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Iraq - Erbil 2013
Marwan	Alhalabi MD	PhD
Professor	in	Reproductive	Medicine	
Faculty	of	Medicine	
Damascus	University
And
Medical	Director	
Orient	Hospital	
Assisted	Reproduction	Center	
Damascus	– Syria
Andalus University	2015
1 – THE RIGHT GROWTH FACTORS
2 – THE RIGHT RECEPTORS
3 – THE RIGHT NUTRIENTS
• Plasticity,	ability	to	differentiate	
• Ability	to	divide	continuously
• Immunological	immaturity
“Self
renewal”
“Stem cell”
“Progenitor cell”
“TA cells”
“Differentiated cells”
Differentiation
Pluripotency
REPROGRAMMINGDEPROGRAMMING
CREATE THE
FIRST iPS
(2007)
8
MELTON
YAMANAKA
AUGUST 2008
BETA CELL NOT PRODUCING INSULIN
TO ONE THAT PRODUCES INSULIN
** NO STEM CELLS **
REPROGRAMMING
Multipotent
Stem
Cells
Potency
Stem cell type Description Examples
Totipotent
Each cell can develop into a
new individual
Cells from early (1-3
days) embryos
Pluripotent
Cells can form any (212) cell
types
Some cells of
blastocyst (5 to 14
days)
Multipotent
Cells differentiated, but can
form a number of other tissues
Fetal tissue, cord
blood, and adult stem
cells
Unipotent
Cells differentiated, into one
cell lines
Neural Stem cells, etc..
12
Embryo	Splitting
Embryo	Splitting
6-cell	embryo	splitting
• Embryonic	stem	cells
Derived	from	the	blastocyst,	which	
is	a	very	young	embryo	shaped	like	
a	hollow	sphere	that	contains	200-
250	cells	(pre-implantation	
embryos)1
• Adult	stem	cells
Misnomer,	can	be	found	in	children	
and	infants	too
Derived	from	the	umbilical	cord	
and	placenta,	or	from	blood,	bone	
marrow,	skin,	or	other	tissues
ICM
Trophectoderm
ICM	isolation
culture
Feeder	cells
hESC colony
Culture
mechanical passaging Cystic EB formation
7-10 days of culture
Gelatin-coated dishes
(endoderm) (ectoderm) (mesoderm)
Adult	stem	cells	Umbilical	CordIVF	Embryos
Placenta	 Aborted	fetus
• Bone	marrow
• Peripheral	blood	
• Umbilical	cord	blood	
(since	1988)
• Placenta	(LifebankUSA)
• Peripheral	Blood
• Wharton’s	jelly.
• Differentiate	into:	adipocyte,	
chondrocytes,	osteoblasts,	
myocytes,	endothelial	cells,	
hepatic,	and	nervus cells.	
• Role	in	regenerative	medicen.
• >13	folds	in	prolifertion.
• Fibroblast-like.
• Having	immunomodulatory
potential:	Application	in	
treatment	of	autoimmune	
deseases (	Rheumatoid	
arthritic	and	crohn’sdesease
and	Multiple	sclerosis.
The	blood	that	is	left	in	
the	umbilical	cord	and	
placenta	after	the	
delivery	of	the	infant
Garbage
Can
Public
Banking
Private
Banking
Cord	
Blood	
what	to	do	with	it?
Option Advantages Disadvantages
The Garbage can •No cost
•No headaches
•Wasting of valuable
stem cells
Public cord blood
banking
(donation)
•Can be used by anyone in
need
•Increases the pool of HSC
donors
•Increases the pool of
minority donors
•No cost to the donor
•Needs
public/government
financial support
•Not designated for the
donor / family
Private cord blood
collection
•Saved for own use
•Future potential ???
Regenerative use ??
•Cost $$$
•Will probably never be
used
•Socioeconomic disparity
•Reducing public pool
•Professional liability
•Legal/ownership issues
•Safety of use
•Viability, duration of
storage
• Rich	in	hematopoietic	stem	cell.	Pluripotent stem	cell??	
• Younger	cells.		Longer	life	span
• Less	GVHD	when	used	for	allogeniec transplant
• Immediate	easy	availability
• Less	likely	to	be	contaminated	with	viruses.
• 100%	Compatible	graft	for	the	child.
• Not	painful.
• Could	be	used	in	conjunction	with	future	medical	advance.
Stem	Cell	Donor	Registries	Need	Help!
• Both	bone	marrow	and	cord	blood	donors	are	needed	world	
wide.
• Arab	HLA	types	are	severely	under	represented	on	
International	Stem	Cell	Registries.
§ Today	the	world	registries	are	where	UAE	patients	find	
stem	cell	donors.	On	the	International	Registries	Arab	
populations	are	<1%.
Criteria	for	Donor	Eligibility	
1. informed	consent.
2. Absence	of	family	History	of	inherited	diseases	and
negative	history	for	Hepatitis	B,	hepatitis	C	and	HIV	
antibodies.
3. Obstetric	criteria:	
1. Gestation	≥	34	weeks.
2. Rupture	of	membranes	<	12	hrs
3. Absence	of	maternal	fever	intrapartum
4. Absence	of	congenital	abnormalities	.
Insert	needle	close	to	cord
blood	clamp.
Gravity	or	syringe.
Collect	a	minimum	of	40ml
(incl.	anticoag.).
Collection	time:	2-5	minutes.
Collection	of	cord	blood
37
41
• Depends	on	kind	of	twin	
pregnancy
• If	2	separate	sacs,	can	be	
collected	after	each	twin	
is	born
• If	1	sac,	collect	only	
AFTER	the	birth	of	the	
second	twin
• Mother:
• Hepatitis	B,C
• HIV,	HTLV
• CMV
• RPR.
• Antibody	screen
• Baby:
• ABO/RH	typing
• Total	nucleated	cells
• CD34+	cell	count
• Bacterial	and	fungal	cultures
• Trypan Blue	viability.
• HLA
Bone	Marrow
Qty of	harvest	larger
Engraftment	faster
GVHR	75%
Contamination	more
Tedious	collection
Longer	time	to	find	donors
HLA	typing	–5/6	or	6/6
Limited	supply
Cord	blood
Harvest	quantum	less
Engraftment	takes	longer
GVHR	38%
Less	contamination
Simple	collection
Donor	search	time	–halved
HLA	match	–3/6	or	4/6
Limitless	supply
ü 1958 – HLA typing
ü 1988 – First reported cord blood transplant in France to cure
fanconi Anemia
ü 1992 – international Cord Blood transplant registry founded.
ü 1996 – First unrelated cord blood transplant at Tata Memorial
Hospital, Bombay.
ü 2007 – First Collection of UCB in ORIENT HOSPITSL – Syria
(OCBB)
• Use of umbilical cord blood stem cells is growing every
year.
• 30,000-40,000 transplants performedyearly worldwide.
• >20,000 patients have survived >5 years
Lazarus	HM.	Autologous	and	
allogeneic	transplantation	
procedures	for	hematologic	
malignancies.	Manual	of	
Clinical	Hematology,	3rd
edition	2002:399-409
• Cancer
• High	risk
• Relapse
• Bone	marrow	failure
• Immunodeficiency
• Hemoglobinopathy
• Thalassemia
• Sickle	cell	disease
• Aplastic anemia
• Metabolic/Genetic	disorders	
• Autoimmune	disorders
• Cellular	repair	(regenerative	
medicine)?
1. Define the problem
2. Find the right type of stem cell
3. Match the stem cells with the
transplant recipient
4. Put the stem cells in the right place
5. Make the transplanted cells perform
Current	Stem	Cell	Applications
Acute	Leukemias
Acute	Biphenotypic Leukemia
Acute	Lymphocytic	Leukemia	(ALL)
Acute	Myelogenous Leukemia	(AML)
Acute	Undifferentiated	Leukemia
Chronic	Leukemias
Chronic	Lymphocytic	Leukemia	(CLL)
Chronic	Myelogenous Leukemia	(CML)
Juvenile	Chronic	Myelogenous Leukemia	
(JCML)
Juvenile	Myelomonocytic Leukemia	(JMML)
Myelodysplastic Syndromes
Amyloidosis
Chronic	Myelomonocytic Leukemia	(CMML)
Refractory	Anemia	(RA)
Refractory	Anemia	with	Excess	Blasts	(RAEB)
Refractory	Anemia	with	Excess	Blasts	in	
Transformation	 (RAEB-T)
Refractory	Anemia	with	Ringed	Sideroblasts
(RARS)
Stem	Cell	Disorders
Aplastic	Anemia	(Severe)
Congenital	Cytopenia
Dyskeratosis Congenita
Fanconi Anemia
Paroxysmal	 Nocturnal	Hemoglobinuria (PNH)
Myeloproliferative Disorders
Acute	Myelofibrosis
Agnogenic Myeloid	Metaplasia	
(Myelofibrosis)
Essential	Thrombocythemia
Polycythemia	Vera
Lymphoproliferative Disorders
Hodgkin's	Disease
Non-Hodgkin's	Lymphoma
Prolymphocytic Leukemia
Plasma	Cell	Disorders
Multiple	Myeloma
Plasma	Cell	Leukemia
Waldenstrom's Macroglobulinemia
nPhagocyte	Disorders
Chediak-Higashi	Syndrome
Chronic	Granulomatous	Disease
Neutrophil	Actin	Deficiency
Reticular	Dysgenesis
nLiposomal	Storage	Diseases
Adrenoleukodystrophy
Gaucher's Disease
Hunter's	Syndrome	(MPS-II)
Hurler's	Syndrome	(MPS-IH)
Krabbe Disease
Maroteaux-Lamy Syndrome	(MPS-VI)
Metachromatic	Leukodystrophy
Morquio Syndrome	(MPS-IV)
Mucolipidosis II	(I-cell	Disease)
Mucopolysaccharidoses (MPS)
Niemann-Pick	DiseaseSanfilippo Syndrome	(MPS-III)
Scheie Syndrome	(MPS-IS)
Sly	Syndrome,	Beta-Glucuronidase Deficiency	(MPS-VII)
Wolman	Disease
Histiocytic Disorders
Familial	Erythrophagocytic
Lymphohistiocytosis
Hemophagocytosis
Histiocytosis-X
Langerhans'	Cell	Histiocytosis
Inherited	Erythrocyte	Abnormalities
Beta	Thalassemia	Major
Blackfan-Diamond	 Anemia
Pure	Red	Cell	Aplasia
Sickle	Cell	Disease
Congenital	(Inherited)	 Immune	System	Disorders
Absence	of	T	&	B	Cells	SCID
Absence	of	T	Cells,	Normal	B	Cell	SCID
Ataxia-Telangiectasia
Bare	Lymphocyte	Syndrome
Common	 Variable	Immunodeficiency
DiGeorge Syndrome
Kostmann Syndrome
Leukocyte	Adhesion	Deficiency
Omenn's Syndrome
Severe	Combined	Immunodeficiency	 (SCID)
SCID	with	Adenosine	Deaminase Deficiency
Wiskott-Aldrich	Syndrome
X-Linked	Lymphoproliferative Disorder
Inherited	Platelet	Abnormalities
Amegakaryocytosis /	Congenital
Thrombocytopenia
Other	Malignancies
Brain	Tumors
Breast	Cancer
Ewing	Sarcoma
Neuroblastoma
Ovarian	Cancer
Renal	Cell	Carcinoma
Small-Cell	Lung	Cancer
Testicular	Cancer	
Autoimmune	Diseases
Evan	Syndrome
Multiple	Sclerosis	(Experimental)
Rheumatoid	Arthritis	(Experimental)
Systemic	Lupus	Erythematosus (Experimental)
Other	Inherited	Disorders
Cartilage-Hair	Hypoplasia
Ceroid Lipofuscinosis
Congenital	Erythropoietic Porphyria
Glanzmann Thrombasthenia
Lesch-Nyhan Syndrome
Osteopetrosis
Tay Sachs	Disease
Potential	Future	Stem	Cell	Applications*
Alzheimer's	Disease
Diabetes
Heart	Disease
Liver	Disease
Muscular	Dystrophy
Parkinson's	Disease
Spinal	Cord	Injury
Stroke
52
53
Adult cord blood stem cells injected
into the hearts arteries are believed
to improve cardiac function in
victims of heart failure or heart
attack.
• Regenerate	spinal	cord or	any	other	major	
tissue	in	the	body.
• Studies	show	leukemia	patients	treated	with	stem	cells	
emerge	free	of	disease.
• Injection	of	stem	cells	have	also	reduced	pancreatic	
cancer	in	some	patieents.
Stem	Cell	and	Dermatology	
57
ParkinsonLiver cirrhosis Diabetes
Future	Potential	of	Stem	Cells
• Probably	indefinitely.	At	least	10	years.
Why	do	families	choose	to	collect	and	
store	their	baby’s	cord	blood?
Once	– in- a- lifetime	opportunity	– only	at	birth
• Our	estimates	:
(for	self,	for	cancer):	1	in	
2000
• Cord	Blood	RegistryR:
• For	self:	1	in	400
• For	other	family	
members:	1	in	200
It’s	better	to	have	them	and	
not	need	them	,
Than	need	them	and	not	have	
them	.
Acknowledgement
Clinical	Team	
S.	Samawi
N.	Kafri
S.	Modi
M.	Mousa
IVF	Lab
J.	Sharif	
R.	Doghoz
A.	Kadri
A.	Konali
Fetal	Med.
A.	Taha
M.	Khalaf
M.	Hazemah
Andrology Lab
W.	Hamad
N.	Assaf
M.	Othman
N.	Mazzawi
S.		Sheko
Bio-Ginitic Lab
H.	Droubi
A.	Khatib
M.	Kinj
A.	Othman Administration	
F.	Hamad
R.	Qamar
M.	Haj	hasan
N.	Olabi
E.	Fayad
W.	Saker
Med	Engineering	
Y.	Khabori
S.	Khayat
Anesthesia
R.	Tarko
Y.	Lakkis
M.	Khadra
H.	Sulaiman
Cord Blood Stem Cells

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