Effects of hypoxia on stress proteins in the piglet heart at birth

Louapre, Pamela; Grongnet, Jean‐François; Tanguay, Robert M.; David, Jean‐Claude

doi:10.1379/csc-74r.1

Cited by 41 publications

(37 citation statements)

References 31 publications

(47 reference statements)

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“…12 ␣B-crystallin expression is up-regulated during in vitro angiogenesis 17 and is increased in heart tissues undergoing hypoxia. 15 We recently showed that after chemical hypoxia, ␣B-crystallin demonstrated an initial increase in expression followed by down-regulation at later time points. 16 These results suggest that the effect of hypoxia on expression of ␣B-crystallin varies in different cell types and types of hypoxia.…”

Section: Discussionmentioning

confidence: 99%

“…13 In addition to being a molecular chaperone, ␣B-crystallin functions in apoptosis inhibition, cellular protection, and proteasomal interactions. 12,14 It was recently shown that ␣B-crystallin expression was modulated by hypoxia 15,16 and regulates tumor angiogenesis 17 ; however, little is known about the mechanistic role of ␣B-crystallin in angiogenesis. The aim of this study was to investigate vascular pathology of ␣B-crystallin Ϫ/Ϫ and wild-type mice in 2 distinct models of intraocular neovascularization, with particular emphasis on VEGF-A mRNA and protein expression.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

αB-crystallin regulation of angiogenesis by modulation of VEGF

Kase

Sonoda

et al. 2010

Blood

143

164

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

αB-crystallin regulation of angiogenesis by modulation of VEGF

Kase

Sonoda

et al. 2010

Blood

143

164

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“…It is worthwhile to mention that expression of different small heat shock protein is tissue-specific and is also dependent on the physiological stage. However, on the average, the levels of HspB1 and HspB5 expression are comparable, exceeding by up two times the level of HspB6 and by up to four times the levels of HspB8, respectively (Kato et al 1992(Kato et al , 1994Louapre et al 2005;Verschuure et al 2003;Huey et al 2004). This fact together with the low probability of subunit exchange makes participation of HspB8 in the formation of heterooligomeric complexes with other small heat shock proteins rather improbable.…”

Section: Discussionmentioning

confidence: 99%

Heterooligomeric complexes of human small heat shock proteins

Mymrikov

Seit-Nebi

Gusev

2012

Cell Stress and Chaperones

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Oligomeric association of human small heat shock proteins HspB1, HspB5, HspB6 and HspB8 was analyzed by means of size-exclusion chromatography, analytical ultracentrifugation and chemical cross-linking. Wild-type HspB1 and Cys mutants of HspB5, HspB6 and HspB8 containing a single Cys residue in position homologous to that of Cys137 of human HspB1 were able to generate heterodimers cross-linked by disulfide bond. Cross-linked heterodimers between HspB1/HspB5, HspB1/ HspB6 and HspB5/HspB6 were easily produced upon mixing, whereas formation of any heterodimers with participation of HspB8 was significantly less efficient. The size of heterooligomers formed by HspB1/HspB6 and HspB5/HspB6 was different from the size of the corresponding homooligomers. Disulfide cross-linked homodimers of small heat shock proteins were unable to participate in heterooligomer formation. Thus, monomers can be involved in subunit exchange leading to heterooligomer formation and restriction of flexibility induced by disulfide cross-linking prevents subunit exchange.

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“…For example, in newborn piglets that have been subjected to hypoxiaischemia in laboratory experiments, modified expression patterns of stress related proteins have been demonstrated in brain, heart and intestines [5][6][7]. Apparently this attributes to clinical signs, varying from www.theriojournal.com delivery of less viable piglets [1,2] and reduced early postnatal vitality [2,3] to decreased growth and survival rates until the age of 10 days [3].…”

Section: Introductionmentioning

confidence: 99%

Umbilical cord clamping in term piglets: A useful model to study perinatal asphyxia?

et al. 2008

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Perinatal asphyxia results in tissue and cellular changes during the reperfusion period and clinical signs like perinatal mortality and decreased vitality at birth in newborn piglets. This study aimed to develop and validate a model of birth asphyxia, mimicking the evolvement of birth asphyxia in natural farrowings by conducting umbilical cord clamping (UCC) in term piglets during caesarean sections under general anaesthesia. In total 23 piglets were subjected to 5-8 min of UCC and 24 piglets served as controls. Acid-base balance values and heart rates measured before UCC remained fairly constant throughout the surgical procedure, indicating nearly identical starting conditions of piglets within and between litters. UCC resulted in a significant, mild, mixed respiratory-metabolic acidosis (pH 7.22, pCO 2 9.8 kPa, BE ecf 2 mmol/L, lactate 6.5 mmol/L; controls: pH 7.31, pCO 2 8.5 kPa, BE ecf 5 mmol/L, lactate 4 mmol/L) at 10 min after birth (defined as simultaneous cutting of the umbilical cord and removal of a plastic bag that had been placed over the head to avoid air intake). Heart rates were significantly decreased during UCC (range: 83-107 beats/min versus 128-134 beats/ min in controls). Rectal temperatures and changes in body weight until 72 h of life were not affected by UCC. Interestingly, four control and seven clamped piglets did not survive as no independent respiration could be attained. Birth weights and duration of UCC of these piglets did not differ significantly from those in surviving control and clamped piglets. In conclusion the mixed respiratory-metabolic acidosis arising in the surviving clamped piglets is not as severe as can be expected in highly asphyxiated, vaginally delivered newborn piglets. Repeatability of the model is compromised by considerable variation in the individual response to UCC. #

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Effects of hypoxia on stress proteins in the piglet heart at birth

Cited by 41 publications

References 31 publications

αB-crystallin regulation of angiogenesis by modulation of VEGF

αB-crystallin regulation of angiogenesis by modulation of VEGF

Heterooligomeric complexes of human small heat shock proteins

Umbilical cord clamping in term piglets: A useful model to study perinatal asphyxia?

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