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Lawrence I. Grossman, Ph.D.
Professor
Director

3303 Scott Hall
540 East Canfield
Detroit, MI 48201
Voice: 313-577-5326
FAX: 313-577-5218
l.grossman@wayne.edu

Grossman Lab


Professor and Director (also with Internal Medicine); Ph.D., Yeshiva (Einstein), 1971. Molecular genetics and evolution of the electron transport chain; cytochrome c oxidase; mitochondria and mitochondrial diseases.

Research Interests

My lab studies the molecular genetics and evolution of mitochondrial genes. The genes of the electron transport chain proteins are encoded partly by mitochondrial DNA and partly by nuclear DNA. We have largely focused on the nuclear-encoded subunits, particularly those of cytochrome c oxidase (COX), the terminal enzyme complex of the respiratory chain. The known functions of COX are carried out by the three subunits specified by mitochondrial DNA; the role of the nuclear subunits is only beginning to emerge and includes regulation.

In our focus on the function, regulation, and molecular evolution of the nuclear subunits, we have needed to first establish the players. To that end, we recently discovered three new isoforms of COX, a lung and trachea-specific isoform of subunit IV, a testes-specific isoform of subunit VIb, and a third isoform of subunit VIII. We are currently examining the lung-specific isoform in particular detail, both by studying its transcriptional regulation, especially by hypoxia, to understand its signalling circuitry and interaction with other cellular components, and by examining a recently created mouse null mutant.

Another approach to function we are using is molecular evolution; we have developed the picture that cytochrome c and subunits of complex III and COX that interact with it have undergone a period of accelerated evolution suggestive of positive selection at similar times in an ancestor of modern primates. We believe that this remodeling of the electron transport chain supported the expansion of the energy-consuming enlarged neocortex that was taking place in these primate lineages. We are now seeking to characterize biochemically any modifications in electron transport that resulted. Finally, we are interested in the relation between rapidly evolving genes and human disease.

Selected Publications

T.R. Schmidt, M. Goodman and L.I. Grossman (2002). Amino acid replacement is rapid in primates for the mature polypeptides of COX subunits, but not for their targeting presequences. Gene 286, 13-19.

M. Yu, S.A. Jaradat and L.I. Grossman (2002). Genomic organization and promoter regulation of human cytochrome c oxidase subunit viia heart/muscle isoform (COX7AH). Biochim. Biophys. Acta 1574, 345-353.

Wildman D.E., Grossman L.I., and Goodman M. (2002). Human and chimpanzee functional DNA shows they are more similar to each other than either is to other apes.  In M. Goodman and A.S. Moffat, Eds. Probing Human Origins. Cambridge: American Academy of Arts & Sciences Press, pp. 1-10.

D.E. Wildman, W. Wu, M. Goodman and L.I. Grossman (2002). Episodic positive selection in ape cytochrome c oxidase subunit iv. Mol. Biol. Evol. 19, 1812-1815.

T.R. Schmidt, W. Wu, J.R. Doan, M. Goodman and L.I. Grossman (2003). Retention of a duplicate gene through changes of the subcellular localization signal: a cytochrome c oxidase subunit VIIa-related protein localizes to the Golgi apparatus. J. Mol. Evol. 57, 222-228.

A. Goldberg, T.R. Schmidt, M. Hüttemann, D. Wildman, M. Weiss, M. Goodman and L.I. Grossman (2003). Adaptive evolution of cytochrome c oxidase subunit viii in anthropoid primates. Proc. Natl. Acad. Sci. USA 100, 5873-5878.

M. Hüttemann, S. Jaradat and L.I. Grossman (2003). Cytochrome c oxidase of mammals contains a testes-specific isoform of subunit VIb-the counterpart to testes-specific cytochrome c?. Molec. Repro. Dev. 66, 8-16.

M. Hüttemann, T.R. Schmidt and L.I. Grossman (2003). A third isoform of cytochrome c oxidase subunit VIII is present in mammals. Gene 312, 95-102.

D.E. Wildman, M. Uddin, G. Liu, L.I. Grossman and M. Goodman (2003). The 99.4% nonsynonymous and 98.4% synonymous sequence identity between chimpanzees and humans: implications for Darwinian selection and for enlarging the genus Homo. Proc. Natl. Acad. Sci. USA 100, 7181-7188.

M. Uddin, D.E. Wildman, G. Liu, W. Xu, R.M. Johnson, P.R. Hof, G. Kapatos, L.I. Grossman and M. Goodman (2004). Sister grouping of chimpanzees and humans as revealed by genome-wide phylogenetic analysis of brain gene expression profiles. Proc. Natl. Acad. Sci. USA 101, 2957-2962.

J.W. Doan, T.R. Schmidt, D.E. Wildman, M. Uddin, A. Goldberg, M. Hüttemann, M. Goodman, M.L. Weiss and L.I. Grossman (2004). Coevolution of a multiprotein complex: cytochrome c oxidase subunits show accelerated rates of nonsynonymous substitution in anthropoid primates. Mol. Phylogenet Evol. 33, 944-950.

L.I. Grossman, D.E. Wildman, T.R. Schmidt and M. Goodman (2004). Accelerated evolution of the electron transport chain in anthropoid primates. Trends Genet. 20 , 579-585.

J.W. Doan, T.R. Schmidt, D.E. Wildman, M Goodman, M.L. Weiss and L.I. Grossman (2005). Rapid nonsynonymous evolution of the iron sulfur protein in anthropoid primates. J. Bioenerg. Biomembr., in press.

I. Lee, A.R. Salomon, S. Ficarro, I. Mathes, F. Lottspeich, L.I. Grossman, and M. Hüttemann (2005). cAMP-dependent tyrosine phosphorylation of subunit I inhibits cytochrome c oxidase activity. J. Biol. Chem., in press.

 

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Lab members (Fall 2003), from left: Larry Grossman, Monica Uddin, Ick Soo Lee, Maik Hüttemann, Tim Schmidt, Derek Wildman, Jeff Doan

Grossman Lab


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