Inactivation of bcl-2 Results in Progressive Degeneration of Motoneurons, Sympathetic and Sensory Neurons during Early Postnatal Development

Michaelidis, Theologos M.; Sendtner, Michael; Cooper, Jonathan D.; Airaksinen, Matti S.; Holtmann, Bettina; Meyer, Michaël; Thoenen, H.

doi:10.1016/s0896-6273(00)80282-2

Cited by 255 publications

(165 citation statements)

References 85 publications

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“…Furthermore, a simple down-regulation of a single receptor cannot account for the change because postnatal RGCs fail to rapidly extend axons in response to all tested axon growth-promoting stimuli and substrates. The anti-apoptotic protein Bcl-2 was proposed as an intrinsic genetic switch that decreases axon growth rate by RGCs (Chen et al 1997), but Bcl-2 overexpression by purified RGCs in culture neither promotes axon growth nor enhances axon growth in response to neurotrophic signaling in vitro or in vivo (Goldberg et al 2002b), a result consistent with other findings (Greenlund et al 1995;Michaelidis et al 1996;Chierzi et al 1999;Goldberg and Barres 2000;Lodovichi et al 2001).…”

Section: What Molecular Changes Underlie the Developmental Loss In Rasupporting

confidence: 70%

How does an axon grow?

Goldberg¹

2003

Genes Dev.

204

139

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How do axons grow during development, and why do they fail to regrow when injured? In the complicated mesh of our nervous system, the axon is the information superhighway, carrying all of the data we use to sense our environment and carry out behaviors. To wire up our nervous system properly, neurons must elongate their axons during development to reach their targets. This is no simple task, however. The complex morphology of axons and dendrites puts neurons among the most intricate and beautiful cells in the body. Knowledge of how neurons extend axons and dendrites, elongate at a particular rate, and stop growing at the proper time is critical to understanding the development of our nervous system, yet the regulation of these processes is poorly understood. Considerable attention in recent years has focused on understanding how growth cones are guided and steered through complicated pathways (for review, see Schmidt and Hall 1998;Mueller 1999), and even how neurons initiate new processes (for review, see Da Silva and Dotti 2002), but what mechanisms are involved in elongation itself? Are environmental signals needed to drive axon growth and, if so, what are the intracellular molecular mechanisms by which they induce elongation? What controls the rate of axon growth? How do CNS neurons know whether to extend axons or dendrites? Is the signaling of axon versus dendrite growth attributable to different extracellular signals, different neuronal states, or both? All of these questions bear critically on our understanding of axon growth and here I review recent answers and approaches to the above questions, and highlight their relevance during development, injury, and disease.

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Section: What Molecular Changes Underlie the Developmental Loss In Rasupporting

confidence: 70%

How does an axon grow?

Goldberg¹

2003

Genes Dev.

204

139

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“…Whether Beclin-1 can be manipulated to enhance the death of cancer cells expressing high amounts of Bcl-2 needs to be tested. It will be equally important to assess whether Beclin-1 disturbs the pro-survival effect of Bcl-2 in the nervous system, given that some classes of neurons depend on Bcl-2 for long-term survival (Michaelidis et al, 1996).…”

Section: Discussionmentioning

confidence: 99%

Bcl-2 complexed with Beclin-1 maintains full anti-apoptotic function

et al. 2009

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The binding of Bcl-2 to Beclin-1 reduces Beclin-1's capacity to induce autophagy. Here, we have tested whether the interaction is reciprocated by loss of Bcl-2's anti-apoptotic function. We targeted Bcl-2 to mitochondria or endoplasmic reticulum (ER) and induced apoptosis using several apoptotic stimuli that initiate ER and/or mitochondrial signaling pathways (UV radiation, TNF and cycloheximide, staurosporine, thapsigargin and tunicamycin). When Beclin-1 and Bcl-2 were expressed together in HeLa cells, Beclin-1 (but not Beclin-1 lacking the Bcl-2-binding domain) followed Bcl-2 to the appropriate organelle with complete or near-complete overlap (comprising 60 and 30% of cells, respectively). The interaction between Beclin-1 and Bcl-2 was verified by immunoprecipitation, and a membrane-proximate localization of Beclin-1 was shown by immunoelectron microscopy. Apoptosis was followed by measuring changes in nuclear morphology, caspase-3 activity, poly-ADP-ribose polymerase cleavage or punctation of mRFP-Bax on mitochondria. Binding of Beclin-1 to Bcl-2 did not modify apoptosis irrespective of Bcl-2 concentration, location or apoptotic stimulus. A similar result was obtained in Atg5À/À cells that are autophagy-deficient, arguing against compensation for the loss of protection by Bcl-2 by autophagy-mediated survival induced by Beclin-1. Hence, although Beclin-1 contains a BH3-only motif typical of pro-apoptotic proteins, it is a negligible modulator of Bcl-2's anti-apoptotic function.

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“…Homologous recombination (Table 2) revealed that Bcl-2 de®ciency is deleterious for certain cell types including lymphocytes (Nakayama et al, 1994), melanocytes (Yamamura et al, 1996), intestinal epithelial cells (Kamada et al, 1995), and some classes of neurons (Michaelidis et al, 1996). De®ciency of Bcl-X causes intrauterine death accompanied by massive loss of postmitotic immature neurons (Motoyama et al, 1995).…”

Section: Knock-out Studiesmentioning

confidence: 99%

“…Thus, a swap of a 23 aminoacid segment surrounding BH3 from Bax into Bcl-2 converted Bcl-2 from a death antagonist to a death agonist . (Nakayama et al, 1994) Lymphopenia (Nakayama et al, 1994) Accelerated G1-S cell cycle progression in T cells (Linette et al, 1996) Multicystic kidney, renal hypoplasia and renal failure (Nakayama et al, 1994;Sorenson et al, 1996) Gray hair due to accelerated loss of melanocytes (Yamamura et al, 1996) Decrease in the number of oocytes and primordial follicles (Ratts et al, 1995) Distorted small intestine with accelerated exfoliation of epithelial cells (Kamada et al, 1995) Degeneration of motoneurons, sympathetic, and sensory neurons during early postnatal development (Michaelidis et al, 1996) Enhanced susceptibility of cerebellar granule neurons to undergo apoptosis in vitro (Tanabe et al, 1997) Reduced axon growth rate in embryonic sensory neurons culutured in vitro (Hilton et al, 1997) Bcl-X Intrauterine death (E13) (Motoyama et al, 1995) Massive death of postmitotic immature neurons (Motoyama et al, 1995) Shortened life-span of immature lymphocytes (Motoyama et al, 1995) Enhanced death of serum-depleted telencephalic cells in vitro Bxl-w Sterility with progressive testicular degeneration, blockade in late spermiogenesis (Ross et al, 1998) (Deckwerth et al, 1996) More neurons in cervical ganglia and facial nuclei (Deckwerth et al, 1996) Prevents increased cell death of immature neurons in Bcl-X 7/7 mice (Shindler et al, 1997) Asymmetric receptor/ligand interactions among members of the Bcl-2 family Mutagenesis studies and NMR data revealed that intact BH1, BH2 and BH3 domains of the antagonists (Bcl-2, Bcl-X L ) are required for them to heterodimerize with the BH3 domain of Bak or Bax and to repress cell death (Sattler et al, 1997;Sedlak et al, 1995;Ying et al, 1994). It appears that the BH3 region forms and a helix which nestles into a crevice formed by the apposition of the BH1, BH2 and BH3 regions (Sattler et al, 1997).…”

Section: Bcl-2 Homology Regionsmentioning

confidence: 99%

Subcellular and submitochondrial mode of action of Bcl-2-like oncoproteins

et al. 1998

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Bcl-2 is the prototype of a class of oncogenes which regulates apoptosis. Bcl-2-related gene products with either death-promoting and death-inhibitory activity are critically involved in numerous disease states and thus constitute prime targets for therapeutic interventions. The relative amount of death agonists and antagonists from the Bcl-2 family constitutes a regulatory rheostat whose function is determined, at least in part, by selective protein-protein interactions. Bcl-2 and its homologs insert into intracellular membranes including mitochondria, the endoplasmatic reticulum and the nuclear envelope. Many of the molecular genetic, ultrastructural, crystallographic and functional studies suggest that Bcl-2-related molecules exert their apoptosis-regulatory e ects via regulating mitochondrial alterations preceding the activation of apoptogenic proteases and nucleases. Via a direct e ect on mitochondrial membranes, Bcl-2 prevents all hallmarks of the early stage of apoptosis including disruption of the inner mitochondrial transmembrane potential and the release of apoptogenic protease activators from mitochondria. The mitochondrial permeability transition (PT) pore, also called mitochondrial megachannel or multiple conductance channel, is a multiprotein complex formed at the contact site between the mitochondrial inner and outer membranes, exactly at the same localization at which Bax, Bcl-2, and Bcl-X L are particularly abundant. The PT pore participates in the regulation of matrix Ca 2+ , pH, DC m , and volume and functions as a Ca 2+ -, voltage-, pH-, and redox-gated channel with several levels of conductance and little if any ion selectivity. Experiments involving the puri®ed PT pore complex indicate that Bax, Bcl-2, and Bcl-X L exert at least part of their apoptosis-regulatory function by facilitating (Bax) or inhibiting (Bcl-2, Bcl-X L ) PT pore opening. These ®ndings clarify the principal (but not exclusive) mechanism of Bcl-2-mediated cytoprotection.

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Inactivation of bcl-2 Results in Progressive Degeneration of Motoneurons, Sympathetic and Sensory Neurons during Early Postnatal Development

Cited by 255 publications

References 85 publications

How does an axon grow?

How does an axon grow?

Bcl-2 complexed with Beclin-1 maintains full anti-apoptotic function

Subcellular and submitochondrial mode of action of Bcl-2-like oncoproteins

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