Cell Therapy
Infographic
Published: June 28, 2023
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Anna MacDonald
Senior Science Editor
Anna is a senior science editor at Technology Networks. She holds a first-class honours degree in biological sciences from the University of East Anglia, before joining Technology Networks she helped organize scientific conferences.
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&
Kate Robinson
Assistant Editor
Kate Robinson is the assistant editor at Technology Networks. She joined the team in 2021 after obtaining a bachelor's degree in biomedical sciences.
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Credit: Technology Networks
Cell therapy involves the transfer of intact, live cells into a patient to help lessen or cure a disease. This is done by either replacing cells lost through disease or promoting the repair response for damaged or diseased tissues.
This infographic explores how cell therapies can be made and the potential diseases that they are, and could be, used to treat.
Download this infographic to discover:
- Methods of production
- Current uses
- The future of cell therapy
The American Society of Gene and Cell Therapy defines cell therapy as the transfer
of intact, live cells into a patient to help lessen or cure a disease. This is done by either
replacing cells lost through disease or promoting the repair response for damaged
or diseased tissues.
In this infographic, we explore how cell therapies can be made and the potential
diseases that they are - and could - be used to treat.
Improvements in cell therapy manufacturing processes are needed to
ensure cell therapies are produced:
• Safely
• Reliably
• Cost-efficiently
The first US approval for a stem cell-based therapy came in 2011, when Hemacord was
approved for hematopoietic progenitor cell transplantation procedures in patients with
diseases that affect the hematopoietic system.
Currently, the only stem cell-based treatments approved by the FDA are for hematopoietic
stem cell transplantation.
At the end of 2022, tabelecleucel (Ebvallo), an autologous T-cell based therapy, was approved
for Epstein-Barr virus-positive posttransplant lymphoproliferative disease (PTLD) in the
EU. PTLD is a potentially fatal complication of solid organ transplantation that results in the
overproduction of lymphocytes.
Worldwide, 60 non-genetically modified cell therapies have been approved for clinical use.
Data obtained from the Gene, Cell and RNA Therapy Landscape Q4 quarterly report by the American Society of Gene
and Cell Therapy.
The majority of cell therapies in development are for either cancer or rare disease indications.
*This is a non-exhaustive list
Sipuleucel-T (2010):
Metastatic castrate-resistant
prostate cancer. (autologous,
activated/expanded)
Azficel-T (2011):
Nasolabial fold wrinkles
in adults. (autologous,
expanded)
Autologous cultured
chondrocytes on a porcine
collagen membrane (2016):
Cartilage defects of the
knee in adults. (autologous,
expanded)
Axicabtagene
ciloleucel (2017):
B-cell non-Hodgkin
lymphoma and follicular
lymphoma. (CAR T-cell
therapy. Autologous,
modified)
Idecabtagene
vicleucel (2021):
Multiple myeloma. (CAR
T-cell therapy. Autologous)
Allogeneic processed
thymus tissue–agdc (2021):
Congenital athymia.
(allogeneic)
Elivaldogene
autotemcel (2022):
Early, active cerebral
adrenoleukodystrophy.
(autologous, modified)
Motor neurons grown from
iPSCs were administered to
mice after their sciatic nerves
were cut. The cells innervated
the muscle and helped to
maintain muscle mass in the
mice compared to mice that
did not receive the cells.
Cografting astrocytes
was shown to enhance
neural progenitor cellbased cell therapeutic
outcomes in a model
of Parkinson’s disease.
Research is underway
to engineer microglia
in a neuroprotective
state to transplant
into ALS patients.
Treatment can be incredibly expensive.
There is risk of serious adverse effects such
as cytokine release syndrome.
The efficacy of CAR T-cell therapy has also been
questioned, with long-term benefits less clear
when compared to alternate therapies.
Reproducing the success seen in hematological
cancers to solid tumors remains a challenge.
HEMACORD (HPC,
Cord Blood) (2011):
Disorders affecting the
hematopoietic system.
(allogeneic)
Allogeneic cultured
keratinocytes and
fibroblasts in bovine
collagen (2012):
Mucogingival conditions in
adults. (allogeneic)
Tisagenlecleucel (2017):
B-cell acute lymphoblastic
leukemia and B-cell nonHodgkin lymphoma. (CAR
T-cell therapy. Autologous,
modified)
Brexucabtagene
autoleucel (2020):
Mantle cell lymphoma and
B-cell acute lymphoblastic
leukemia. (CAR T-cell
therapy. Autologous,
modified)
Lisocabtagene
maraleucel (2021):
B-cell non-Hodgkin
lymphoma. (CAR T-cell
therapy. Autologous)
Ciltacabtagene
autoleucel (2022):
Multiple myeloma. (CAR
T-cell therapy. Autologous)
Allogeneic cultured
keratinocytes and dermal
fibroblasts in murine
collagen- dsat (2021):
Thermal burns. (allogeneic)
Betibeglogene
autotemcel (2022):
ß-thalassemia. (autologous,
modified)
Number of cell therapies in preclinical through pre-registration
stages of development per indication
Cells originating from the patient are classed as autologous. These cells are typically
collected, processed, expanded and then re-injected.
Cells originating from a donor are called allogeneic cells. Allogeneic cells are used to
treat blood disorders and immune system diseases, such as sickle cell anemia.
Instead of using mature cells like T cells, other cell therapy approaches utilize immature
stem cells. These cells are especially suited to regenerative medicine approaches, such
as restoring nerve cells and preventing neurodegeneration.
Stem cells can be grown into different types of nerve cells, such as motor neurons, which
can then be administered to patients.
Alongside gene therapies, cell therapies are increasingly being
investigated for their potential to treat rare diseases.
While a disease is considered rare if it affects fewer than 1 in 2000
people, collectively these diseases affect a significant proportion of the
population – around 300 million people are living with a rare disease.
Ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) is a rare
disease affecting the skin, hair, nails, teeth and other tissues, caused
by a mutation in TP63. Cell therapy approaches are being considered as
a treatment for skin fragility in AEC patients. Such approaches would
involve the following steps:
Interest in and the development
of cell therapies is expected to
continue to grow: The FDA predicts
that it will be approving 10 to 20
cell and gene therapy products a
year by 2025. The global cell and
gene therapy clinical trials market
is projected to reach USD 16,054.93
million by 2030.
However, such approaches are expensive, time-consuming, complex and face
regulatory hurdles.
Of particular interest is the development of advanced CAR T-cell therapies
that present a lower chance of causing severe side effects such as cytokine
release syndrome or are able to recognize two targets on cancer cells,
helping to overcome resistance seen with single-targeted CAR T cells.
Alternative cell types, such as NK cells, could overcome some of the
limitations of relying on T cells. Expressing a variety of unique receptors, NK
cell therapies could offer similar potency without the associated side effects.
Referred to as the “fifth pillar” of cancer treatment, immunotherapy is a growing area
of interest, with promise to transform the treatment of cancer.
Alongside other approaches that harness the immune system, such as monoclonal
antibodies and vaccines, cell therapies are being developed to improve treatment
options for cancer patients.
Six CAR T-cell therapies have been approved by the FDA since 2017, all for the
treatment of blood cancers and targeting CD19 or BCMA antigens on B cells.
The types of cells used for cell therapies fall into one of two categories, stem cells or
somatic cells.
Methods of production
Neurodegeneration
Rare diseases
The future
Cell therapy applications
Current uses
CAR T-cell therapy
FDA approved cell therapies*
Despite the promise, CAR T-cell therapy
is not without limitations:
Autologous vs allogeneic
Cancer
Stem cells vs somatic cells
Pluripotent stem cells: Give rise to
all cell types except extraembryonic
placental cells. These include embryonic
stem cells (ESCs), epiblast stem cells
(EpiSCs), embryonic germ cells (EGCs)
and induced pluripotent stem cells
(iPSCs).
Adult stem cells: Include hematopoietic
stem cells (HSCs), skin stem cells
(SSCs), neural stem cells (NSCs) and
mesenchymal stem cells (MSCs). Are
typically used to replace cells lost to
disease or contribute to the healing of
damaged/diseased cells.
Cancer stem cells: Found within solid
tumors or blood cancers and exhibit
characteristics of both stem cells and
cancer cells. Can be used as a target for
cancer treatments.
Fibroblasts: Produce extracellular
matrix (ECM) and collagen.
Chondrocytes: Maintain the ECM and
produce the cartilage matrix.
Keratinocytes: Major cell type of the
outermost layers of the skin.
Immune cells: T cells, dendritic
cells, natural killer (NK) cells and
macrophages.
350
ANTICANCER
RARE DISEASES
ALIMENTARY/METABOLIC
MUSCULOSKELETAL
NEUROLOGICAL
CARDIOVASCULAR
IMMUNOLOGICAL
RESPIRATORY
SENSORY
DERMATOLOGICAL
MISCELLANEOUS
GENITOURINARY
ANTI-INFECTIVE
BLOOD AND CLOTTING
NA/UNSPECIFIED
HORMONAL
300
250
200
150
100
50
0
Autologous
Human iPSC
Stem cell-based
cell therapy
Allogeneic
Non stem cell-based
cell therapy
Sponsored by:
Cells
collected
Cells re-injected
to patient
Cells
processed
Cells expanded
in the lab
Donor Patient
Pluripotent
stem cells
Adult stem
cells
Fibroblasts Keratinocytes Cancer
stem cells
Immune
cells
Chondrocytes
Stem cells are either
used, or targeted, by the
cell therapy. Examples of
cells used include:
Somatic cells are isolated from
the body (either autologous or
allogenic in nature), expanded
and modified in vitro before
being returned to the body. Cell
types used can include:
• T cells
• Dendritic cells
• Natural killer cells
• Macrophages
Cell therapy utilizes dierent types of cells, typically categorized as:
T cell
T cell
Antigens
CAR T cell
CAR T cell
Insert gene for CAR
Chimeric antigen
receptor (CAR)
T cells are collected from a
patient or donor’s blood.
The CAR T cells recognize and bind to
antigens on cancer cells and kill the
cancer cells
The CAR T cells are grown
in large numbers.
The CAR T cells are administered
back to patients.
The T cells are engineered to express a chimeric antigen
receptor (CAR) that recognizes unique tumor antigens.
Cancer cell
Cancer cell
1
2 3 4
Patient somatic
cells obtained by
skin biopsy or
blood collection.
5
Reprogramming
factors
TP63 mutation corrected
Patient specific iPSCs
generated
Repaired iPSCs
Dierentiation into
keratinocytes.
Transplantation
Sponsored by
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