Figure 3.
Figure 3. Model for the multistep molecular pathogenesis of MM. Two largely nonoverlapping pathways (Ig translocations vs multiple trisomies) are primary events associated with dysregulated cyclin D expression. The most common secondary genetic events associated with tumor progression are shown, including early and late dysregulation of MYC and late-inactivating mutations of p53.

Model for the multistep molecular pathogenesis of MM. Two largely nonoverlapping pathways (Ig translocations vs multiple trisomies) are primary events associated with dysregulated cyclin D expression. The most common secondary genetic events associated with tumor progression are shown, including early and late dysregulation of MYC and late-inactivating mutations of p53.

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