Osteopetrosis in mice lacking NF-κB1 and NF-κB2

Abstract: The nfkb1 and nfkb2 genes encode closely related products regulating immune and inflammatory responses. Their role during development and differentiation remains unclear. The generation of nfkb1 null mice (p50-/-) resulted in altered immune responses, but had no effect on development. Similarly, nfkb2 knockout mice (p52-/-) did not show developmental defects (J.C. et al., manuscript submitted). We have investigated the potential for in vivo compensatory functions of these genes by generating double-knockout mi… Show more

“…Bone remodeling is dependent on bone resorption by myeloid lineage-derived osteoclasts. Although osteoclast numbers are markedly reduced in these double mutant mice and nfkb1 7/7 nfkb2 7/7 osteoclast progenitors cannot di erentiate in vitro , transplantation of normal marrow into newborn nfkb1 7/7 nfkb2 7/7 mice only partially rescues this osteopetrotic phenotype (Franzoso et al, 1997;Iotsova et al, 1997). This indicates that the combined de®ciency of nfkb1 and nfkb2 a icts cells of a hemopoietic origin and the bone marrow microenvironment.…”

“…Indeed, mice lacking multiple Rel/NF-kB proteins often exhibit novel phenotypes or more severe versions of those phenotypes seen in single mutants. nfbk1 7/7 nfkb2 7/7 mice Mice de®cient in both nfkb1 and nfkb2, while phenotypically indistinguishable from control litter mates at birth, soon exhibit growth retardation and cranofacial abnormalities, the latter being a result of bone thickening due to osteopetrosis (Franzoso et al, 1997;Iotsova et al, 1997). Bone remodeling is dependent on bone resorption by myeloid lineage-derived osteoclasts.…”

Genetic approaches in mice to understand Rel/NF-κB and IκB function: transgenics and knockouts

“…Bone remodeling is dependent on bone resorption by myeloid lineage-derived osteoclasts. Although osteoclast numbers are markedly reduced in these double mutant mice and nfkb1 7/7 nfkb2 7/7 osteoclast progenitors cannot di erentiate in vitro , transplantation of normal marrow into newborn nfkb1 7/7 nfkb2 7/7 mice only partially rescues this osteopetrotic phenotype (Franzoso et al, 1997;Iotsova et al, 1997). This indicates that the combined de®ciency of nfkb1 and nfkb2 a icts cells of a hemopoietic origin and the bone marrow microenvironment.…”

“…Indeed, mice lacking multiple Rel/NF-kB proteins often exhibit novel phenotypes or more severe versions of those phenotypes seen in single mutants. nfbk1 7/7 nfkb2 7/7 mice Mice de®cient in both nfkb1 and nfkb2, while phenotypically indistinguishable from control litter mates at birth, soon exhibit growth retardation and cranofacial abnormalities, the latter being a result of bone thickening due to osteopetrosis (Franzoso et al, 1997;Iotsova et al, 1997). Bone remodeling is dependent on bone resorption by myeloid lineage-derived osteoclasts.…”

Genetic approaches in mice to understand Rel/NF-κB and IκB function: transgenics and knockouts

“…NF-κB is a transcription factor essential for osteoclast development [71,72]. In resting cells, inactive NF-κB resides in the cytoplasm and upon activation translocates to the nucleus where it regulates transcription of a variety of genes involved in cell proliferation, apoptosis, and inflammation [73,74].…”

Expression, signaling, and function of P2X7 receptors in bone

“…To address whether failure of osteoclast formation is due to defects in accessory cells (osteoblast/stromal cells) or cells of the osteoclast lineage (Yoshida et al 1990;Soriano et al 1991;Grigoriadis et al 1994;Franzoso et al 1997;Iotsova et al 1997), we have performed in vitro culture experiments. Primary osteoblasts, derived from calvariae of newborn normal ddY mice were cocultured with splenocytes either from TRAF6 ¹/¹ mice or their normal littermates.…”

Severe osteopetrosis, defective interleukin‐1 signalling and lymph node organogenesis in TRAF6‐deficient mice