Palling, and Rebecca Soska

Subjects

chemistry.chemical_classification, Mutation, endocrine system diseases, Mutant, nutritional and metabolic diseases, Endogeny, Cell Biology, Biology, Pharmacology, medicine.disease_cause, Biochemistry, Molecular biology, Glucosylceramidase, Pharmacological chaperone, Dose–response relationship, Enzyme, chemistry, Oral administration, medicine, Molecular Biology, medicine.drug

Abstract

Gaucher disease is caused by mutations in the gene that encodes the lysosomal enzyme acid beta-glucosidase (GCase). We have shown previously that the small molecule pharmacological chaperone isofagomine (IFG) binds and stabilizes N370S GCase, resulting in increased lysosomal trafficking and cellular activity. In this study, we investigated the effect of IFG on L444P GCase. Incubation of Gaucher patient-derived lymphoblastoid cell lines (LCLs) or fibroblasts with IFG led to approximately 3.5- and 1.3-fold increases in L444P GCase activity, respectively, as measured in cell lysates. The effect in fibroblasts was increased approximately 2-fold using glycoprotein-enrichment, GCase-immunocapture, or by incubating cells overnight in IFG-free media prior to assay, methods designed to maximize GCase activity by reducing IFG carryover and inhibition in the enzymatic assay. IFG incubation also increased the lysosomal trafficking and in situ activity of L444P GCase in intact cells, as measured by reduction in endogenous glucosylceramide levels. Importantly, this reduction was seen only following three-day incubation in IFG-free media, underscoring the importance of IFG removal to restore lysosomal GCase activity. In mice expressing murine L444P GCase, oral administration of IFG resulted in significant increases (2- to 5-fold) in GCase activity in disease-relevant tissues, including brain. Additionally, eight-week IFG administration significantly lowered plasma chitin III and IgG levels, and 24-week administration significantly reduced spleen and liver weights. Taken together, these data suggest that IFG can increase the lysosomal activity of L444P GCase in cells and tissues. Moreover, IFG is orally available and distributes into multiple tissues, including brain, and may thus merit therapeutic evaluation for patients with neuronopathic and non-neuronopathic Gaucher disease.

Published

2010

14. The Pharmacological Chaperone 1-Deoxygalactonojirimycin Reduces Tissue Globotriaosylceramide Levels in a Mouse Model of Fabry Disease

Author

Sheela Sitaraman, Jessie Feng, Michelle Frascella, Lee Pellegrino, Rebecca Soska, Nastry Brignol, David J. Lockhart, Brandy Young, Robert J. Desnick, Kenneth J. Valenzano, Elfrida R. Benjamin, Richie Khanna, and Yi Lun

Subjects

1-Deoxynojirimycin, Blotting, Western, Globotriaosylceramide, Mice, Transgenic, Pharmacology, Biology, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Oral administration, Migalastat, Drug Discovery, Genetics, medicine, Animals, Humans, Molecular Biology, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Alpha-galactosidase, Trihexosylceramides, Original Articles, medicine.disease, Immunohistochemistry, Fabry disease, 3. Good health, Mice, Inbred C57BL, Pharmacological chaperone, Disease Models, Animal, chemistry, alpha-Galactosidase, Immunology, biology.protein, Fabry Disease, Molecular Medicine, 030217 neurology & neurosurgery, medicine.drug

Abstract

Fabry disease is an X-linked lysosomal storage disorder caused by a deficiency in alpha-galactosidase A (alpha-Gal A) activity and subsequent accumulation of the substrate globotriaosylceramide (GL-3), which contributes to disease pathology. The pharmacological chaperone (PC) DGJ (1-deoxygalactonojirimycin) binds and stabilizes alpha-Gal A, increasing enzyme levels in cultured cells and in vivo. The ability of DGJ to reduce GL-3 in vivo was investigated using transgenic (Tg) mice that express a mutant form of human alpha-Gal A (R301Q) on a knockout background (Tg/KO), which leads to GL-3 accumulation in disease-relevant tissues. Four-week daily oral administration of DGJ to Tg/KO mice resulted in significant and dose-dependent increases in alpha-Gal A activity, with concomitant GL-3 reduction in skin, heart, kidney, brain, and plasma; 24-week administration resulted in even greater reductions. Compared to daily administration, less frequent DGJ administration, including repeated cycles of 4 days with DGJ followed by 3 days without or every other day with DGJ, resulted in even greater GL-3 reductions that were comparable to those obtained with Fabrazyme. Collectively, these data indicate that oral administration of DGJ increases mutant alpha-Gal A activity and reduces GL-3 in disease-relevant tissues in Tg/KO mice, and thus merits further evaluation as a treatment for Fabry disease.

Published

2010

15. The pharmacological chaperone 1‐deoxygalactonojirimycin increases α‐galactosidase A levels in Fabry patient cell lines

Author

C.W. Pine, Hui-Hwa Chang, Adriane Schilling, Robert J. Desnick, Brandon W. Wustman, Elfrida R. Benjamin, John J. Flanagan, Evan Katz, Xiaoyang Wu, Kenneth J. Valenzano, David J. Lockhart, and L. Agarwal

Subjects

Male, Models, Molecular, medicine.medical_specialty, 1-Deoxynojirimycin, Mutant, Drug Evaluation, Preclinical, Mutation, Missense, Globotriaosylceramide, Biology, Cell Line, chemistry.chemical_compound, Migalastat, Internal medicine, Genetics, medicine, Humans, Missense mutation, Lymphocytes, Genetics (clinical), chemistry.chemical_classification, Glycosphingolipid, Fibroblasts, medicine.disease, Fabry disease, Up-Regulation, Enzyme Activation, Pharmacological chaperone, Enzyme, Endocrinology, chemistry, alpha-Galactosidase, Fabry Disease, Half-Life, Molecular Chaperones, medicine.drug

Abstract

Fabry disease is an X-linked lysosomal storage disorder caused by mutations in the gene encoding alpha-galactosidase A (alpha-Gal A), with consequent accumulation of its major glycosphingolipid substrate, globotriaosylceramide (GL-3). Over 500 Fabry mutations have been reported; approximately 60% are missense. The iminosugar 1-deoxygalactonojirimycin (DGJ, migalastat hydrochloride, AT1001) is a pharmacological chaperone that selectively binds alpha-Gal A, increasing physical stability, lysosomal trafficking, and cellular activity. To identify DGJ-responsive mutant forms of alpha-Gal A, the effect of DGJ incubation on alpha-Gal A levels was assessed in cultured lymphoblasts from males with Fabry disease representing 75 different missense mutations, one insertion, and one splice-site mutation. Baseline alpha-Gal A levels ranged from 0 to 52% of normal. Increases in alpha-Gal A levels (1.5- to 28-fold) after continuous DGJ incubation for 5 days were seen for 49 different missense mutant forms with varying EC(50) values (820 nmol/L to1 mmol/L). Amino acid substitutions in responsive forms were located throughout both structural domains of the enzyme. Half of the missense mutant forms associated with classic (early-onset) Fabry disease and a majority (90%) associated with later-onset Fabry disease were responsive. In cultured fibroblasts from males with Fabry disease, the responses to DGJ were comparable to those of lymphoblasts with the same mutation. Importantly, elevated GL-3 levels in responsive Fabry fibroblasts were reduced after DGJ incubation, indicating that increased mutant alpha-Gal A levels can reduce accumulated substrate. These data indicate that DGJ merits further evaluation as a treatment for patients with Fabry disease with various missense mutations.

Published

2009

16. Detecting genetic variation in microarray expression data

Author

Mario Cáceres, Ondrej Libiger, Nicholas J. Schork, David J. Lockhart, Matthew A. Zapala, Jennifer A. Greenhall, and Carrolee Barlow

Subjects

Resource, Candidate gene, DNA, Complementary, Pan troglodytes, Mice, Inbred Strains, Biology, medicine.disease_cause, Mice, Species Specificity, Genetic linkage, Genetic variation, Gene expression, Genetics, medicine, Animals, Humans, Gene, Genetics (clinical), Oligonucleotide Array Sequence Analysis, Mutation, Oligonucleotide, Gene Expression Profiling, Genetic Variation, Gene expression profiling, Algorithms

Abstract

The use of high-density oligonucleotide arrays to measure the expression levels of thousands of genes in parallel has become commonplace. To take further advantage of the growing body of data, we developed a method, termed “GeSNP,” to mine the detailed hybridization patterns in oligonucleotide array expression data for evidence of genetic variation. To demonstrate the performance of the algorithm, the hybridization patterns in data obtained previously from SAMP8/Ta, SAMP10/Ta, and SAMR1/Ta inbred mice and from humans and chimpanzees were analyzed. Genes with consistent strain-specific and species-specific hybridization pattern differences were identified, and ∼90% of the candidate genes were independently confirmed to harbor sequence differences. Importantly, the quality of gene expression data was also improved by masking the probes of regions with putative sequence differences between species and strains. To illustrate the application to human disease groups, data from an inflammatory bowel disease study were analyzed. GeSNP identified sequence differences in candidate genes previously discovered in independent association and linkage studies and uncovered many promising new candidates. This approach enables the opportunistic extraction of genetic variation information from new or pre-existing gene expression data obtained with high-density oligonucleotide arrays.

Published

2007

17. Inhibition of drug-resistant mutants of ABL, KIT, and EGF receptor kinases

Author

Charles L. Sawyers, Zdravko V. Milanov, Miles A. Fabian, David J. Lockhart, Darren E. Insko, Philip T. Edeen, Lisa Wodicka, Anne Marie Velasco, Corey E. Atteridge, Julia M. Ford, Hitesh Patel, William H. Biggs, William Pao, Daniel K. Treiber, Sanna Herrgard, Patrick Parvis Zarrinkar, Neil P. Shah, Shamal A. Mehta, Robert M. Grotzfeld, Todd A. Carter, Harold E. Varmus, and Mark Floyd

Subjects

Indoles, Morpholines, Aurora inhibitor, Naphthalenes, Biology, Pharmacology, Piperazines, Cell Line, T790M, Gefitinib, Neoplasms, hemic and lymphatic diseases, Sunitinib, medicine, Humans, Pyrroles, Organic Chemicals, Oncogene Proteins v-abl, Protein Kinase Inhibitors, neoplasms, EGFR inhibitors, Aniline Compounds, Multidisciplinary, ABL, Biological Sciences, respiratory tract diseases, ErbB Receptors, Kinetics, Proto-Oncogene Proteins c-kit, Drug Resistance, Neoplasm, Mutation, Aminoquinolines, Cancer research, Pyrazoles, Erlotinib, FLT3 Inhibitor, medicine.drug

Abstract

To realize the full potential of targeted protein kinase inhibitors for the treatment of cancer, it is important to address the emergence of drug resistance in treated patients. Mutant forms of BCR-ABL, KIT, and the EGF receptor (EGFR) have been found that confer resistance to the drugs imatinib, gefitinib, and erlotinib. The mutations weaken or prevent drug binding, and interestingly, one of the most common sites of mutation in all three kinases is a highly conserved “gatekeeper” threonine residue near the kinase active site. We have identified existing clinical compounds that bind and inhibit drug-resistant mutant variants of ABL, KIT, and EGFR. We found that the Aurora kinase inhibitor VX-680 and the p38 inhibitor BIRB-796 inhibit the imatinib- and BMS-354825-resistant ABL(T315I) kinase. The KIT/FLT3 inhibitor SU-11248 potently inhibits the imatinib-resistant KIT(V559D/T670I) kinase, consistent with the clinical efficacy of SU-11248 against imatinib-resistant gastrointestinal tumors, and the EGFR inhibitors EKB-569 and CI-1033, but not GW-572016 and ZD-6474, potently inhibit the gefitinib- and erlotinib-resistant EGFR(L858R/T790M) kinase. EKB-569 and CI-1033 are already in clinical trials, and our results suggest that they should be considered for testing in the treatment of gefitinib/erlotinib-resistant non-small cell lung cancer. The results highlight the strategy of screening existing clinical compounds against newly identified drug-resistant mutant variants to find compounds that may serve as starting points for the development of next-generation drugs, or that could be used directly to treat patients that have acquired resistance to first-generation targeted therapy.

Published

2005

18. Oral Migalastat HCl Leads to Greater Systemic Exposure and Tissue Levels of Active α-Galactosidase A in Fabry Patients when Co-Administered with Infused Agalsidase

Author

Sheela Sitaraman, Mathews Adera, Myrl Holida, Mark Thomas, Kathy Nicholls, David G. Warnock, François Eyskens, Carrolee Barlow, Pol Boudes, Jay A. Barth, David J. Lockhart, John J. Flanagan, Daniel G. Bichet, Brandon Wustman, Ozlem Goker-Alpan, Suma P. Shankar, Franklin K. Johnson, Kenneth J. Valenzano, Richie Khanna, and Bigger, Brian W

Subjects

Oral, Adult, Male, 1-Deoxynojirimycin, General Science & Technology, Clinical Trials and Supportive Activities, Globotriaosylceramide, lcsh:Medicine, Administration, Oral, Pharmacology, chemistry.chemical_compound, Pharmacokinetics, Clinical Research, Migalastat, Blood plasma, Medicine, Humans, lcsh:Science, Infusion Pumps, Skin, Demography, Multidisciplinary, Alpha-galactosidase, biology, business.industry, lcsh:R, Neurosciences, Evaluation of treatments and therapeutic interventions, Enzyme replacement therapy, Middle Aged, medicine.disease, Fabry disease, Recombinant Proteins, Isoenzymes, chemistry, Tolerability, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, alpha-Galactosidase, Area Under Curve, Administration, biology.protein, Fabry Disease, lcsh:Q, Development of treatments and therapeutic interventions, business, Engineering sciences. Technology, Research Article

Abstract

Migalastat HCl (AT1001, 1-Deoxygalactonojirimycin) is an investigational pharmacological chaperone for the treatment of α-galactosidase A (α-Gal A) deficiency, which leads to Fabry disease, an X-linked, lysosomal storage disorder. The currently approved, biologics-based therapy for Fabry disease is enzyme replacement therapy (ERT) with either agalsidase alfa (Replagal) or agalsidase beta (Fabrazyme). Based on preclinical data, migalastat HCl in combination with agalsidase is expected to result in the pharmacokinetic (PK) enhancement of agalsidase in plasma by increasing the systemic exposure of active agalsidase, thereby leading to increased cellular levels in disease-relevant tissues. This Phase 2a study design consisted of an open-label, fixed-treatment sequence that evaluated the effects of single oral doses of 150 mg or 450 mg migalastat HCl on the PK and tissue levels of intravenously infused agalsidase (0.2, 0.5, or 1.0 mg/kg) in male Fabry patients. As expected, intravenous administration of agalsidase alone resulted in increased α-Gal A activity in plasma, skin, and peripheral blood mononuclear cells (PBMCs) compared to baseline. Following co-administration of migalastat HCl and agalsidase, α-Gal A activity in plasma was further significantly increased 1.2- to 5.1-fold compared to agalsidase administration alone, in 22 of 23 patients (95.6%). Importantly, similar increases in skin and PBMC α-Gal A activity were seen following co-administration of migalastat HCl and agalsidase. The effects were not related to the administered migalastat HCl dose, as the 150 mg dose of migalastat HCl increased α-Gal A activity to the same extent as the 450 mg dose. Conversely, agalsidase had no effect on the plasma PK of migalastat. No migalastat HCl-related adverse events or drug-related tolerability issues were identified. Trial Registration ClinicalTrials.gov {"type":"clinical-trial","attrs":{"text":"NCT01196871","term_id":"NCT01196871"}}NCT01196871

Published

2015

19. DNA arrays and neurobiology — what's new and what's next?

Author

Carrolee Barlow and David J. Lockhart

Subjects

Gene Expression Profiling, General Neuroscience, Brain, Computational biology, Biology, chemistry.chemical_compound, Neurobiology, chemistry, Animals, Profiling (information science), DNA microarray, Neuroscience, DNA, Oligonucleotide Array Sequence Analysis

Abstract

Genomic technologies such as DNA microarrays have been used to study biological processes involved in various normal and disease states; in addition, parallel transcriptional profiling methods hold a great deal of promise for the neurosciences. However, such experiments are technically more demanding and there are unique methodological difficulties for their use in the context of neurobiology and the study of central nervous system disorders.

Published

2002

20. Parallel Identification of New Genes in Saccharomyces cerevisiae

Author

Guy Oshiro, John R. Yates, Elizabeth A. Winzeler, Lisa Wodicka, Michael P. Washburn, and David J. Lockhart

Subjects

Saccharomyces cerevisiae Proteins, Letter, Transcription, Genetic, Genes, Fungal, Molecular Sequence Data, Saccharomyces cerevisiae, Biology, Genome, Mice, Open Reading Frames, Databases, Genetic, Genetics, Animals, Drosophila Proteins, Amino Acid Sequence, ORFS, Gene, Conserved Sequence, Genetics (clinical), Whole genome sequencing, Sequence Homology, Amino Acid, Gene Expression Profiling, Chromosome Mapping, Computational Biology, Genome project, biology.organism_classification, Gene expression profiling, Open reading frame, Protein Biosynthesis, Chromosomes, Fungal, Genome, Fungal, Peptides, Sequence Alignment

Abstract

Short open reading frames (ORFs) occur frequently in primary genome sequence. Distinguishing bona fide small genes from the tens of thousands of short ORFs is one of the most challenging aspects of genome annotation. Direct experimental evidence is often required. Here we use a combination of expression profiling and mass spectrometry to verify the independent transcription of 138 and the translation of 50 previously nonannotated genes in the Saccharomyces cerevisiae genome. Through combined evidence, we propose the addition of 62 new genes to the genome and provide experimental support for the inclusion of 10 previously identified genes.[The following individuals kindly provided reagents, samples, or unpublished information as indicated in the paper: V. Velculescu. Supplementary material is available online at http://www.genome.org.]

Published

2002

21. Chipping away at complex behavior: Transcriptome/phenotype correlations in the mouse brain

Author

Carrolee Barlow, Todd A. Carter, Jennifer A. Greenhall, Jo A. Del Rio, David J. Lockhart, and Mark L. Latronica

Subjects

Genetics, Candidate gene, Behavior, Animal, Transcription, Genetic, Brain, Gene Expression, Mice, Inbred Strains, Experimental and Cognitive Psychology, Motor Activity, Quantitative trait locus, Biology, Phenotype, Gene expression profiling, Transcriptome, Mice, Behavioral Neuroscience, Quantitative Trait, Heritable, Gene expression, Animals, DNA microarray, Gene

Abstract

Highly parallel gene expression profiling has the potential to provide new insight into the molecular mechanisms of complex brain diseases and behavioral traits. We review how gene expression profiling in various brain regions of inbred mouse strains has been used to identify genes that may contribute to strain-specific phenotypes. New data, which demonstrate the use of gene expression profiling in combination with behavioral testing to identify candidate genes involved in mediating variation in running wheel activity, are also presented. These and other studies suggest that a combination of gene expression profiling and more traditional genetic approaches, such as quantitative trait locus analysis, can be used to identify genes responsible for specific neurobehavioral phenotypes.

Published

2001

22. Analysis of gene expression profiles in normal and neoplastic ovarian tissue samples identifies candidate molecular markers of epithelial ovarian cancer

Author

Garret M. Hampton, Cynthia Behling, Robert A. Burger, David J. Lockhart, Suzanne G. Kern, Bradley J. Monk, John B. Welsh, Lisa M. Sapinoso, and Patrick P. Zarrinkar

Subjects

Genetic Markers, Cell, Biology, Malignancy, Cell Line, Reference Values, Gene expression, Biomarkers, Tumor, Tumor Cells, Cultured, medicine, Humans, RNA, Neoplasm, Gene, Oligonucleotide Array Sequence Analysis, Ovarian Neoplasms, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Ovary, Proteins, Reproducibility of Results, RNA, Biological Sciences, medicine.disease, Molecular biology, Adenocarcinoma, Papillary, medicine.anatomical_structure, Gene chip analysis, Female, Human genome, Ovarian cancer

Abstract

Epithelial ovarian cancer is the leading cause of death from gynecologic cancer, in part because of the lack of effective early detection methods. Although alterations of several genes, such as c-erb-B2, c-myc , and p53 , have been identified in a significant fraction of ovarian cancers, none of these mutations are diagnostic of malignancy or predictive of tumor behavior over time. Here, we used oligonucleotide microarrays with probe sets complementary to >6,000 human genes to identify genes whose expression correlated with epithelial ovarian cancer. We extended current microarray technology by simultaneously hybridizing ovarian RNA samples in a highly parallel manner to a single glass wafer containing 49 individual oligonucleotide arrays separated by gaskets within a custom-built chamber (termed “array-of-arrays”). Hierarchical clustering of the expression data revealed distinct groups of samples. Normal tissues were readily distinguished from tumor tissues, and tumors could be further subdivided into major groupings that correlated both to histological and clinical observations, as well as cell type-specific gene expression. A metric was devised to identify genes whose expression could be considered ideal for molecular determination of epithelial ovarian malignancies. The list of genes generated by this method was highly enriched for known markers of several epithelial malignancies, including ovarian cancer. This study demonstrates the rapidity with which large amounts of expression data can be generated. The results highlight important molecular features of human ovarian cancer and identify new genes as candidate molecular markers.

Published

2001

23. Effects of environmental enrichment on gene expression in the brain

Author

Claire Rampon, Yinghe Hu, Cecilia H. Jiang, Helin Dong, Ya-Ping Tang, Joe Z. Tsien, David J. Lockhart, and Peter G. Schultz

Subjects

Genetics, Environmental enrichment, Time Factors, Multidisciplinary, Gene Expression Profiling, Brain, Gene Expression, Cognition, Biological Sciences, Biology, Mice, Inbred C57BL, Gene expression profiling, Mice, Oligonucleotide Microarrays, Cognitive Changes, Gene expression, Synaptic plasticity, Mice, Inbred CBA, Animals, sense organs, Gene, Neuroscience

Abstract

An enriched environment is known to promote structural changes in the brain and to enhance learning and memory performance in rodents [Hebb, D. O. (1947)Am. Psychol.2, 306–307]. To better understand the molecular mechanisms underlying these experience-dependent cognitive changes, we have used high-density oligonucleotide microarrays to analyze gene expression in the brain. Expression of a large number of genes changes in response to enrichment training, many of which can be linked to neuronal structure, synaptic plasticity, and transmission. A number of these genes may play important roles in modulating learning and memory capacity.

Published

2000

24. Genomics, gene expression and DNA arrays

Author

Elizabeth A. Winzeler and David J. Lockhart

Subjects

Genetics, Messenger RNA, Genome, Multidisciplinary, Gene Expression Profiling, Gene Expression, RNA, Genomics, DNA, Computational biology, Biology, chemistry.chemical_compound, Gene Expression Regulation, Genes, chemistry, Data Interpretation, Statistical, Gene expression, Animals, Humans, Gene, Functional genomics, Oligonucleotide Array Sequence Analysis

Abstract

Experimental genomics in combination with the growing body of sequence information promise to revolutionize the way cells and cellular processes are studied. Information on genomic sequence can be used experimentally with high-density DNA arrays that allow complex mixtures of RNA and DNA to be interrogated in a parallel and quantitative fashion. DNA arrays can be used for many different purposes, most prominently to measure levels of gene expression (messenger RNA abundance) for tens of thousands of genes simultaneously. Measurements of gene expression and other applications of arrays embody much of what is implied by the term 'genomics'; they are broad in scope, large in scale, and take advantage of all available sequence information for experimental design and data interpretation in pursuit of biological understanding.

Published

2000

25. Myoseverin, a microtubule-binding molecule with novel cellular effects

Author

Daniel P. Sutherlin, Helin Dong, David J. Lockhart, Omar Perez, Peter G. Schultz, Gustavo R. Rosania, and Young-Tae Chang

Subjects

Transcription, Genetic, Cell division, medicine.medical_treatment, Cellular differentiation, Biomedical Engineering, Bioengineering, Biology, Microtubules, Applied Microbiology and Biotechnology, Cell Line, Mice, Peptide Library, Tubulin, Microtubule, In Situ Nick-End Labeling, medicine, Animals, Regeneration, Biotinylation, Microscopy, Phase-Contrast, Cytoskeleton, Gene Library, Genetics, Wound Healing, DNA synthesis, Myogenesis, Cell growth, Growth factor, Cell Cycle, Flow Cytometry, Immunohistochemistry, Actins, Cell biology, Purines, Cell culture, Molecular Medicine, Cell Division, Protein Binding, Biotechnology

Abstract

A new microtubule-binding molecule, myoseverin, was identified from a library of 2,6,9-trisubstituted purines in a morphological differentiation screen. Myoseverin induces the reversible fission of multinucleated myotubes into mononucleated fragments. Myotube fission promotes DNA synthesis and cell proliferation after removal of the compound and transfer of the cells to fresh growth medium. Transcriptional profiling and biochemical analysis indicate that myoseverin alone does not reverse the biochemical differentiation process. Instead, myoseverin affects the expression of a variety of growth factor, immunomodulatory, extracellular matrix-remodeling, and stress response genes, consistent with the activation of pathways involved in wound healing and tissue regeneration.

Published

2000

26. High density synthetic oligonucleotide arrays

Author

Stephen P. A. Fodor, David J. Lockhart, Thomas R. Gingeras, and Robert J. Lipshutz

Subjects

Genetics, Base Sequence, Genotype, Oligonucleotide, Oligonucleotides, Gene Expression, High density, Sequence (biology), Genomics, Computational biology, Biology, Animals, Database Management Systems, Humans, DNA microarray, Oligonucleotide Arrays, Molecular probe, Gene, Oligonucleotide Array Sequence Analysis

Abstract

Experimental genomics involves taking advantage of sequence information to investigate and understand the workings of genes, cells and organisms. We have developed an approach in which sequence information is used directly to design high-density, two-dimensional rays of synthetic oligonucleotides. The GeneChipe probe arrays are made using spatially patterned, light-directed combinatorial chemical synthesis and contain up to hundreds of thousands of different oligonucleotides on a small glass surface. The arrays have been designed and used for quantitative and highly parallel measurements of gene expression, to discover polymorphic loci and to detect the presence of thousands of alternative alleles. Here, we describe the fabrication of the arrays, their design and some specific applications to high-throughput genetic and cellular analysis.

Published

1999

27. A Genome-Wide Transcriptional Analysis of the Mitotic Cell Cycle

Author

Tyra G. Wolfsberg, Elizabeth A. Winzeler, Lisa Wodicka, David J. Lockhart, Lars M. Steinmetz, David Landsman, Ronald W. Davis, Andrew R. Conway, Michael J. Campbell, Raymond J. Cho, and Andrei Gabrielian

Subjects

Genetics, Regulation of gene expression, Cyclin-dependent kinase 1, Transcription, Genetic, Cell Cycle, Saccharomyces cerevisiae, Chromosome Mapping, Mitosis, RNA, Fungal, Cell Biology, Cell cycle, Biology, biology.organism_classification, Genome, Cell cycle phase, Mitotic cell cycle, Gene Expression Regulation, Fungal, RNA, Messenger, Chromosomes, Fungal, Genome, Fungal, DNA, Fungal, Molecular Biology, Gene

Abstract

cell cycle make it an attractive model for the study of genome-wide regulation of gene activity. Parallel identification of all of the genes in a genome that are coordinately regulated during such a process provides a conSummary sistent internal standard for comparison of gene activity over time and makes it possible to search statistically Progression through the eukaryotic cell cycle is known for candidate regulatory sequences. Although the cell to be both regulated and accompanied by periodic cycle‐dependent regulation of many individual genes fluctuation in the expression levels of numerous has been studied, comprehensive results for a genome genes. We report here the genome-wide characteriza- are likely to reveal novel functional and physical organition of mRNA transcript levels during the cell cycle of zation in coordinate gene regulation. These results also the budding yeast S. cerevisiae. Cell cycle‐dependent provide an opportunity to identify related genes in the periodicity was found for 416 of the 6220 monitored human genome that may be involved in cell cycle periodtranscripts. More than 25% of the 416 genes were specific roles. found directly adjacent to other genes in the genome One of the key mechanisms of gene regulation takes that displayed induction in the same cell cycle phase, place on the level of mRNA transcription. Availability of suggesting a mechanism for local chromosomal orga- complete sequence for the Saccharomyces cerevisiae nization in global mRNA regulation. More than 60% of genome has made it possible to quantitate mRNA tranthe characterized genes that displayed mRNA fluctua- script levels for virtually every yeast gene (DeRisi et al., tion have already been implicated in cell cycle period- 1997; Wodicka et al., 1997). In this study, commercially specific biological roles. Because more than 20% of available high-density oligonucleotide arrays were used human proteins display significant homology to yeast to quantitate mRNA transcript levels in synchronized proteins, these results also link a range of human yeast cells at regular intervals during the cell cycle. DNA genes to cell cycle period-specific biological func- oligonucleotide probes are directly synthesized on these tions.

Published

1998

28. Risk of Death in Heart Disease is Associated With Elevated Urinary Globotriaosylceramide

Author

Brian D. Lowes, Xiaoyang Wu, Paul A. Grayburn, Elfrida R. Benjamin, Maria Fuller, Nastry Brignol, Matthew R.G. Taylor, Xuan Wang, Caren Swift, David J. Lockhart, Derek Blankenship, Sabrina Forni, Raphael Schiffmann, and Lawrence Sweetman

Subjects

Adult, Male, medicine.medical_specialty, Heart Diseases, Heart disease, Epidemiology, Urinary system, DNA Mutational Analysis, Globotriaosylceramide, heart disease, Urine, Gastroenterology, chemistry.chemical_compound, Risk Factors, Tandem Mass Spectrometry, Internal medicine, medicine, Humans, Prospective Studies, Risk factor, Aged, Original Research, globotriaosylceramide, sphingolipids, Alpha-galactosidase, biology, business.industry, Trihexosylceramides, Case-control study, Clinical Enzyme Tests, Middle Aged, Prognosis, medicine.disease, Fabry disease, 6. Clean water, Up-Regulation, 3. Good health, Endocrinology, risk factor, chemistry, Case-Control Studies, alpha-Galactosidase, Mutation, biology.protein, Fabry Disease, Female, Cardiology and Cardiovascular Medicine, business, Biomarkers

Abstract

Background Elevated urinary globotriaosylceramide (Gb 3 ) has been considered a hallmark of F abry disease, an X‐linked lysosomal disorder that is a risk factor for most types of heart disease. Methods and Results We screened 1421 consecutive patients with common forms of heart disease for F abry disease by measuring urinary Gb 3 in whole urine using tandem mass spectrometry, α‐galactosidase A activity in dried blood spots, and we looked for GLA mutations by parallel sequencing of the whole gene (exons and introns) in pooled genomic DNA samples followed by Sanger sequencing verification. GLA variants were found in 13 patients. In the 1408 patients without GLA mutations, urinary Gb 3 levels were significantly higher in heart disease patients compared to 116 apparently healthy controls (median difference=10.0 ng/mL and P F abry disease (n=7) and heart disease patients with elevated urinary Gb 3 (n=6). Sphingomyelin and Gb 3 levels were abnormal in the left ventricular wall of patients with ischemic heart failure. Elevated levels of urinary Gb 3 were independently associated with increased risk of death in the average follow‐up of 17 months (hazard ratio=1.59 for increase in Gb 3 of 200, 95% CI =1.36 and 1.87, and P Conclusions In heart disease patients who do not have F abry disease or GLA gene mutations, a higher level of urinary Gb 3 is positively associated with near‐term mortality. The elevation of urinary Gb 3 and that of other lipids suggests that heart disease is associated with multiorgan lipid abnormalities. Clinical Trial Registration URL: clinicaltrials.gov. Unique Identifier: NCT 01019629.

Published

2014

29. The pharmacological chaperone AT2220 increases the specific activity and lysosomal delivery of mutant acid alpha-glucosidase, and promotes glycogen reduction in a transgenic mouse model of Pompe disease

Author

Kenneth J. Valenzano, Richie Khanna, Rohini Dhulipala, Nastry Brignol, Yi Lun, David J. Lockhart, Su Xu, Hung V. Do, Rebecca Soska, Michelle Frascella, Brandon Wustman, Jessie Feng, Lee Pellegrino, Anadina Garcia, Matthew J. Toth, and Allan C. Powe

Subjects

lcsh:Medicine, Administration, Oral, Endoplasmic Reticulum, Biochemistry, chemistry.chemical_compound, Gene Knockout Techniques, Mice, Glycogen storage disease type II, Chlorocebus aethiops, Enzyme Stability, Drug Discovery, Medicine and Health Sciences, lcsh:Science, Multidisciplinary, Glycogen, Glycogen Storage Disease Type II, Pharmacological chaperone, Isoenzymes, Protein Transport, COS Cells, Acid alpha-glucosidase, Metabolic Pathways, Glycogen Storage Diseases, Genetic Dominance, medicine.drug, Research Article, Biotechnology, Genetically modified mouse, congenital, hereditary, and neonatal diseases and abnormalities, 1-Deoxynojirimycin, Drug Research and Development, Biological Availability, Mice, Transgenic, Biology, Isozyme, Autosomal Recessive Diseases, medicine, Genetics, Animals, Humans, Pharmacology, Endoplasmic reticulum, lcsh:R, nutritional and metabolic diseases, Biology and Life Sciences, medicine.disease, Molecular biology, Disease Models, Animal, Metabolism, chemistry, Metabolic Disorders, Mutation, Proteolysis, Biocatalysis, lcsh:Q, Mutant Proteins, Glucan 1,4-alpha-Glucosidase, Lysosomes

Abstract

Pompe disease is an inherited lysosomal storage disorder that results from a deficiency in acid α-glucosidase (GAA) activity due to mutations in the GAA gene. Pompe disease is characterized by accumulation of lysosomal glycogen primarily in heart and skeletal muscles, which leads to progressive muscle weakness. We have shown previously that the small molecule pharmacological chaperone AT2220 (1-deoxynojirimycin hydrochloride, duvoglustat hydrochloride) binds and stabilizes wild-type as well as multiple mutant forms of GAA, and can lead to higher cellular levels of GAA. In this study, we examined the effect of AT2220 on mutant GAA, in vitro and in vivo, with a primary focus on the endoplasmic reticulum (ER)-retained P545L mutant form of human GAA (P545L GAA). AT2220 increased the specific activity of P545L GAA toward both natural (glycogen) and artificial substrates in vitro. Incubation with AT2220 also increased the ER export, lysosomal delivery, proteolytic processing, and stability of P545L GAA. In a new transgenic mouse model of Pompe disease that expresses human P545L on a Gaa knockout background (Tg/KO) and is characterized by reduced GAA activity and elevated glycogen levels in disease-relevant tissues, daily oral administration of AT2220 for 4 weeks resulted in significant and dose-dependent increases in mature lysosomal GAA isoforms and GAA activity in heart and skeletal muscles. Importantly, oral administration of AT2220 also resulted in significant glycogen reduction in disease-relevant tissues. Compared to daily administration, less-frequent AT2220 administration, including repeated cycles of 4 or 5 days with AT2220 followed by 3 or 2 days without drug, respectively, resulted in even greater glycogen reductions. Collectively, these data indicate that AT2220 increases the specific activity, trafficking, and lysosomal stability of P545L GAA, leads to increased levels of mature GAA in lysosomes, and promotes glycogen reduction in situ. As such, AT2220 may warrant further evaluation as a treatment for Pompe disease.

Published

2014

30. Genome-wide expression monitoring in Saccharomyces cerevisiae

Author

Helin Dong, David J. Lockhart, Michael Mittmann, Lisa Wodicka, and Ming-Hsiu Ho

Subjects

Light, Saccharomyces cerevisiae, Oligonucleotides, Biomedical Engineering, Bioengineering, Biology, Polymerase Chain Reaction, Applied Microbiology and Biotechnology, Genome, Nucleic acid thermodynamics, Gene Expression Regulation, Fungal, Gene expression, RNA, Messenger, Gene, Oligonucleotide, Nucleic acid sequence, Nucleic Acid Hybridization, Reproducibility of Results, RNA, Fungal, biology.organism_classification, Molecular biology, Yeast, Biochemistry, Molecular Medicine, Genome, Fungal, Cell Division, Biotechnology

Abstract

The genomic sequence of the budding yeast Saccharomyces cerevisiae has been used to design and synthesize high-density oligonucleotide arrays for monitoring the expression levels of nearly all yeast genes. This direct and highly parallel approach involves the hybridization of total mRNA populations to a set of four arrays that contain a total of more than 260,000 specifically chosen oligonucleotides synthesized in situ using light-directed combinatorial chemistry. The measurements are quantitative, sensitive, specific, and reproducible. Expression levels ranging from less than 0.1 copies to several hundred copies per cell have been measured for cells grown in rich and minimal media. Nearly 90% of all yeast mRNAs are observed to be present under both conditions, with approximately 50% present at levels between 0.1 and 1 copy per cell. Many of the genes observed to be differentially expressed under these conditions are expected, but large differences are also observed for many previously uncharacterized genes.

Published

1997

31. Response to Molecule–kinase interaction map

Author

William H. Biggs, David J. Lockhart, Daniel K. Treiber, Miles A. Fabian, and Patrick P. Zarrinkar

Subjects

Kinase, Chemistry, Biomedical Engineering, Biophysics, Molecular Medicine, Molecule, Bioengineering, Applied Microbiology and Biotechnology, Biotechnology

Published

2005

32. Accessing Genetic Information with High-Density DNA Arrays

Author

David Stern, Xiaohua C. Huang, Anthony Berno, Stephen P. A. Fodor, Earl Hubbell, Jim Winkler, Macdonald S. Morris, Robert Yang, Mark S. Chee, and David J. Lockhart

Subjects

medicine.medical_specialty, Mitochondrial DNA, Gene Expression, Computational biology, Biology, medicine.disease_cause, DNA, Mitochondrial, Polymerase Chain Reaction, Human mitochondrial genetics, chemistry.chemical_compound, Genetic linkage, Molecular genetics, medicine, Humans, Genetic variability, Cloning, Molecular, Genetics, Base Composition, Mutation, Genome, Polymorphism, Genetic, Multidisciplinary, Base Sequence, Genetic Variation, Nucleic Acid Hybridization, Phycoerythrin, Sequence Analysis, DNA, Fluoresceins, Mitochondria, chemistry, Fluorescein, Oligonucleotide Probes, Molecular probe, Algorithms, DNA

Abstract

Rapid access to genetic information is central to the revolution taking place in molecular genetics. The simultaneous analysis of the entire human mitochondrial genome is described here. DNA arrays containing up to 135,000 probes complementary to the 16.6-kilobase human mitochondrial genome were generated by light-directed chemical synthesis. A two-color labeling scheme was developed that allows simultaneous comparison of a polymorphic target to a reference DNA or RNA. Complete hybridization patterns were revealed in a matter of minutes. Sequence polymorphisms were detected with single-base resolution and unprecedented efficiency. The methods described are generic and can be used to address a variety of questions in molecular genetics including gene expression, genetic linkage, and genetic variability.

Published

1996

33. Migalastat HCl reduces globotriaosylsphingosine (lyso-Gb3) in Fabry transgenic mice and in the plasma of Fabry patients

Author

Hui-Hwa Chang, Sheela Sitaraman, Pol Boudes, Elfrida R. Benjamin, David J. Lockhart, Atul Mehta, Dominique P. Germain, Roberto Giugliani, Kathy Nicholls, Kenneth J. Valenzano, Derralynn Hughes, Nastry Brignol, Maria Fuller, Richie Khanna, Brandy Young-Gqamana, Rebecca Soska, Division of Medical Biochemistry, and Faculty of Health Sciences

Subjects

Male, Proteomics, Pathology, Mouse, Hydrolases, lcsh:Medicine, Administration, Oral, Pharmacology, Blood plasma, Urine, Mouse models, Biochemistry, Doença de Fabry, chemistry.chemical_compound, Mice, Clinical trials, Oral administration, Sphingosine, lcsh:Science, Camundongos transgênicos, Mice, Knockout, Kidney, Multidisciplinary, Spectrometric Identification of Proteins, biology, Enzyme Classes, Trihexosylceramides, Heart, Animal Models, Phase II, Enzymes, Pharmacological chaperone, medicine.anatomical_structure, Nephrology, Medicine, lipids (amino acids, peptides, and proteins), Phase II clinical investigation, medicine.drug, Research Article, medicine.medical_specialty, 1-Deoxynojirimycin, Preclinical Models, Globotriaosylceramide, Model Organisms, medicine, Animals, Humans, Animal Models of Disease, Liquid chromatography-mass spectrometry, Biology, Retrospective Studies, Sphingolipids, Alpha-galactosidase, Drug administration, lcsh:R, Reproducibility of Results, Kidneys, medicine.disease, Fabry disease, Mice, Inbred C57BL, chemistry, alpha-Galactosidase, Metabolic Disorders, Mutation, biology.protein, Fabry Disease, lcsh:Q, Glycolipids, Clinical research design

Abstract

Fabry disease (FD) results from mutations in the gene ( GLA ) that encodes the lysosomal enzyme α-galactosidase A (α-Gal A), and involves pathological accumulation of globotriaosylceramide (GL-3) and globotriaosylsphingosine (lyso-Gb 3 ). Migalastat hydrochloride (GR181413A) is a pharmacological chaperone that selectively binds, stabilizes, and increases cellular levels of α-Gal A. Oral administration of migalastat HCl reduces tissue GL-3 in Fabry transgenic mice, and in urine and kidneys of some FD patients. A liquid chromatography-tandem mass spectrometry method was developed to measure lyso-Gb 3 in mouse tissues and human plasma. Oral administration of migalastat HCl to transgenic mice reduced elevated lyso-Gb 3 levels up to 64%, 59%, and 81% in kidney, heart, and skin, respectively, generally equal to or greater than observed for GL-3. Furthermore, baseline plasma lyso-Gb 3 levels were markedly elevated in six male FD patients enrolled in Phase 2 studies. Oral administration of migalastat HCl (150 mg QOD) reduced urine GL-3 and plasma lyso-Gb 3 in three subjects (range: 15% to 46% within 48 weeks of treatment). In contrast, three showed no reductions in either substrate. These results suggest that measurement of tissue and/or plasma lyso-Gb 3 is feasible and may be warranted in future studies of migalastat HCl or other new potential therapies for FD.

Published

2012

34. O2‐04‐05: A cell‐based model for presenilin 1 early‐onset familial Alzheimer's disease (EOFAD): Dominant negative effects and relative stabilities of presenilin 1 with EOFAD mutations

Author

John J. Flanagan, Gary Lee, Brandon Wustman, Leo B. Dungan, David J. Lockhart, Anthony Stevens, Vernon Alford, Darlene Guillen, Hadis Williams, Evan Katz, Eric Sjoberg, Xiaoyang Wu, Carolyn Collins, and Sam Gandy

Subjects

Genetics, Epidemiology, Health Policy, Dominant negative, Biology, Presenilin, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Familial Alzheimer's disease, Neurology (clinical), Geriatrics and Gerontology, Early onset, Cell based

Published

2012

35. O1‐11‐05: Pharmacological chaperones increase wild type presenilin 1 levels and promote the normalization of gamma‐secretase function in presenilin 1 early‐onset familial Alzheimer's disease models

Author

Hadis Williams, Xiaoyang Wu, Vernon Alford, Leo B. Dungan, Richie Khanna, Anthony Stevens, Sam Gandy, Michelle Fascella, Nastry Brignol, Evan Katz, David J. Lockhart, Mark P. Mattson, Eric Sjoberg, Anadina Garcia, Brandon Wustman, Mohammed Mughal, Carolyn Collins, Julia Zhu, and Gary Lee

Subjects

Normalization (statistics), Epidemiology, Health Policy, Wild type, Biology, Presenilin, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Familial Alzheimer's disease, Cancer research, Neurology (clinical), Geriatrics and Gerontology, Function (biology), Gamma secretase, Early onset

Published

2012

36. Lysosomal dysfunction in a mouse model of Sandhoff disease leads to accumulation of ganglioside-bound amyloid-β peptide

Author

Frédéric Checler, Eric Sjoberg, Joseph D. Buxbaum, David J. Lockhart, Kenneth J. Valenzano, Katsuhiko Yanagisawa, Sam Gandy, Hadis Williams, Serene Keilani, Richie Khanna, Yi Lun, Brandon Wustman, Anthony Stevens, Departments of Neurology and Psychiatry, Alzheimer's Disease Research Center, Icahn School of Medicine at Mount Sinai [New York] (MSSM), Amicus Therapeutics, Institut de pharmacologie moléculaire et cellulaire (IPMC), Centre National de la Recherche Scientifique (CNRS)-Université Nice Sophia Antipolis (... - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Université Côte d'Azur (UCA), Friedman Brain Institute, Mount Sinai, National Center for Geriatrics and Gerontology, and Research Institute

Subjects

G(M2) Ganglioside, Vacuole, MESH: Mice, Knockout, Pathogenesis, MESH: Spinal Cord, Mice, 0302 clinical medicine, Gangliosides, Amyloid precursor protein, MESH: Animals, MESH: Brain Chemistry, MESH: Lipid Metabolism, Mice, Knockout, 0303 health sciences, Medulla Oblongata, General Neuroscience, MESH: G(M2) Ganglioside, Sandhoff Disease, Articles, MESH: Infant, Immunohistochemistry, MESH: Amyloid beta-Peptides, Cell biology, MESH: tau Proteins, Substantia Nigra, Biochemistry, Spinal Cord, MESH: Young Adult, Child, Preschool, alpha-Synuclein, Adult, Endosome, MESH: Hexosaminidase B, Blotting, Western, MESH: Substantia Nigra, Substantia nigra, tau Proteins, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Sandhoff disease, Biology, 03 medical and health sciences, Young Adult, Hexosaminidase B, MESH: Mice, Inbred C57BL, MESH: Medulla Oblongata, MESH: alpha-Synuclein, medicine, MESH: Blotting, Western, Animals, Humans, MESH: Mice, 030304 developmental biology, MESH: Gangliosides, Brain Chemistry, Ganglioside, MESH: Humans, Amyloid beta-Peptides, MESH: Child, Preschool, Infant, MESH: Adult, MESH: Immunohistochemistry, medicine.disease, Lipid Metabolism, HEXB, Mice, Inbred C57BL, biology.protein, MESH: Sandhoff Disease, Lysosomes, 030217 neurology & neurosurgery, MESH: Lysosomes

Abstract

Alterations in the lipid composition of endosomal–lysosomal membranes may constitute an early event in Alzheimer's disease (AD) pathogenesis. In this study, we investigated the possibility that GM2 ganglioside accumulation in a mouse model of Sandhoff disease might be associated with the accumulation of intraneuronal and extracellular proteins commonly observed in AD. Our results show intraneuronal accumulation of amyloid-β peptide (Aβ)-like, α-synuclein-like, and phospho-tau-like immunoreactivity in the brains of β-hexosaminidase knock-out (HEXBKO) mice. Biochemical and immunohistochemical analyses confirmed that at least some of the intraneuronal Aβ-like immunoreactivity (iAβ-LIR) represents amyloid precursor protein C-terminal fragments (APP-CTFs) and/or Aβ. In addition, we observed increased levels of Aβ40 and Aβ42 peptides in the lipid-associated fraction ofHEXBKO mouse brains, and intraneuronal accumulation of ganglioside-bound Aβ (GAβ) immunoreactivity in a brain region-specific manner. Furthermore, α-synuclein and APP-CTFs and/or Aβ were found to accumulate in different regions of the substantia nigra, indicating different mechanisms of accumulation or turnover pathways. Based on the localization of the accumulated iAβ-LIR to endosomes, lysosomes, and autophagosomes, we conclude that a significant accumulation of iAβ-LIR may be associated with the lysosomal–autophagic turnover of Aβ and fragments of APP-containing Aβ epitopes. Importantly, intraneuronal GAβ immunoreactivity, a proposed prefibrillar aggregate found in AD, was found to accumulate throughout the frontal cortices of postmortem human GM1 gangliosidosis, Sandhoff disease, and Tay–Sachs disease brains. Together, these results establish an association between the accumulation of gangliosides, autophagic vacuoles, and the intraneuronal accumulation of proteins associated with AD.

Published

2012

37. The pharmacological chaperone AT2220 increases recombinant human acid α-glucosidase uptake and glycogen reduction in a mouse model of Pompe disease

Author

Jessie Feng, Darlene Guillen, David J. Lockhart, Richie Khanna, Yi Lun, Kenneth J. Valenzano, John J. Flanagan, Michelle Frascella, Lee Pellegrino, and Rebecca Soska

Subjects

Protein Denaturation, Mouse, lcsh:Medicine, Biochemistry, chemistry.chemical_compound, Mice, Glycogen storage disease type II, Enzyme Stability, Drug Discovery, Lysosomal storage disease, lcsh:Science, Mice, Knockout, Multidisciplinary, Glycogen, Glycogen Storage Disease Type II, Enzyme replacement therapy, Animal Models, Recombinant Proteins, Enzymes, Pharmacological chaperone, medicine.drug, Half-Life, Research Article, Biotechnology, medicine.medical_specialty, 1-Deoxynojirimycin, Buffers, Enzyme activator, Model Organisms, In vivo, Internal medicine, medicine, Genetics, Animals, Humans, Biology, lcsh:R, Proteins, alpha-Glucosidases, Human Genetics, medicine.disease, Rats, Enzyme Activation, Disease Models, Animal, Endocrinology, chemistry, Small Molecules, Genetics of Disease, Rat, lcsh:Q

Abstract

Pompe disease is an inherited lysosomal storage disease that results from a deficiency in the enzyme acid α-glucosidase (GAA), and is characterized by progressive accumulation of lysosomal glycogen primarily in heart and skeletal muscles. Recombinant human GAA (rhGAA) is the only approved enzyme replacement therapy (ERT) available for the treatment of Pompe disease. Although rhGAA has been shown to slow disease progression and improve some of the pathophysiogical manifestations, the infused enzyme tends to be unstable at neutral pH and body temperature, shows low uptake into some key target tissues, and may elicit immune responses that adversely affect tolerability and efficacy. We hypothesized that co-administration of the orally-available, small molecule pharmacological chaperone AT2220 (1-deoxynojirimycin hydrochloride, duvoglustat hydrochloride) may improve the pharmacological properties of rhGAA via binding and stabilization. AT2220 co-incubation prevented rhGAA denaturation and loss of activity in vitro at neutral pH and 37°C in both buffer and blood. In addition, oral pre-administration of AT2220 to rats led to a greater than two-fold increase in the circulating half-life of intravenous rhGAA. Importantly, co-administration of AT2220 and rhGAA to GAA knock-out (KO) mice resulted in significantly greater rhGAA levels in plasma, and greater uptake and glycogen reduction in heart and skeletal muscles, compared to administration of rhGAA alone. Collectively, these preclinical data highlight the potentially beneficial effects of AT2220 on rhGAA in vitro and in vivo. As such, a Phase 2 clinical study has been initiated to investigate the effects of co-administered AT2220 on rhGAA in Pompe patients.

Published

2012

38. Liquid chromotography-tandem mass spectrometry determination of AT2220 in rodent plasma and tissues

Author

David J. Lockhart, Leo B. Dungan, Hui H. Chang, Richie Khanna, Nastry Brignol, Kenneth J. Valenzano, Rick Hamler, Elfrida R. Benjamin, Su Xu, and John J. Flanagan

Subjects

Endocrinology, Chromatography, Chemistry, Endocrinology, Diabetes and Metabolism, Genetics, Plasma, Tandem mass spectrometry, Molecular Biology, Biochemistry

Published

2014

39. Internal Stark Effect Measurement of the Electric Field at the Amino Terminus of an α Helix

Author

David J. Lockhart and Peter S. Kim

Subjects

Models, Molecular, Quantitative Biology::Biomolecules, Multidisciplinary, Field (physics), Protein Conformation, Chemistry, Molecular Sequence Data, Proteins, Water, Dielectric, Electrostatics, Molecular physics, symbols.namesake, Electric dipole moment, Nuclear magnetic resonance, Stark effect, Electric field, Helix, Electrochemistry, symbols, Spectrophotometry, Ultraviolet, Amino Acid Sequence, Amino Acids, Peptides, Alpha helix

Abstract

The strengths of electrostatic interactions in biological molecules are difficult to calculate or predict because they occur in complicated, inhomogeneous environments. The electric field at the amino terminus of an alpha helix in water has been determined by measuring the shift in the absorption band for a covalently attached, neutral probe molecule with an electric dipole moment difference between the ground and excited electronic states (an internal Stark effect). The field at the interface between the helix and the solvent is found to be an order of magnitude stronger than expected from the dielectric properties of bulk water. Furthermore, although the total electric dipole moment of the helix increases with length, the electric field at the amino terminus does not.

Published

1992

40. Arylcarboxyamino-substituted diaryl ureas as potent and selective FLT3 inhibitors

Author

Robert M. Grotzfeld, Shamal A. Mehta, Joyce James, Miles A. Fabian, Zdravko V. Milanov, David J. Lockhart, Shripad Bhagwat, Patrick P. Zarrinkar, Qi Chao, Andiliy G. Lai, Todd A. Carter, Anne Marie Velasco, Hitesh K. Patel, Daniel K. Treiber, and Kelly G. Sprankle

Subjects

medicine.drug_class, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Mice, Nude, Carboxamide, Antineoplastic Agents, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Mice, Structure-Activity Relationship, In vivo, Amide, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Urea, Molecular Biology, chemistry.chemical_classification, biology, Bicyclic molecule, Chemistry, Organic Chemistry, Xenograft Model Antitumor Assays, Bioavailability, Enzyme, fms-Like Tyrosine Kinase 3, Enzyme inhibitor, biology.protein, Molecular Medicine

Abstract

A series of diaryl ureas with an amide substitution at the 4-position was prepared and found to be potent and selective FLT3 inhibitors with good oral bioavailability and efficacy in a tumor xenograft model.

Published

2009

41. The pharmacological chaperone 1-deoxynojirimycin increases the activity and lysosomal trafficking of multiple mutant forms of acid alpha-glucosidase

Author

Elfrida R. Benjamin, Maria Rosaria Tuzzi, Katherine Tang, Kenneth J. Valenzano, John J. Flanagan, Federica Fontana, Maria Vittoria Cubellis, David J. Lockhart, Generoso Andria, Giancarlo Parenti, Xiaoyang Wu, Kirsten Mascioli, Hung V. Do, Caterina Porto, Barbara Rossi, Francesca Donaudy, Flanagan, Jj, Rossi, B, Tang, K, Wu, X, Mascioli, K, Donaudy, F, Tuzzi, Mr, Fontana, F, Cubellis, MARIA VITTORIA, Porto, C, Benjamin, E, Lockhart, Dj, Valenzano, Kj, Andria, Generoso, Parenti, Giancarlo, and Do, Hv

Subjects

Adult, Models, Molecular, congenital, hereditary, and neonatal diseases and abnormalities, 1-Deoxynojirimycin, Adolescent, Mutant, Biology, Protein Structure, Secondary, chemistry.chemical_compound, Chlorocebus aethiops, Enzyme Stability, Genetics, medicine, Animals, Humans, Genetics (clinical), Secretory pathway, chemistry.chemical_classification, LAMP2, Glycogen Storage Disease Type II, nutritional and metabolic diseases, Infant, alpha-Glucosidases, Transfection, Fibroblasts, Recombinant Proteins, Pharmacological chaperone, Protein Transport, Enzyme, chemistry, Biochemistry, COS Cells, Acid alpha-glucosidase, Mutant Proteins, Lysosomes, medicine.drug

Abstract

Pompe disease is a lysosomal storage disorder (LSD) caused by mutations in the gene that encodes acid α-glucosidase (GAA). Recently, small molecule pharmacological chaperones have been shown to increase protein stability and cellular levels for mutant lysosomal enzymes and have emerged as a new therapeutic strategy for the treatment of LSDs. In this study, we characterized the pharmacological chaperone 1-deoxynojirimycin (DNJ) on 76 different mutant forms of GAA identified in Pompe disease. DNJ significantly increased enzyme activity and protein levels for 16 different GAA mutants in patient-derived fibroblasts and in transiently transfected COS-7 cells. Additionally, DNJ increased the processing of these GAA mutants to their mature lysosomal forms, suggesting facilitated trafficking through the secretory pathway. Immunofluorescence microscopy studies showed increased colocalization of GAA with the lysosomal marker LAMP2 after incubation with DNJ, confirming increased lysosomal trafficking. Lastly, a GAA structural model was constructed based on the related eukaryotic glucosidase maltase-glucoamylase. The mutated residues identified in responsive forms of GAA are located throughout most of the structural domains, with half of these residues located in two short regions within the catalytic domain. Taken together, these data support further evaluation of DNJ as a potential treatment for Pompe disease in patients that express responsive forms of GAA. Hum Mutat 30:1–10, 2009. © 2009 Wiley-Liss, Inc.

Published

2009

42. Electric field effects on emission line shapes when electron transfer competes with emission: an example from photosynthetic reaction centers

Author

Stefan Franzen, Steven G. Boxer, David J. Lockhart, and Sharon L. Hammes

Subjects

Photosynthetic reaction centre, Electron transfer, symbols.namesake, Stark effect, Chemistry, Electric field, General Engineering, Analytical chemistry, symbols, Emission spectrum, Physical and Theoretical Chemistry, Atomic physics

Published

1991

43. Tuning a three-component reaction for trapping kinase substrate complexes

Author

Markus A. Seeliger, John Kuriyan, Miles A. Fabian, Dustin J. Maly, Patrick P. Zarrinkar, Kevan M. Shokat, William H. Biggs, David J. Lockhart, and Alexander V. Statsuk

Subjects

Adenosine, medicine.drug_class, Stereochemistry, Molecular Conformation, Thiophenes, Biochemistry, Catalysis, Article, Colloid and Surface Chemistry, Protein structure, medicine, Moiety, Humans, Cysteine, Phosphorylation, Fluorescent Dyes, biology, Chemistry, Kinase, Lysine, Phosphotransferases, Active site, Substrate (chemistry), Proteins, General Chemistry, Protein kinase inhibitor, Protein Structure, Tertiary, Cross-Linking Reagents, Models, Chemical, biology.protein, Peptides, HeLa Cells

Abstract

The upstream protein kinases responsible for thousands of phosphorylation events in the phosphoproteome remain to be discovered. We developed a three-component chemical reaction which converts the transient noncovalent substrate-kinase complex into a covalently cross-linked product by utilizing a dialdehyde-based cross-linker, 1. Unfortunately, the reaction of 1 with a lysine in the kinase active site and an engineered cysteine on the substrate to form an isoindole cross-linked product could not be performed in the presence of competing cellular proteins due to nonspecific side reactions. In order to more selectively target the cross-linker to protein kinases in cell lysates, we replaced the weak, kinase-binding adenosine moiety of 1 with a potent protein kinase inhibitor scaffold. In addition, we replaced the o-phthaldialdehyde moiety in 1 with a less-reactive thiophene-2,3-dicarboxaldehyde moiety. The combination of these two structural modifications provides for cross-linking of a cysteine-containing substrate to its corresponding kinase in the presence of competing cellular proteins.

Published

2008

44. Electric field effects on the initial electron-transfer kinetics in bacterial photosynthetic reaction centers

Author

David J. Lockhart, Steven G. Boxer, Christine Kirmaier, and Dewey Holten

Subjects

Photosynthetic reaction centre, Chemistry, Kinetics, General Engineering, Field effect, Quantum yield, Molecular physics, Gibbs free energy, Electron transfer, symbols.namesake, Superexchange, Electric field, symbols, Physical and Theoretical Chemistry, Atomic physics

Abstract

The effect of an applied electric field on the kinetics of the initial picosecond electron-transfer reaction in Rb. sphaeroides reaction centers has been measured in isotropic samples at 77 K. The net rate of formation of H{sub L} is reduced upon application of an electric field of 10{sup 6} V/cm, consistent with the previously observed increase in the quantum yield of the competing prompt fluorescence. The observed magnitude of the effect on the initial reaction is compared with the predictions of various models, and the consequences of including indirect electronic coupling between the initial and final states through a third state (superexchange) are investigated. It is found that the treatments of the initial electron-transfer reaction commonly in use greatly overestimate the magnitude of the field effect they are based on a dependence of the rate of electron transfer on the free energy change which is steeper than appears to be appropriate for this process.

Published

1990

45. DNA Chip Revolution

Author

David J. Lockhart

Subjects

Genetics, chemistry.chemical_compound, Microarray, Drug development, chemistry, Genetic variation, Genomics, Computational biology, DNA microarray, Biology, Massively parallel, Functional genomics, DNA

Abstract

The deoxyribonucleic acid (DNA) chips, arrays or microarrays are powerful new tools, designed and built based on genomic sequence information, that are changing the face of biological and biomedical research. The arrays enable massively parallel measurements of gene expression and genetic variation, and are dramatically increasing our understanding of biology and disease, and promise to have a great impact on drug development and the practice of medicine. Keywords: DNA arrays; microarrays; genomics; gene expression; polymorphisms

Published

2006

46. Structure of the kinase domain of an imatinib-resistant Abl mutant in complex with the Aurora kinase inhibitor VX-680

Author

Charles L. Sawyers, Markus A. Seeliger, Neil P. Shah, Luke H. Chao, Matthew A. Young, William H. Biggs, Hitesh K. Patel, Zdravko V. Milanov, John Kuriyan, Daniel K. Treiber, Patrick P. Zarrinkar, and David J. Lockhart

Subjects

Cancer Research, Protein Conformation, Mutant, Aurora inhibitor, Dasatinib, Fusion Proteins, bcr-abl, Biology, Genes, abl, Protein Serine-Threonine Kinases, Piperazines, chemistry.chemical_compound, Aurora kinase, Aurora Kinases, hemic and lymphatic diseases, Catalytic Domain, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, medicine, Escherichia coli, Humans, Phosphorylation, VX-680, Proto-Oncogene Proteins c-abl, neoplasms, Protein Kinase Inhibitors, ABL, Crystallography, Imatinib, Hydrogen Bonding, Thiazoles, Pyrimidines, Oncology, chemistry, Protein kinase domain, Drug Resistance, Neoplasm, Benzamides, Cancer research, Imatinib Mesylate, medicine.drug

Abstract

We present a high-resolution (2.0 Å) crystal structure of the catalytic domain of a mutant form of the Abl tyrosine kinase (H396P; Abl-1a numbering) that is resistant to the Abl inhibitor imatinib. The structure is determined in complex with the small-molecule inhibitor VX-680 (Vertex Pharmaceuticals, Cambridge, MA), which blocks the activity of various imatinib-resistant mutant forms of Abl, including one (T315I) that is resistant to both imatinib and BMS-354825 (dasatinib), a dual Src/Abl inhibitor that seems to be clinically effective against all other imatinib-resistant forms of BCR-Abl. VX-680 is shown to have significant inhibitory activity against BCR-Abl bearing the T315I mutation in patient-derived samples. The Abl kinase domain bound to VX-680 is not phosphorylated on the activation loop in the crystal structure but is nevertheless in an active conformation, previously unobserved for Abl and inconsistent with the binding of imatinib. The adoption of an active conformation is most likely the result of synergy between the His396Pro mutation, which destabilizes the inactive conformation required for imatinib binding, and the binding of VX-680, which favors the active conformation through hydrogen bonding and steric effects. VX-680 is bound to Abl in a mode that accommodates the substitution of isoleucine for threonine at residue 315 (the “gatekeeper” position). The avoidance of the innermost cavity of the Abl kinase domain by VX-680 and the specific recognition of the active conformation explain the effectiveness of this compound against mutant forms of BCR-Abl, including those with mutations at the gatekeeper position. (Cancer Res 2006; 66(2): 1007-14)

Published

2006

47. An Introduction to DNA Microarrays

Author

Kimberly S. Johnson, David J. Lockhart, and Patrick McConnell

Subjects

Microarray, Microarray analysis techniques, Gene chip analysis, Data analysis, Experimental validation, DNA microarray, Data science

Abstract

Oligonucleotide and DNA arrays, or microarrays, have proven to be useful tools to investigate biological function, and are the focal point of an increasing number of studies. However, most papers shed little light on the underlying basis and best use of microarray technology, often leaving a number of important questions unanswered. Under what conditions are microarrays helpful? How should microarray data be analyzed? What data analysis methods should be avoided? Which biological questions can microarrays address? Which biological questions are not best answered by microarrays? Here, we examine the technology itself, the data produced, proper experimental design, data analysis techniques, and experimental validation. These are issues important to all users of DNA arrays, from the mathematician who may have only limited knowledge of the biology behind the technology, to the biologist who is concerned with experimental design and the details of data analysis. Finally, we stress the importance of great experimental care, sample and data triage, well-characterized and rigorous analysis, and the need for appropriate follow-up and verification, especially when using animal or human tissue.

Published

2005

48. Aberrant recombination involving the granzyme locus occurs in Atm-/- T-cell lymphomas

Author

Winrow Christopher J, Zoë Weaver, Amy J. Warren, David J. Lockhart, Daniel G. Pankratz, Karl W. Hasel, Anthony Wynshaw-Boris, Marie A. Callahan, Carrolee Barlow, T. J. Bowen, Brian S. Hilbush, and Cecile Rose T. Vibat

Subjects

Population, Locus (genetics), Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, Biology, Protein Serine-Threonine Kinases, Lymphoma, T-Cell, Models, Biological, Granzymes, Loss of heterozygosity, Mice, Cell Line, Tumor, Genetics, medicine, Gene family, Animals, education, Molecular Biology, Genetics (clinical), In Situ Hybridization, Fluorescence, DNA Primers, Mice, Knockout, Recombination, Genetic, education.field_of_study, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Tumor Suppressor Proteins, Serine Endopeptidases, Computational Biology, General Medicine, medicine.disease, Blotting, Northern, Microarray Analysis, Molecular biology, Lymphoma, Granzyme B, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Granzyme, Ataxia-telangiectasia, Cytogenetic Analysis, Mutation, Cancer research, biology.protein

Abstract

Ataxia telangiectasia (A-T) is an autosomal recessive disease caused by loss of function of the serine/ threonine protein kinase ATM (ataxia telangiectasia mutated). A-T patients have a 250-700-fold increased risk of developing lymphomas and leukemias which are typically highly invasive and proliferative. In addition, a subset of adult acute lymphoblastic leukemias and aggressive B-cell chronic lymphocytic leukemias that occur in the general population show loss of heterozygosity for ATM. To define the specific role of ATM in lymphomagenesis, we studied T-cell lymphomas isolated from mice with mutations in ATM and/or p53 using cytogenetic analysis and mRNA transcriptional profiling. The analyses identified genes misregulated as a consequence of the amplifications, deletions and translocation events arising as a result of ATM loss. A specific recurrent disruption of the granzyme gene family locus was identified resulting In an aberrant granzyme B/C fusion product. The combined application of cytogenetic and gene expression approaches identified specific loci and genes that define the pathway of initiation and progression of lymphoreticular malignancies in the absence of ATM.

Published

2005

49. Adult mouse brain gene expression patterns bear an embryologic imprint

Author

Ron S. Broide, Warren G. Young, Wendy Tynan, Iiris Hovatta, Julie A. Ellison, Richard S. Tennant, Barbara S. Stoveken, Jo A. Del Rio, Daniel J. Lockhart, Lisa Wodicka, Rob Helton, David J. Lockhart, Floyd E. Bloom, John F. Reilly, Matthew A. Zapala, Carrolee Barlow, and Christopher J. Winrow

Subjects

Nervous system, Central Nervous System, Models, Neurological, Biology, Mice, Gene expression, Databases, Genetic, medicine, Animals, Cluster Analysis, Gene, Genetics, Regulation of gene expression, Multidisciplinary, Microarray analysis techniques, Gene Expression Profiling, Neural tube, Gene Expression Regulation, Developmental, Biological Sciences, Microarray Analysis, Biological Evolution, Gene expression profiling, medicine.anatomical_structure, Evolutionary biology, Homeobox, Algorithms

Abstract

The current model to explain the organization of the mammalian nervous system is based on studies of anatomy, embryology, and evolution. To further investigate the molecular organization of the adult mammalian brain, we have built a gene expression-based brain map. We measured gene expression patterns for 24 neural tissues covering the mouse central nervous system and found, surprisingly, that the adult brain bears a transcriptional “imprint” consistent with both embryological origins and classic evolutionary relationships. Embryonic cellular position along the anterior–posterior axis of the neural tube was shown to be closely associated with, and possibly a determinant of, the gene expression patterns in adult structures. We also observed a significant number of embryonic patterning and homeobox genes with region-specific expression in the adult nervous system. The relationships between global expression patterns for different anatomical regions and the nature of the observed region-specific genes suggest that the adult brain retains a degree of overall gene expression established during embryogenesis that is important for regional specificity and the functional relationships between regions in the adult. The complete collection of extensively annotated gene expression data along with data mining and visualization tools have been made available on a publicly accessible web site ( www.barlow-lockhart-brainmapnimhgrant.org ).

Published

2005

50. Glyoxalase 1 and glutathione reductase 1 regulate anxiety in mice

Author

Inder M. Verma, Carrolee Barlow, Robert A. Marr, Iiris Hovatta, Julie A. Ellison, Richard S. Tennant, Jeffrey M. Redwine, David J. Lockhart, Robert Helton, Eric E. Schadt, and Oded Singer

Subjects

Male, Glutathione reductase, Mice, Inbred Strains, Biology, Anxiety, Mice, Inbred strain, Transduction, Genetic, Gene expression, medicine, Animals, Gene, Genetics, Regulation of gene expression, Multidisciplinary, Panic disorder, Gene Expression Profiling, Lentivirus, Lactoylglutathione Lyase, Brain, medicine.disease, Gene expression profiling, Oxidative Stress, Glutathione Reductase, Phenotype, Gene Expression Regulation, Female, medicine.symptom

Abstract

Anxiety and fear are normal emotional responses to threatening situations. In human anxiety disorders--such as panic disorder, obsessive-compulsive disorder, post-traumatic stress disorder, social phobia, specific phobias and generalized anxiety disorder--these responses are exaggerated. The molecular mechanisms involved in the regulation of normal and pathological anxiety are mostly unknown. However, the availability of different inbred strains of mice offers an excellent model system in which to study the genetics of certain behavioural phenotypes. Here we report, using a combination of behavioural analysis of six inbred mouse strains with quantitative gene expression profiling of several brain regions, the identification of 17 genes with expression patterns that correlate with anxiety-like behavioural phenotypes. To determine if two of the genes, glyoxalase 1 and glutathione reductase 1, have a causal role in the genesis of anxiety, we performed genetic manipulation using lentivirus-mediated gene transfer. Local overexpression of these genes in the mouse brain resulted in increased anxiety-like behaviour, while local inhibition of glyoxalase 1 expression by RNA interference decreased the anxiety-like behaviour. Both of these genes are involved in oxidative stress metabolism, linking this pathway with anxiety-related behaviour.

Published

2005