HomeSearchTranslate
PhotosBiographyFacebookTwitter

From Wikipedia, the free encyclopedia

Robert K. Naviaux
Born
Robert Keith Naviaux

(1956-06-27)June 27, 1956
Woodland, California, U.S.
Education Georg August University, Göttingen, Germany (undergraduate biochemistry)

University of California, Davis (BS)

Indiana University (MA, MD, PhD; human genetics and virology)
Known forDiscovery of the cause of Alpers syndrome, Metabolic features of the cell danger response (CDR), Mitochondrial and metabolic features and stages of the healing cycle (salugenesis), Hyperpurinergia hypothesis for the genesis and treatment of autism
Spouse(s)
Jane Crowley Naviaux, MD, PhD
( m. 1987)
Children2
AwardsInaugural Kelsey Wright Award, UMDF (2001)

Autism trailblazer award, Autism Speaks (2011) Lifetime achievement award, MMS (2018) Pioneering achievement award, ISEAI (2019)

The Vanguard Award, UMDF (2023)
Scientific career
FieldsMitochondrial medicine, molecular and medical genetics, biochemical genetics, inborn errors of metabolism, metabolomics, virology, immunology, ecosystem biology, environmental medicine
Institutions UC San Diego
Thesis Construction and characterization of three infectious molecular clones of encephalomyocarditis virus (1989)
Doctoral advisorW. Dean Fraser, Milton W. Taylor, M. Ed Hodes, Joe C. Christian, George W. Jordan, Stuart H. Cohen
Website https://naviauxlab.ucsd.edu

Robert K. Naviaux (born in 1956) is an American physician-scientist who specializes in mitochondrial medicine and complex chronic disorders. He discovered the cause of Alpers syndrome, [1] [2] and was part of the team that reported the first mitochondrial DNA (mtDNA) mutation to cause genetic forms of autism. [3] Naviaux proposed the cell danger response (CDR) and hyperpurinergia hypothesis for complex disorders in 2014 [4] and directed the first FDA-approved clinical trial to study the safety and efficacy of the antipurinergic drug suramin as a new treatment for autism spectrum disorder (ASD). [5]

Naviaux is the founder and co-director of the Mitochondrial and Metabolic Disease Center (MMDC) at UCSD and is a Professor of Genetics in the departments of Medicine, Pediatrics, and Pathology at the UCSD School of Medicine, where he directs a core laboratory for metabolomics. He is the co-founder and a former president of the Mitochondrial Medicine Society (MMS) and a founding associate editor of the journal Mitochondrion. Naviaux received the 2023 United Mitochondrial Disease Foundation Vanguard Award. [6] [7]

Training

Naviaux received his B.S. in biological sciences from the University of California Davis. He studied natural killer cell biology and cancer immunology as an undergraduate research intern at the National Institutes of Health (NIH) and studied biochemistry and medical sociology at Georg August University in Göttingen, Germany as an education abroad student.[ citation needed] In 1981, he earned a master's in zoology and microbiology from Indiana University in Bloomington, Indiana. He was trained in the medical scientist training program (MSTP) at Indiana University and received his MD and PhD in medical genetics and virology in 1989. He was a resident and medical scholar in the clinical investigator pathway of the American Board of Internal Medicine (ABIM) at UC Davis Medical Center from 1986 to 1990.[ citation needed] In 1990, Naviaux was named a National Medical Resident of the Year by the National Institute of Diabetes, Digestive, and Kidney Disease (NIDDK, NIH). He did his postdoctoral training in gene therapy and retrovirus biology at the Salk Institute from 1990 to 1994, where he invented the pCL retroviral gene transfer vectors. [8] Naviaux was a Fogarty International scholar in India in 1994. He did his medical subspecialty training in pediatrics as a fellow in biochemical genetics and inborn errors of metabolism from 1994 to 1997 at the University of California, San Diego (UCSD) School of Medicine. In 1996, Naviaux founded the Mitochondrial and Metabolic Disease Center (MMDC) at UCSD. [9]

Research career

Naviaux joined the faculty of the University of California, San Diego in 1997. In 1999, he reported the cause of the classical neurogenetic disease Alpers-Huttenlocher syndrome. [1] [2] From 2003 to 2007, he studied the biophysical response of mitochondria to genetic and environmental stress. [10] [11] Studies on the role of mitochondria in regeneration and healing in the MRL mouse followed. [12] In 2008, he developed the concept of the cell danger response (CDR) and the hyperpurinergia hypothesis [13] that focused on abnormalities in ATP signaling as a root cause for the genesis and treatment of autism spectrum disorder (ASD). This led to a Trailblazer Award from Autism Speaks in 2011. After successful testing in several mouse models of ASD, [14] [15] [16] the antipurinergic drug suramin was found to be safe and effective as a new treatment for the core symptoms of autism in a small clinical trial of 10 children in the SAT1 trial. [5] Recent work in the Naviaux lab has showcased the connection between mitochondria, incomplete healing and aging, [17] and the connections between environmental health, mitochondria, the cell danger response, and the rising prevalence of chronic illness. [18]

References

  1. ^ a b Naviaux, Robert K.; Nyhan, William L.; Barshop, Bruce A.; Poulton, Joanna; Markusic, David; Karpinski, Nancy C.; Haas, Richard H. (January 1999). "Mitochondrial DNA polymerase ? deficiency and mtDNA depletion in a child with Alpers' syndrome". Annals of Neurology. 45 (1): 54–58. doi: 10.1002/1531-8249(199901)45:1<54::aid-art10>3.0.co;2-b. ISSN  0364-5134. PMID  9894877. S2CID  72829923.
  2. ^ a b ALPERS, BERNARD J. (March 1, 1931). "Diffuse Progressive Degeneration of the Gray Matter of the Cerebrum". Archives of Neurology and Psychiatry. 25 (3): 469. doi: 10.1001/archneurpsyc.1931.02230030027002. ISSN  0096-6754.
  3. ^ Graf, William D.; Marin-Garcia, Jose; Gao, H.G.; Pizzo, Senia; Naviaux, Robert K.; Markusic, David; Barshop, Bruce A.; Courchesne, Eric; Haas, Richard H. (June 1, 2000). "Autism Associated With the Mitochondrial DNA G8363A Transfer RNALys Mutation". Journal of Child Neurology. 15 (6): 357–361. doi: 10.1177/088307380001500601. ISSN  0883-0738. PMID  10868777. S2CID  37548666.
  4. ^ Naviaux, Robert K. (May 1, 2014). "Metabolic features of the cell danger response". Mitochondrion. 16: 7–17. doi: 10.1016/j.mito.2013.08.006. ISSN  1567-7249. PMID  23981537.
  5. ^ a b Naviaux, Robert K.; Curtis, Brooke; Li, Kefeng; Naviaux, Jane C.; Bright, A. Taylor; Reiner, Gail E.; Westerfield, Marissa; Goh, Suzanne; Alaynick, William A.; Wang, Lin; Capparelli, Edmund V. (2017). "Low-dose suramin in autism spectrum disorder: a small, phase I/II, randomized clinical trial". Annals of Clinical and Translational Neurology. 4 (7): 491–505. doi: 10.1002/acn3.424. ISSN  2328-9503. PMC  5497533. PMID  28695149.
  6. ^ "UMDF Celebrates 2023 Vanguard Award Winner".
  7. ^ "Robert K Naviaux Receives United Mitochondrial Disease Foundations Vanguard Award".
  8. ^ Naviaux, R K; Costanzi, E; Haas, M; Verma, I M (August 1996). "The pCL vector system: rapid production of helper-free, high-titer, recombinant retroviruses". Journal of Virology. 70 (8): 5701–5705. doi: 10.1128/jvi.70.8.5701-5705.1996. ISSN  0022-538X. PMC  190538. PMID  8764092.
  9. ^ Haas, RH; Naviaux, RK (2019). "A brief history of the Mitochondrial Medicine Society—The first 20 years, 1998-2018". Mitochondrial and Metabolic Medicine. 1: 1–7.
  10. ^ Gourley, Paul Lee; Hendricks, Judy Kay; McDonald, Anthony E.; Copeland, R. G.; Yaffe, Michael P.; Naviaux, Robert K. (September 2007). "Reactive biomolecular divergence in genetically altered yeast cells and isolated mitochondria as measured by biocavity laser spectroscopy: rapid diagnostic method for studying cellular responses to stress and disease". Journal of Biomedical Optics. 12 (5): 054003. Bibcode: 2007JBO....12e4003G. doi: 10.1117/1.2799198. ISSN  1083-3668. PMID  17994891. S2CID  21850240.
  11. ^ Gourley, Paul L.; Hendricks, Judy K.; McDonald, Anthony E.; Copeland, R. Guild; Barrett, Keith E.; Gourley, Cheryl R.; Singh, Keshav K; Naviaux, Robert K. (December 2005). "Mitochondrial Correlation Microscopy and Nanolaser Spectroscopy — New Tools for Biophotonic Detection of Cancer in Single Cells". Technology in Cancer Research & Treatment. 4 (6): 585–592. doi: 10.1177/153303460500400602. ISSN  1533-0346. PMID  16292878. S2CID  28063390.
  12. ^ Naviaux, Robert K.; Le, Thuy P.; Bedelbaeva, Khamilia; Leferovich, John; Gourevitch, Dmitri; Sachadyn, Pawel; Zhang, Xiang-Ming; Clark, Lise; Heber-Katz, Ellen (March 1, 2009). "Retained features of embryonic metabolism in the adult MRL mouse". Molecular Genetics and Metabolism. 96 (3): 133–144. doi: 10.1016/j.ymgme.2008.11.164. ISSN  1096-7192. PMC  3646557. PMID  19131261.
  13. ^ "The Neuroscience of Autism Spectrum Disorders - 1st Edition". www.elsevier.com. Retrieved April 28, 2021.
  14. ^ Naviaux, Jane C.; Wang, Lin; Li, Kefeng; Bright, A. Taylor; Alaynick, William A.; Williams, Kenneth R.; Powell, Susan B.; Naviaux, Robert K. (January 13, 2015). "Antipurinergic therapy corrects the autism-like features in the Fragile X (Fmr1 knockout) mouse model". Molecular Autism. 6 (1): 1. doi: 10.1186/2040-2392-6-1. ISSN  2040-2392. PMC  4334917. PMID  25705365.
  15. ^ Naviaux, J. C.; Schuchbauer, M. A.; Li, K.; Wang, L.; Risbrough, V. B.; Powell, S. B.; Naviaux, R. K. (June 2014). "Reversal of autism-like behaviors and metabolism in adult mice with single-dose antipurinergic therapy". Translational Psychiatry. 4 (6): e400. doi: 10.1038/tp.2014.33. ISSN  2158-3188. PMC  4080315. PMID  24937094.
  16. ^ Naviaux, Robert K.; Zolkipli, Zarazuela; Wang, Lin; Nakayama, Tomohiro; Naviaux, Jane C.; Le, Thuy P.; Schuchbauer, Michael A.; Rogac, Mihael; Tang, Qingbo; Dugan, Laura L.; Powell, Susan B. (March 13, 2013). "Antipurinergic Therapy Corrects the Autism-Like Features in the Poly(IC) Mouse Model". PLOS ONE. 8 (3): e57380. Bibcode: 2013PLoSO...857380N. doi: 10.1371/journal.pone.0057380. ISSN  1932-6203. PMC  3596371. PMID  23516405.
  17. ^ Naviaux, Robert K. (June 2019). "Incomplete Healing as a Cause of Aging: The Role of Mitochondria and the Cell Danger Response". Biology. 8 (2): 27. doi: 10.3390/biology8020027. PMC  6627909. PMID  31083530.
  18. ^ Naviaux, Robert K. (March 2020). "Perspective: Cell danger response Biology—The new science that connects environmental health with mitochondria and the rising tide of chronic illness". Mitochondrion. 51: 40–45. doi: 10.1016/j.mito.2019.12.005. ISSN  1567-7249. PMID  31877376. S2CID  209488913.
Retrieved from " https://en.wikipedia.org/?title=Robert_K._Naviaux&oldid=1193271623"
From Wikipedia, the free encyclopedia

Robert K. Naviaux
Born
Robert Keith Naviaux

(1956-06-27)June 27, 1956
Woodland, California, U.S.
Education Georg August University, Göttingen, Germany (undergraduate biochemistry)

University of California, Davis (BS)

Indiana University (MA, MD, PhD; human genetics and virology)
Known forDiscovery of the cause of Alpers syndrome, Metabolic features of the cell danger response (CDR), Mitochondrial and metabolic features and stages of the healing cycle (salugenesis), Hyperpurinergia hypothesis for the genesis and treatment of autism
Spouse(s)
Jane Crowley Naviaux, MD, PhD
( m. 1987)
Children2
AwardsInaugural Kelsey Wright Award, UMDF (2001)

Autism trailblazer award, Autism Speaks (2011) Lifetime achievement award, MMS (2018) Pioneering achievement award, ISEAI (2019)

The Vanguard Award, UMDF (2023)
Scientific career
FieldsMitochondrial medicine, molecular and medical genetics, biochemical genetics, inborn errors of metabolism, metabolomics, virology, immunology, ecosystem biology, environmental medicine
Institutions UC San Diego
Thesis Construction and characterization of three infectious molecular clones of encephalomyocarditis virus (1989)
Doctoral advisorW. Dean Fraser, Milton W. Taylor, M. Ed Hodes, Joe C. Christian, George W. Jordan, Stuart H. Cohen
Website https://naviauxlab.ucsd.edu

Robert K. Naviaux (born in 1956) is an American physician-scientist who specializes in mitochondrial medicine and complex chronic disorders. He discovered the cause of Alpers syndrome, [1] [2] and was part of the team that reported the first mitochondrial DNA (mtDNA) mutation to cause genetic forms of autism. [3] Naviaux proposed the cell danger response (CDR) and hyperpurinergia hypothesis for complex disorders in 2014 [4] and directed the first FDA-approved clinical trial to study the safety and efficacy of the antipurinergic drug suramin as a new treatment for autism spectrum disorder (ASD). [5]

Naviaux is the founder and co-director of the Mitochondrial and Metabolic Disease Center (MMDC) at UCSD and is a Professor of Genetics in the departments of Medicine, Pediatrics, and Pathology at the UCSD School of Medicine, where he directs a core laboratory for metabolomics. He is the co-founder and a former president of the Mitochondrial Medicine Society (MMS) and a founding associate editor of the journal Mitochondrion. Naviaux received the 2023 United Mitochondrial Disease Foundation Vanguard Award. [6] [7]

Training

Naviaux received his B.S. in biological sciences from the University of California Davis. He studied natural killer cell biology and cancer immunology as an undergraduate research intern at the National Institutes of Health (NIH) and studied biochemistry and medical sociology at Georg August University in Göttingen, Germany as an education abroad student.[ citation needed] In 1981, he earned a master's in zoology and microbiology from Indiana University in Bloomington, Indiana. He was trained in the medical scientist training program (MSTP) at Indiana University and received his MD and PhD in medical genetics and virology in 1989. He was a resident and medical scholar in the clinical investigator pathway of the American Board of Internal Medicine (ABIM) at UC Davis Medical Center from 1986 to 1990.[ citation needed] In 1990, Naviaux was named a National Medical Resident of the Year by the National Institute of Diabetes, Digestive, and Kidney Disease (NIDDK, NIH). He did his postdoctoral training in gene therapy and retrovirus biology at the Salk Institute from 1990 to 1994, where he invented the pCL retroviral gene transfer vectors. [8] Naviaux was a Fogarty International scholar in India in 1994. He did his medical subspecialty training in pediatrics as a fellow in biochemical genetics and inborn errors of metabolism from 1994 to 1997 at the University of California, San Diego (UCSD) School of Medicine. In 1996, Naviaux founded the Mitochondrial and Metabolic Disease Center (MMDC) at UCSD. [9]

Research career

Naviaux joined the faculty of the University of California, San Diego in 1997. In 1999, he reported the cause of the classical neurogenetic disease Alpers-Huttenlocher syndrome. [1] [2] From 2003 to 2007, he studied the biophysical response of mitochondria to genetic and environmental stress. [10] [11] Studies on the role of mitochondria in regeneration and healing in the MRL mouse followed. [12] In 2008, he developed the concept of the cell danger response (CDR) and the hyperpurinergia hypothesis [13] that focused on abnormalities in ATP signaling as a root cause for the genesis and treatment of autism spectrum disorder (ASD). This led to a Trailblazer Award from Autism Speaks in 2011. After successful testing in several mouse models of ASD, [14] [15] [16] the antipurinergic drug suramin was found to be safe and effective as a new treatment for the core symptoms of autism in a small clinical trial of 10 children in the SAT1 trial. [5] Recent work in the Naviaux lab has showcased the connection between mitochondria, incomplete healing and aging, [17] and the connections between environmental health, mitochondria, the cell danger response, and the rising prevalence of chronic illness. [18]

References

  1. ^ a b Naviaux, Robert K.; Nyhan, William L.; Barshop, Bruce A.; Poulton, Joanna; Markusic, David; Karpinski, Nancy C.; Haas, Richard H. (January 1999). "Mitochondrial DNA polymerase ? deficiency and mtDNA depletion in a child with Alpers' syndrome". Annals of Neurology. 45 (1): 54–58. doi: 10.1002/1531-8249(199901)45:1<54::aid-art10>3.0.co;2-b. ISSN  0364-5134. PMID  9894877. S2CID  72829923.
  2. ^ a b ALPERS, BERNARD J. (March 1, 1931). "Diffuse Progressive Degeneration of the Gray Matter of the Cerebrum". Archives of Neurology and Psychiatry. 25 (3): 469. doi: 10.1001/archneurpsyc.1931.02230030027002. ISSN  0096-6754.
  3. ^ Graf, William D.; Marin-Garcia, Jose; Gao, H.G.; Pizzo, Senia; Naviaux, Robert K.; Markusic, David; Barshop, Bruce A.; Courchesne, Eric; Haas, Richard H. (June 1, 2000). "Autism Associated With the Mitochondrial DNA G8363A Transfer RNALys Mutation". Journal of Child Neurology. 15 (6): 357–361. doi: 10.1177/088307380001500601. ISSN  0883-0738. PMID  10868777. S2CID  37548666.
  4. ^ Naviaux, Robert K. (May 1, 2014). "Metabolic features of the cell danger response". Mitochondrion. 16: 7–17. doi: 10.1016/j.mito.2013.08.006. ISSN  1567-7249. PMID  23981537.
  5. ^ a b Naviaux, Robert K.; Curtis, Brooke; Li, Kefeng; Naviaux, Jane C.; Bright, A. Taylor; Reiner, Gail E.; Westerfield, Marissa; Goh, Suzanne; Alaynick, William A.; Wang, Lin; Capparelli, Edmund V. (2017). "Low-dose suramin in autism spectrum disorder: a small, phase I/II, randomized clinical trial". Annals of Clinical and Translational Neurology. 4 (7): 491–505. doi: 10.1002/acn3.424. ISSN  2328-9503. PMC  5497533. PMID  28695149.
  6. ^ "UMDF Celebrates 2023 Vanguard Award Winner".
  7. ^ "Robert K Naviaux Receives United Mitochondrial Disease Foundations Vanguard Award".
  8. ^ Naviaux, R K; Costanzi, E; Haas, M; Verma, I M (August 1996). "The pCL vector system: rapid production of helper-free, high-titer, recombinant retroviruses". Journal of Virology. 70 (8): 5701–5705. doi: 10.1128/jvi.70.8.5701-5705.1996. ISSN  0022-538X. PMC  190538. PMID  8764092.
  9. ^ Haas, RH; Naviaux, RK (2019). "A brief history of the Mitochondrial Medicine Society—The first 20 years, 1998-2018". Mitochondrial and Metabolic Medicine. 1: 1–7.
  10. ^ Gourley, Paul Lee; Hendricks, Judy Kay; McDonald, Anthony E.; Copeland, R. G.; Yaffe, Michael P.; Naviaux, Robert K. (September 2007). "Reactive biomolecular divergence in genetically altered yeast cells and isolated mitochondria as measured by biocavity laser spectroscopy: rapid diagnostic method for studying cellular responses to stress and disease". Journal of Biomedical Optics. 12 (5): 054003. Bibcode: 2007JBO....12e4003G. doi: 10.1117/1.2799198. ISSN  1083-3668. PMID  17994891. S2CID  21850240.
  11. ^ Gourley, Paul L.; Hendricks, Judy K.; McDonald, Anthony E.; Copeland, R. Guild; Barrett, Keith E.; Gourley, Cheryl R.; Singh, Keshav K; Naviaux, Robert K. (December 2005). "Mitochondrial Correlation Microscopy and Nanolaser Spectroscopy — New Tools for Biophotonic Detection of Cancer in Single Cells". Technology in Cancer Research & Treatment. 4 (6): 585–592. doi: 10.1177/153303460500400602. ISSN  1533-0346. PMID  16292878. S2CID  28063390.
  12. ^ Naviaux, Robert K.; Le, Thuy P.; Bedelbaeva, Khamilia; Leferovich, John; Gourevitch, Dmitri; Sachadyn, Pawel; Zhang, Xiang-Ming; Clark, Lise; Heber-Katz, Ellen (March 1, 2009). "Retained features of embryonic metabolism in the adult MRL mouse". Molecular Genetics and Metabolism. 96 (3): 133–144. doi: 10.1016/j.ymgme.2008.11.164. ISSN  1096-7192. PMC  3646557. PMID  19131261.
  13. ^ "The Neuroscience of Autism Spectrum Disorders - 1st Edition". www.elsevier.com. Retrieved April 28, 2021.
  14. ^ Naviaux, Jane C.; Wang, Lin; Li, Kefeng; Bright, A. Taylor; Alaynick, William A.; Williams, Kenneth R.; Powell, Susan B.; Naviaux, Robert K. (January 13, 2015). "Antipurinergic therapy corrects the autism-like features in the Fragile X (Fmr1 knockout) mouse model". Molecular Autism. 6 (1): 1. doi: 10.1186/2040-2392-6-1. ISSN  2040-2392. PMC  4334917. PMID  25705365.
  15. ^ Naviaux, J. C.; Schuchbauer, M. A.; Li, K.; Wang, L.; Risbrough, V. B.; Powell, S. B.; Naviaux, R. K. (June 2014). "Reversal of autism-like behaviors and metabolism in adult mice with single-dose antipurinergic therapy". Translational Psychiatry. 4 (6): e400. doi: 10.1038/tp.2014.33. ISSN  2158-3188. PMC  4080315. PMID  24937094.
  16. ^ Naviaux, Robert K.; Zolkipli, Zarazuela; Wang, Lin; Nakayama, Tomohiro; Naviaux, Jane C.; Le, Thuy P.; Schuchbauer, Michael A.; Rogac, Mihael; Tang, Qingbo; Dugan, Laura L.; Powell, Susan B. (March 13, 2013). "Antipurinergic Therapy Corrects the Autism-Like Features in the Poly(IC) Mouse Model". PLOS ONE. 8 (3): e57380. Bibcode: 2013PLoSO...857380N. doi: 10.1371/journal.pone.0057380. ISSN  1932-6203. PMC  3596371. PMID  23516405.
  17. ^ Naviaux, Robert K. (June 2019). "Incomplete Healing as a Cause of Aging: The Role of Mitochondria and the Cell Danger Response". Biology. 8 (2): 27. doi: 10.3390/biology8020027. PMC  6627909. PMID  31083530.
  18. ^ Naviaux, Robert K. (March 2020). "Perspective: Cell danger response Biology—The new science that connects environmental health with mitochondria and the rising tide of chronic illness". Mitochondrion. 51: 40–45. doi: 10.1016/j.mito.2019.12.005. ISSN  1567-7249. PMID  31877376. S2CID  209488913.
Retrieved from " https://en.wikipedia.org/?title=Robert_K._Naviaux&oldid=1193271623"

Videos

Youtube | Vimeo | Bing

Websites

Google | Yahoo | Bing

Encyclopedia

Google | Yahoo | Bing

Facebook




Top Of Page

HomeSearchTranslate

© CSE