Edward A Lakatta126 Briarcliff Ln, Bel Air, MD 21014

Edward Lakatta Phones & Addresses

126 Briarcliff Ln, Bel Air, MD 21014 (410) 879-8782

530 Murdock Rd, Baltimore, MD 21212 (410) 377-9229

221 Stony Run Dr, Baltimore, MD 21210 (410) 243-9929

1 Chase St, Baltimore, MD 21202

128 Overbrook Rd, Govans, MD 21212 (410) 377-9229

48 82Nd St, New York, NY 10024

Work

Company: National Institute On Aging Address: 251 Bayview Blvd Suite 100, Baltimore, MD 21224 Phones: (410) 558-8573 (Phone)

Education

School / High School: Georgetown University 1970

Languages

English

Awards

Healthgrades Honor Roll

Ranks

Certificate: Cardiovascular Disease, 1977

Mentions for Edward A Lakatta

Career records & work history

Lawyers & Attorneys

Edward Lakatta Photo 1

Edward A Lakatta - Lawyer

Address:
(302) 282-3019 (Office)
Licenses:
Delaware - Active 2006
Edward Lakatta Photo 2

Edward Alexander Lakatta, Baltimore MD - Lawyer

Address:
530 Murdock Rd, Baltimore, MD 21212
(302) 282-3019 (Office)
Licenses:
Maryland - Active 1996

Medicine Doctors

Edward Lakatta Photo 3

Dr. Edward G Lakatta, Baltimore MD - MD (Doctor of Medicine)

Specialties:
Cardiology
Address:
National Institute On Aging
251 Bayview Blvd Suite 100, Baltimore, MD 21224
(410) 558-8573 (Phone)
Certifications:
Cardiovascular Disease, 1977
Internal Medicine, 1973
Awards:
Healthgrades Honor Roll
Languages:
English
Education:
Medical School
Georgetown University
Graduated: 1970
Medical School
Strong Memorial Hospital
Graduated: 1970
Medical School
Medstar-Georgetown University Medical Center
Graduated: 1970
Medical School
The Johns Hopkins Hospital
Graduated: 1970
Medical School
Univ Coll
Graduated: 1970

Edward G. Lakatta

Specialties:
Cardiovascular Disease
Work:
National Institute On Aging
251 Bayview Blvd STE 100, Baltimore, MD 21224
(410) 558-8573 (phone) (410) 558-8137 (fax)
Education:
Medical School
Georgetown University School of Medicine
Graduated: 1970
Languages:
English, Spanish
Description:
Dr. Lakatta graduated from the Georgetown University School of Medicine in 1970. He works in Baltimore, MD and specializes in Cardiovascular Disease.
Edward Lakatta Photo 4

Edward Gerard Lakatta, Baltimore MD

Specialties:
Internal Medicine
Cardiovascular Disease
Cardiology
Work:
National Institute On Aging
5600 Nathan Shock Dr, Baltimore, MD 21224
Education:
Georgetown University (1970)
Edward Lakatta Photo 5

Edward Gerard Lakatta, Baltimore MD

Specialties:
Cardiologist
Address:
5600 Nathan Shock Dr, Baltimore, MD 21224
Education:
Georgetown University, School of Medicine - Doctor of Medicine
Georgetown University Hospital - Fellowship - Cardiology
Johns Hopkins Hospital - Fellowship - Cardiology
Board certifications:
American Board of Internal Medicine Certification in Internal Medicine
American Board of Internal Medicine Sub-certificate in Cardiovascular Disease (Internal Medicine)

Resumes & CV records

Resumes

Edward Lakatta Photo 15

Edward Nihniairp Lakatta

Edward Lakatta Photo 16

Edward Lakatta

Publications & IP owners

Us Patents

Nucleic Acid Modules For Expression And Tagging Of Membrane Proteins And Methods Of Use

US Patent:
8501925, Aug 6, 2013
Filed:
Jan 5, 2010
Appl. No.:
12/652395
Inventors:
Li Lin - Baltimore MD, US
John Pang - Baltimore MD, US
Wen Wei - Cockeysville MD, US
Edward G. Lakatta - Bel Air MD, US
Assignee:
The United States of America, as represented by the Secretary, Department of Health and Human Resources - Washington DC
International Classification:
C07H 21/04
C12Q 1/68
US Classification:
536 235, 435 61
Abstract:
Described herein are nucleic acid modules for cloning, expression and tagging of eukaryotic membrane proteins. The nucleic acid modules include a receptor for advanced glycation end products (RAGE) signal sequence, a nucleic acid sequence encoding a tag and a multiple cloning sequence (MCS). Any membrane protein of interest can be cloned into the MCS for expression in cells. The nucleic acid modules can encode any type of tag, such as an epitope tag or affinity tag. The nucleic acid modules disclosed herein can be used to express any type of membrane protein and are particularly suited to the expression and tagging of Type I and Type III membrane proteins.

Anti-Marinobufagenin Antibodies And Methods For Their Use

US Patent:
2010015, Jun 24, 2010
Filed:
Jun 26, 2006
Appl. No.:
11/993309
Inventors:
Alexei Bagrov - Cockeysville MD, US
Olga V. Fedorova - Lutherville MD, US
Edward G. Lakatta - Bel Air MD, US
Andrey Simbirtsev - St. Petersburg, RU
Alexander Kotov - St. Petersburg, RU
Nikolai Kolodkin - St. Petersburg, RU
International Classification:
C07K 16/18
C12N 5/16
C07K 16/46
G01N 33/566
A61K 39/395
A61P 9/00
A61P 9/12
A61P 9/10
US Classification:
4241331, 435346, 5303881, 5303913, 436501, 4241411, 5303873
Abstract:
Described herein are deposited hybridoma cell lines and the monoclonal antibodies produced by these hybridomas, and antigen binding fragments thereof. These monoclonal antibodies and antigen binding fragments specifically bind marinobufagenin. The disclosure also encompasses the use of these monoclonal antibodies or antigen binding fragments in a method for detecting the presence of marinobufagenin in a biological sample. Also provided are methods for the use of these monoclonal antibodies or antigen binding fragments as prophylactic, therapeutic, and diagnostic agents for the detection, inhibition and treatment of a cardiovascular disease, for example, essential hypertension, hypertension associated with preeclampsia, eclampsia, or renal failure, or myocardial fibrosis in a subject.

Methods For The Detection Of Advanced Glycation Endproducts And Markers For Disease

US Patent:
2011031, Dec 29, 2011
Filed:
Jun 30, 2009
Appl. No.:
13/002106
Inventors:
Richard David Semba - Baltimore MD, US
Luigi Ferruci - Baltimore MD, US
Edward G. Lakatta - Bethesda MD, US
Assignee:
THE JOHNS HOPKINS UNIVERSITY - Baltimore MD
International Classification:
A61K 47/40
G01N 33/566
A61K 47/16
A61K 47/42
A61P 3/10
A61K 47/14
A61K 47/02
A61K 47/04
A61P 13/12
A61P 9/10
G01N 33/53
A61K 47/38
US Classification:
514770, 435 792, 436501, 435 721, 514773, 514776, 514781, 514785, 514769
Abstract:
The present invention provides compositions and methods for detecting carboxymethyl-lysine (CML) and circulating receptor for advanced glycation end (RAGE) products, and methods for correlating CML and RAGE levels with age-related disease, hi particular, serum CML and/or circulating receptor for advanced glycation end (RAGE) products can be used as a clinical biomarker in diagnostics to identify people who are at a higher risk of developing adverse ageing-related outcomes.

Method For The Diagnosis Of Age-Associated Vascular Disorders

US Patent:
2012000, Jan 5, 2012
Filed:
Feb 19, 2010
Appl. No.:
13/202319
Inventors:
Mingyi Wang - Baltimore MD, US
Zongming Fu - Baltimore MD, US
Edward G. Lakatta - Bel Air MD, US
Jennifer Van Eyk - Baltimore MD, US
International Classification:
C40B 30/04
G01N 33/53
G01N 27/447
C12Q 1/68
US Classification:
506 9, 435 61, 435 71, 435 612, 204456, 204451
Abstract:
Methods for determining if a subject has or is susceptible to having an age-associated vascular disorder are disclosed. The method includes determining if the subject exhibits altered expression of a product of one or more of the genes listed in Table 1 relative to a control level of expression of the gene product. Altered expression of one or more of the genes listed in Table 1 indicates that the subject has or is susceptible to having an age-associated vascular disorder. In specific examples the gene product is a product of the MFG-E8 and an increase in expression indicates the subject has or is susceptible to having an age-associated vascular disorder.

Engineered Biological Pacemakers

US Patent:
2012013, May 31, 2012
Filed:
May 21, 2010
Appl. No.:
13/322066
Inventors:
Victor Maltsev - Parkville MD, US
Edward G. Lakatta - Bel Air MD, US
Syevda Sirenko - Baltimore MD, US
Maxim Milkheev - Clairton PA, US
Yoram Vodovotz - Sewickley PA, US
Assignee:
The United States of America, as represented by the Secretary, Dept. of Health and Human Services - Bethesda
International Classification:
A61K 35/34
A61P 9/06
C12N 5/10
US Classification:
424 9321, 435325
Abstract:
Biological pacemakers engineered to intrinsically generate rhythmic excitations are disclosed. In addition, methods of producing the biological pacemakers are disclosed. Methods of treating or preventing arrhythmia and heart disease associated with a defective pacemakers are also disclosed.

Human Soluble Receptor For Advanced Glycation End Products (Srage), Methods Of Preparing Human Srage, And Treatment Methods Using Srage

US Patent:
2015005, Feb 19, 2015
Filed:
Jan 3, 2013
Appl. No.:
14/368374
Inventors:
- Bethesda MD, US
Sungha Park - Seoul, KR
Wen Wei - Cockeysville MD, US
Rui-Ping Xiao - Baltimore MD, US
Mark I. Talan - Baltimore MD, US
Edward G. Lakatta - Bel Air MD, US
International Classification:
C07K 14/705
US Classification:
514 19, 514 212, 536 231, 435 691, 4353201, 435325
Abstract:
The present disclosure provides a method for recombinant production of human sRAGE in mammalian cells, as well as a human sRAGE having a mammalian post-translational modification and compositions thereof. The present disclosure also provides a method of treating a vascular disease, injury, or inflammation in a mammal by administering to a mammal with a vascular disease, injury, or inflammation a composition comprising human sRAGE having a mammalian post-translational modification, thereby treating the vascular disease, injury, or inflammation in the mammal.

Methods For The Detection Of Advanced Glycation Endproducts And Markers For Disease

US Patent:
2015005, Feb 19, 2015
Filed:
Apr 10, 2014
Appl. No.:
14/249451
Inventors:
- Baltimore MD, US
Luigi Ferruci - Baltimore MD, US
Edward G. Lakatta - Bethesda MD, US
Assignee:
THE JOHNS HOPKINS UNIVERSITY - Baltimore MD
International Classification:
G01N 33/53
A61K 31/426
A61K 31/60
A61K 31/40
A61K 31/498
A61K 31/496
A61K 31/155
A61K 38/05
US Classification:
514 2191, 514634, 514365, 514424, 514250, 514369, 51425213, 514165, 435 792
Abstract:
The present invention provides compositions and methods for detecting carboxymethyl-lysine (CML) and circulating receptor for advanced glycation end (RAGE) products, and methods for correlating CML and RAGE levels with age-related disease. In particular, serum CML and/or circulating receptor for advanced glycation end (RAGE) products can be used as a clinical biomarker in diagnostics to identify people who are at a higher risk of developing adverse ageing-related outcomes.

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