Abstract

Brain injury in premature is an important clinical problem due to the increasing number of surviving premature infants and the high incidence of neurodevelopmental handicaps in this population. Disturbances of cerebral blood flow (CBF) and oxygen delivery are thought to be crucial factors in neonatal brain injury. However, the exact mechanisms and timing of injury are not understood. In vivo Near infrared spectroscopy (NIRS) provides a means of direct and continuous bedside monitoring of neonatal cerebral hemodynamics and oxygenation. NIRS may be able to detect alterations of cerebral oxygenation or hemodynamics before injury from cellular energy depletion of this technology in the prevention of newborn brain injury will required further laboratory based and clinical studies. The goal of this proposal is for the PI to become an independent investigator capable of approaching questions in newborn neurology with both laboratory and clinical research tools. To achieve this goal, the PI has established an in-depth program of didactic and research training. In Phase I, the PI will use the response to hypoxia and ischemia in neonatal piglets 1) to characterize changes in brain Hb02 and Hb concentration, 2) to compare NIRS CBV measurements CBF estimations to microsphere measures of CBF, 3) to determine the correlation of NIRS measures of cerebral hemodynamics to magnetic resonance measures cerebral energy state, and 4) to determine the ability of NIRS cerebral blood volume measurements predict loss of cerebrovascular regulation. In phase II, the findings of the animal studies will be applied i a clinical study of premature neonates to examine in control and critically ill neonates 1) regulations of CBF, 2) presence or absence of NIRS changes associated with cerebral energy failure in phase I studies, and 3) differences in the variability of cerebral hemodynamic parameters. These will determine the physiological significance of NIRS with measurements and whether changes in cerebral oxygenation and blood volume thought to be associated with increased risk of brain injury are present in critically ill neonates. The overall program will provide the necessary baseline data, logistics, and training in state-of-the-art in-vivo spectroscopy for the PI to undertake further studies of the relationship between NIRS measurements of altered cerebral hemodynamics nd subsequent brain injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Physician Scientist Award (K11)
Project #
5K11HD001010-02
Application #
2194530
Study Section
Special Emphasis Panel (SRC (TS))
Project Start
1993-12-01
Project End
1995-09-15
Budget Start
1994-12-01
Budget End
1995-09-15
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital Boston
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Lee, Kenneth P K; Dey, Madhusudan; Neculai, Dante et al. (2008) Structure of the dual enzyme Ire1 reveals the basis for catalysis and regulation in nonconventional RNA splicing. Cell 132:89-100
Rice, Sederick C; Vacek, Pamela M; Homans, Alan H et al. (2003) Comparative analysis of HPRT mutant frequency in children with cancer. Environ Mol Mutagen 42:44-9
Finette, Barry A; Kendall, Heather; Vacek, Pamela M (2002) Mutational spectral analysis at the HPRT locus in healthy children. Mutat Res 505:27-41
Yoshioka, M; O'Neill, J P; Vacek, P M et al. (2001) Gestational age and gender-specific in utero V(D)J recombinase-mediated deletions. Cancer Res 61:3432-8
Yoshioka, M; Vacek, P M; Poseno, T et al. (1999) Gender-specific frequency of background somatic mutations at the hypoxanthine phosphoribosyltransferase locus in cord blood T lymphocytes from preterm newborns. Proc Natl Acad Sci U S A 96:586-91
Abramson, L S; Albertini, R J; Pachman, L M et al. (1999) Association among somatic HPRT mutant frequency, peripheral blood T-lymphocyte clonality, and serologic parameters of disease activity in children with juvenile onset dermatomyositis. Clin Immunol 91:61-7
O'Neill, J P; Finette, B A (1998) Transition mutations at CpG dinucleotides are the most frequent in vivo spontaneous single-based substitution mutation in the human HPRT gene. Environ Mol Mutagen 32:188-91
Finette, B A; O'Neill, J P; Vacek, P M et al. (1998) Gene mutations with characteristic deletions in cord blood T lymphocytes associated with passive maternal exposure to tobacco smoke. Nat Med 4:1144-51
Holtzman, D; Mulkern, R; Meyers, R et al. (1998) In vivo phosphocreatine and ATP in piglet cerebral gray and white matter during seizures. Brain Res 783:19-27
Tsuji, M; duPlessis, A; Taylor, G et al. (1998) Near infrared spectroscopy detects cerebral ischemia during hypotension in piglets. Pediatr Res 44:591-5

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