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Dive into the research topics where Ryan Parr is active.

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Featured researches published by Ryan Parr.


Journal of Forensic Sciences | 2010

Integrated DNA and fingerprint analyses in the identification of 60-year-old mummified human remains discovered in an Alaskan glacier.

Odile Loreille; Ryan Parr; Kevin A. McGregor; Colleen M. Fitzpatrick; Chriss Lyon; Dongya Y. Yang; Camilla Speller; Michael R. Grimm; Michael J. Grimm; Jodi A. Irwin; Edward M. Robinson

Abstract:  This report describes the identification of a merchant mariner who perished in 1948 when Northwest Airlines Flight 4422, a DC‐4 carrying 24 seamen and six crew members crashed into Mount Sanford, Alaska. Fifty‐one years later, a human forearm and hand were found close by the wreckage of the plane, prompting identification efforts using DNA and fingerprints. There were significant challenges to both the fingerprint and DNA analyses. The hand was badly desiccated, making fingerprint friction‐ridge detail almost invisible and the remains had been embalmed upon discovery, making DNA amplification difficult. We present the results of an interdisciplinary approach that successfully addressed these challenges and ultimately led to the identification of the remains. These efforts relied on efficient fingerprint rejuvenation and imaging techniques that improved print resolution, as well as new DNA extraction techniques optimized for aggressively embalmed remains.


Forensic Science International-genetics | 2011

Titanic's unknown child: The critical role of the mitochondrial DNA coding region in a re-identification effort

Rebecca S. Just; Odile Loreille; J. Eldon Molto; D. Andrew Merriwether; Scott R. Woodward; Carney Matheson; Jennifer Creed; Stacey E. McGrath; Kimberly Sturk-Andreaggi; Michael D. Coble; Jodi A. Irwin; Alan Ruffman; Ryan Parr

This report describes a re-examination of the remains of a young male child recovered in the Northwest Atlantic following the loss of the Royal Mail Ship Titanic in 1912 and buried as an unknown in Halifax, Nova Scotia shortly thereafter. Following exhumation of the grave in 2001, mitochondrial DNA (mtDNA) hypervariable region 1 sequencing and odontological examination of the extremely limited skeletal remains resulted in the identification of the child as Eino Viljami Panula, a 13-month-old Finnish boy. This paper details recent and more extensive mitochondrial genome analyses that indicate the remains are instead most likely those of an English child, Sidney Leslie Goodwin. The case demonstrates the benefit of targeted mtDNA coding region typing in difficult forensic cases, and highlights the need for entire mtDNA sequence databases appropriate for forensic use.


British Journal of Dermatology | 2010

Real-time polymerase chain reaction analysis of a 3895-bp mitochondrial DNA deletion in epithelial swabs and its use as a quantitative marker for sunlight exposure in human skin

Andrew Harbottle; Jennifer Maki; Brian Reguly; Roy Wittock; Kerry Robinson; Ryan Parr; Mark A. Birch-Machin

Background  The use of mitochondrial DNA (mtDNA) damage as a reliable and highly sensitive biomarker of ultraviolet (UV) radiation exposure in both the dermis and epidermis has now been well developed by our group and others. We have previously identified a 3895‐bp mtDNA deletion which occurred more frequently and to a higher level in usually sun‐exposed skin as opposed to occasionally sun‐exposed skin. This work focused on older‐aged individuals and, in particular, perilesional, histologically normal skin biopsies taken from patients with skin cancer.


BioMed Research International | 2013

Paired Ductal Carcinoma In Situ and Invasive Breast Cancer Lesions in the D-Loop of the Mitochondrial Genome Indicate a Cancerization Field Effect

Maggrah A; Kerry Robinson; Creed Jm; Roy Wittock; Gehman K; Gehman T; Brown H; Andrew Harbottle; Froberg Mk; Klein D; Brian Reguly; Ryan Parr

Alterations in the mitochondrial genome have been chronicled in most solid tumors, including breast cancer. The intent of this paper is to compare and document somatic mitochondrial D-loop mutations in paired samples of ductal carcinoma in situ (DCIS) and invasive breast cancer (IBC) indicating a potential breast ductal epithelial cancerization field effect. Paired samples of these histopathologies were laser-captured microdissected (LCM) from biopsy, lumpectomy, and mastectomy tissues. Blood samples were collected as germplasm control references. For each patient, hypervariable region 1 (HV1) in the D-loop portion of the mitochondrial genome (mtGenome) was sequenced for all 3 clinical samples. Specific parallel somatic heteroplasmic alterations between these histopathologies, particularly at sites 16189, 16223, 16224, 16270, and 16291, suggest the presence of an epithelial, mitochondrial cancerization field effect. These results indicate that further characterization of the mutational pathway of DCIS and IBC may help establish the invasive potential of DCIS. Moreover, this paper indicates that biofluids with low cellularity, such as nipple aspirate fluid and/or ductal lavage, warrant further investigation as early and minimally invasive detection mediums of a cancerization field effect within breast tissue.


Genes | 2017

Complete mitochondrial genome sequencing of a burial from a Romano-Christian cemetery in the Dakhleh Oasis, Egypt: Preliminary indications

J. Eldon Molto; Odile Loreille; Elizabeth K. Mallott; Ripan S. Malhi; Spence Fast; Jennifer Daniels-Higginbotham; Charla Marshall; Ryan Parr

The curse of ancient Egyptian DNA was lifted by a recent study which sequenced the mitochondrial genomes (mtGenome) of 90 ancient Egyptians from the archaeological site of Abusir el-Meleq. Surprisingly, these ancient inhabitants were more closely related to those from the Near East than to contemporary Egyptians. It has been accepted that the timeless highway of the Nile River seeded Egypt with African genetic influence, well before pre-Dynastic times. Here we report on the successful recovery and analysis of the complete mtGenome from a burial recovered from a remote Romano–Christian cemetery, Kellis 2 (K2). K2 serviced the ancient municipality of Kellis, a village located in the Dakhleh Oasis in the southwest desert in Egypt. The data were obtained by high throughput sequencing (HTS) performed independently at two ancient DNA facilities (Armed Forces DNA Identification Laboratory, Dover, DE, USA and Carl R. Woese Institute for Genomic Biology, University of Illinois Urbana-Champaign, Urbana, IL, USA). These efforts produced concordant haplotypes representing a U1a1a haplogroup lineage. This result indicates that Near Eastern maternal influence previously identified at Abusir el-Meleq was also present further south, in ancient Kellis during the Romano–Christian period.


Archive | 2006

Mitochondrial mutations and rearrangements as a diagnostic tool for the detection of sun exposure, prostate cancer and other cancers

Ryan Parr; Robert Thayer; Gabriel Dakubo; Jennifer Maki; Kerry Robinson; Andrea Maggrah; Brian Reguly; Andrew Harbottle; Mark A. Birch-Machin


Experimental Gerontology | 2003

A maternal line study investigating the 4977-bp mitochondrial DNA deletion

Robert Thayer; Roy Wittock; Ryan Parr; Steve Zullo; Mark A. Birch-Machin


Archive | 2008

Methods for Assaying MC1R Variants and Mitochondrial Markers in Skin Samples

Ryan Parr; Mark A. Birch-Machin; Andrew Harbottle; Robert Thayer; Jennifer Creed; Andrea Maggrah; Kerry Robinson; Gabriel Dakubo; Brian Reguly; Katrina Maki


Archive | 2007

3.4 kb mitochondrial DNA deletion for use in the detection of cancer

Ryan Parr; Robert Thayer; Gabriel Dakubo; Jennifer Creed; Kerry Robinson; Andrea Maggrah; Brian Reguly


Journal of Investigative Dermatology: International Investigative Dermatology Meeting | 2008

The use of mitochondrial DNA as a "Biosensor" for UVR induced skin damage: Implications for personalized sun care and effective product formulation

Andrew Harbottle; Mark A. Birch-Machin; Jennifer Maki; Brian Reguly; Gabriel D. Dakubo; C Davies; Ryan Parr

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J. Eldon Molto

University of Western Ontario

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Edward M. Robinson

George Washington University

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