Leslie Spikes
University of Kansas
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Publication
Featured researches published by Leslie Spikes.
American Journal of Respiratory and Critical Care Medicine | 2012
Leslie Spikes; Pranjali Dalvi; Ossama Tawfik; Haihua Gu; Norbert F. Voelkel; Paul Cheney; Amy O’Brien-Ladner; Navneet K. Dhillon
RATIONALE HIV-associated pulmonary arterial hypertension (PAH) is likely a more prevalent noninfectious complication of AIDS than previously recognized. Furthermore, the majority of HIV-PAH cases occur in individuals with a history of intravenous drug use. In this study we used a simian immunodeficiency (SIV) macaque model and a primary cell-culture system to investigate the association between drug abuse and HIV infection in HIV-PAH development. METHODS The archival lung tissues from macaques previously used to study the effect of morphine on SIV infection-associated neuropathogenesis were analyzed for pulmonary vascular changes. The direct effect of HIV proteins and illicit drugs was investigated on oxidative stress, survival, and proliferation of human pulmonary microvascular endothelial cells. MEASUREMENTS AND MAIN RESULTS SIVmacR71/17E-infected rhesus macaques treated with morphine (VM group) demonstrated significant pulmonary vascular remodeling, including the presence of early and advanced complex (plexiform) lesions, when compared with either the SIV-infected (V group) or morphine-treated uninfected (M group) macaques. However, both the V (two of five) and VM (two of six) groups included some animals with Pneumocystis jirovecii pneumonia. The endothelial cells lining the vessels with medial hypertrophy or initial-stage intimal lesions in lung sections from VM macaques demonstrated an increase in positivity for both terminal dUTP nick-end labeling and Ki67. Oxidative stress-mediated enhanced apoptosis followed by enhanced proliferation of endothelial cells was observed on simultaneous treatment with viral proteins and drugs of abuse compared with either treatment alone. CONCLUSIONS Our findings suggest that SIV/HIV protein(s) and morphine interact to cause the proliferation of apoptosis-resistant endothelial cells leading to angio-obliteration.
Infectious Disease Clinics of North America | 2010
Steven Q. Simpson; Leslie Spikes; Saurin Patel; Ibrahim Faruqi
Hantavirus pulmonary syndrome, also known as hantavirus cardiopulmonary syndrome, is a recently described infectious syndrome found throughout the Americas. Although infection is sporadic and uncommon compared with other atypical pneumonia syndromes, its high mortality rate warrants the maintenance of a high index of suspicion in rural settings. Because no specific therapies are available for the disease, prevention and early recognition play an important role in reducing mortality from the disease. This article reviews the nature of the viruses that cause hantavirus pulmonary syndrome, the epidemiology and ecology of disease transmission, and disease recognition, treatment, and prevention.
American Journal of Respiratory Cell and Molecular Biology | 2016
Pranjali Dalvi; Leslie Spikes; Julie Allen; Vijayalaxmi G. Gupta; Himanshu Sharma; Marion Gillcrist; Jamison Montes de Oca; Amy O’Brien-Ladner; Navneet K. Dhillon
Human immunodeficiency virus (HIV)-related pulmonary arterial hypertension has been found to be more prevalent in intravenous drug users. Our earlier cell-culture findings reported down-regulation of bone morphogenetic protein receptors (BMPRs) in combination with enhanced proliferation of human pulmonary arterial smooth muscle cells (PASMCs) in the presence of HIV-Trans-activator of transcription (Tat) and cocaine compared with either treatment alone. Here, we report physiologic evidence of significant increases in mean pulmonary arterial pressure in HIV-transgenic (Tg) rats intraperitoneally administered 40 mg/kg body weight cocaine (HIV-cocaine group) once daily for 21 days when compared with HIV-Tg rats given saline (HIV group) or wild-type (WT) Fischer 334 rats treated with (WT-cocaine group) and without cocaine (WT group). In addition, right ventricle systolic pressure was also found to be significantly higher in the HIV-cocaine rats compared with the WT group. Significant down-regulation in protein expression of BMPR-2 and BMPR-1B was observed in total lung extract from HIV-cocaine rats compared with the other three groups. Furthermore, the PASMCs isolated from HIV-cocaine rats demonstrated a higher level of proliferation and lower levels of apoptosis compared with cells isolated from other rat groups. Interestingly, corroborating our earlier cell-culture findings, we observed higher expression of BMPR-2 and BMPR-1B messenger RNA and significantly lower levels of BMPR-2 and BMPR-1B protein in HIV-cocaine PASMCs compared with cells isolated from all other groups. In conclusion, our findings support an additive effect of cocaine and HIV on smooth muscle dysfunction, resulting in enhanced pulmonary vascular remodeling with associated elevation of mean pulmonary arterial pressure and right ventricle systolic pressure in HIV-Tg rats exposed to cocaine.
Chest | 2016
Allison M. Aripoli; Lucas Meek; Steven Lemons; Leslie Spikes
A 29-year-old woman presented with a 1-week history of fever, weakness, anorexia, darkened urine, and mild cough. The patient described her cough as nonproductive and without hemoptysis. She had no chest pain. The patients medical history was significant for x-linked hypophosphatemia, renal stones, migraine headaches, and chronic back pain managed on prescribed oral opiates for some time. She reported regular cigarette smoking, but denied illicit or IV drug use or any recent travel or sick contacts. The patient also had no known pertinent family history.
Journal of the American College of Cardiology | 2012
Madhu Reddy; Hemant Boolani; Sowjanya Duthuluru; Namratha Reddy; Timothy Williamson; Leslie Spikes; Sudharani Bommana; Donita Atkins; Vineela Chikkam; Jayasree Pillarisetti; Loren Berenbom; Raghuveer Dendi; Martin Emert; Rhean Linette Pimentel; Dhanunjaya Lakkireddy
Pulmonary hypertension is associated with significant changes in the right heart. The safety of performing Implantable Cardiac Defibrillator (ICD) implantation in these patients is not well evaluated. We performed a retrospective analysis of all consecutive patients who had a clinical diagnosis of
american thoracic society international conference | 2012
Leslie Spikes; Haihua Gu; Pranjali Dalvi; Paul Cheney; Amy O'Brien-Ladner; Navneet K. Dhillon
Chest | 2015
Brietta Forbes; Sonia Castillo; Lewis Satterwhite; Leslie Spikes; Timothy Williamson
american thoracic society international conference | 2012
Krishna V. Rangarajan; Samantha Evans; Jennifer McNiel; Leslie Spikes; Lewis Satterwhite; Timothy Williamson
american thoracic society international conference | 2012
Krishna V. Rangarajan; Jocelyn Havener; Amy Heidenreich; Emily Smiley; Lewis Satterwhite; Leslie Spikes; Timothy Williamson
Journal of the American College of Cardiology | 2012
Hemant Boolani; Madhu Reddy; Sowjanya Duthuluru; Timothy Williamson; Leslie Spikes; Namratha Reddy; Sudharani Bommana; Donita Atkins; Jayasree Pillarisetti; Buddhadeb Dawn; Jayant Nath; Dhanunjaya Lakkireddy