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Cellular Damage, Repair & Apoptosis - The Rogers Lab at Yale School of Medicine

February 12, 2026

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13832

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  • 00:05DNA pulls our genomic information,
  • 00:07and unfortunately,
  • 00:09it's not inert and it's
  • 00:10subject to damage.
  • 00:13Because we want to be
  • 00:14able to preserve our genomic
  • 00:16information,
  • 00:17cells have evolved this very
  • 00:19intricate system called DNA damage
  • 00:21response.
  • 00:22And there are two main
  • 00:23pathways
  • 00:24that happen within the system,
  • 00:26DNA repair
  • 00:28and apoptosis.
  • 00:30So if a cell has
  • 00:32DNA damage, it can choose
  • 00:34to use many different mechanisms
  • 00:36to repair that damage.
  • 00:38But in cases when there's
  • 00:39so much damage, the cell
  • 00:41might decide it's in their
  • 00:43best interest to activate apoptosis
  • 00:45or in other words, its
  • 00:47own cell death.
  • 00:53My lab is really interested
  • 00:54in trying to understand how
  • 00:56pathways within the DNA damage
  • 00:58response talk to each other.
  • 01:01We have a specific interest
  • 01:03in altered DNA structures.
  • 01:05So DNA, primarily the structure
  • 01:08is a duplex, meaning it
  • 01:09is comprised of two different
  • 01:11strands of DNA.
  • 01:12But under some biological
  • 01:14processes,
  • 01:15cells can actually form altered
  • 01:17structures that are different from
  • 01:18this duplex.
  • 01:20Our lab is focusing on
  • 01:21triplex DNA.
  • 01:22So that means that instead
  • 01:24of having two strands of
  • 01:25DNA, the cell then has
  • 01:26three strands of DNA.
  • 01:28And that three stranded structure
  • 01:30is actually recognized by the
  • 01:32cell as DNA damage. And
  • 01:34we are trying to understand
  • 01:36what proteins involved in repair
  • 01:38actually are also essential for
  • 01:41determining that repair can be
  • 01:43efficient.
  • 01:44We now need to incorporate
  • 01:45and alert
  • 01:47apoptosis
  • 01:48that it needs to step
  • 01:49in in order to preserve
  • 01:50genomic integrity.
  • 01:57My lab is really using
  • 01:59molecular biology and biochemistry
  • 02:01techniques to try and understand
  • 02:03repair proteins.
  • 02:05We use microscopy to look
  • 02:07at these proteins on a
  • 02:08cellular level and to see
  • 02:09where they go within the
  • 02:10cell. We also use those
  • 02:12microscopy techniques to be able
  • 02:14to understand
  • 02:15where the DNA damage is,
  • 02:17how the damage is getting
  • 02:18repaired
  • 02:19and we look at this
  • 02:20in many different cancer cell
  • 02:22lines, in many different cancer
  • 02:23types. In particular, my lab
  • 02:25is interested
  • 02:26in breast cancer and ovarian
  • 02:28cancer.
  • 02:30In addition to looking at
  • 02:31things on a microscopic level,
  • 02:33we're also interested in looking
  • 02:35at things from a genomic
  • 02:36level. So we do bulk
  • 02:38RNA sequencing and looking at
  • 02:40different genomic techniques so that
  • 02:42we can actually see where
  • 02:43in the genome across the
  • 02:45whole entire cell is this
  • 02:46damage happening.
  • 02:52There are several different types
  • 02:54of cancers, and one type
  • 02:56of cancer are cancers that
  • 02:57have gene amplification.
  • 02:59And so what that means
  • 03:00is that the cell has
  • 03:02determined that in order for
  • 03:03it to grow very aggressively,
  • 03:05it will have multiple copies
  • 03:07of a gene, and that
  • 03:09gene gives it the growth
  • 03:10advantage.
  • 03:11Traditionally,
  • 03:12drug development strategies have been
  • 03:14to target those over expressed
  • 03:16protein products that happen as
  • 03:18a result of the amplified
  • 03:20genes. This has been very
  • 03:21powerful, but it has been
  • 03:23a limiting factor for many
  • 03:24other types of cancers where
  • 03:26small molecule targeting of those
  • 03:28proteins is not effective and
  • 03:30it's not
  • 03:31doable. And so what my
  • 03:32lab has been doing is
  • 03:34to find ways to really
  • 03:35target these cancers on a
  • 03:37genomic level.
  • 03:39We can design these synthetic
  • 03:41oligonucleotide
  • 03:42molecules that bind sequence specifically
  • 03:45to the amplified gene. This
  • 03:47creates a triplet structure.
  • 03:49We know that the triplet
  • 03:50structures, if you have enough
  • 03:51of them formed, can cause
  • 03:53the cell and force the
  • 03:54cancer cell to activate its
  • 03:56own death.
  • 03:57We can use this system
  • 03:59of manipulating DNA repair and
  • 04:01apoptosis
  • 04:02to cause cancer cells to
  • 04:03die.
  • 04:04I think it has far
  • 04:05reaching amplifications
  • 04:07because there are over four
  • 04:08hundred and fifty genes that
  • 04:09are amplified within cancer cells
  • 04:11in more than over fourteen
  • 04:13subtypes of cancer. So this
  • 04:15platform has really broad reaching
  • 04:17applications.