MEDS1002 Study Plan PDF

Summary

This document provides a study plan for MEDS1002, focusing on anatomical concepts, particularly related to skin, associated structures, and fascia. It includes case studies to illustrate understanding of those concepts.

Full Transcript

MEDS1002 STUDY PLAN
Skin Lecture
ASSOCIATED STRUCTURES
- Hair and hair follicles
- Sebaceous glands (secrete sebum into hair follicles)
- Sweat glands (temperature regulation and toxins)
- Nails (plates of keratinised cells)
Layers
- Epidermis
o Keratinocytes ~ 85%
o Varied THICKNESS dependent on function
o Soles and palms = thicker = without
hair follicles
o Cells differentiate as they move up layers,
exfoliated from surface
- Dermis
o Tensile strength and stretch
o Contains collagen and elastin fibres
o Responsible for finger print (between
epidermis and dermis)
- Hypodermis
o Consists of adipose tissue, loose connective tissue, subcutaneous fat, superficial fascia
o Anchors to underlying structures
o ENERGY STORAGE
o INSULATION
o Varied THICKNESS
CASE STUDY: ACNE CASE STUDY: SUNBURN
Results from: Protection: Melanin
- Accumulation of dead skin cells and - Pigment which absorbs / scatters UV and
keratin vis-light
- Excess sebum production
- Bacterial proliferation / inflammation
Consequences
- Inflammation
- Scarring
Solutions
- Accutane
o Vit A
o Reduces sebum production
o Anti-inflammatory
o Reduced bacterial growth
o Shrinks sebaceous glands

CASE STUDY: BOTOX
Blocks nerve cells causing muscle contraction and sweat gland activation
Fascia lecture
Glossary
Fascia: Layer of strong, flexible connective tissue covering/separating/holds together various
organs/muscles/vessels/nerves
Sheath: covering of connective tissue
Viscera: internal organs
Connective tissue: main tissue type consisting of fibroblast cells and collagen fibres
Tendon and aponeuroses: attach muscle to
bone
Parietal: wall of body cavities
Ligaments: attach bone to bone

Fascia is…
→ Mostly DENSE REGULAR (or IRREGULAR)
connective tissue
→ Collagen = arranged in bundles, running
parallel to each other

Superficial ROLE
Loose connective tissue + adipose - Protection and cushioning from impact
Contains sweat glands/vessels/cutaneous - Fat storage
nerves - Anchors skin
- Facilitates movement/flexibility
- Pathway for nerves and vessels
- Contains immune cells

Deep ROLE
Surrounds/separates BONES, MUCLES, - Support and structure of muscles
NERVES, and VESSELS - Muscular force via tendons, ligaments and
Dense REGULAR/IRRECULAR connective aponeuroses
tissue - Compartmentalisation
3 layers… - Prevent infection/inflammation
Proverbial Covers cervical vertebra and - Reduces friction
sheath associated muscles - Support vessels and nerves
Pre- Supportive framework for - Detects changes in tension/pressure and
tracheal anterior neck structures, pain
sheath facilitates movement during Classifications…
swallowing/speaking Epimysia Surrounds muscles
Carotid Protects carotid arteries, jugular Intermuscular Compartmentalisation
sheath vein, and vagus nerve septa
Aponeuroses Wide attachment area
Retinacula Surrounds joints
Investing Surrounding
neurovascular bundles
 APONEUROSES
- Sheet of pearly white connective tissue
- Attaches muscles (requiring qide attachment areas)
- EG palms and soles
-
2 Serosal layers associated with fascia…
Visceral Parietal
Surrounds organs of thoracic, Lines walls of
abdominal, and pelvic cavities body cavities
(organs that move or move next to
each other)
ROLE
- Facilitates organ movement against each other
- Facilitated by fluid in interstitial space
NOTE: a “real space” is made between visceral and parietal
layers → epithelial cells secrete fluid to reduce friction of
organ movement

Injuries to SCALPS bleed profusely… why??
S → skin
Move as a unit, tightly connected, arteries
C → connective tissue (superficial)
unable to retract (help open by fascia)
A → aponeuroses
L → loose connective tissue
P → periosteum
CASE STUDY: issues
1. Overuse / repetitive stress of muscles
2. Trauma – sprain, strain, tear
3. Infection
4. Autoimmune disorders (arthritis)
5. Biomechanics (abnormal gait, poor posture)
6. Natural aging
7. surgery

Muscles lecture
Skeletal muscle attachments:
- contractile component of the muscle (red) = the belly (can be split into two or more heads)
- must be attached to two points (tendons = way muscle attaches)
- upon contraction the two points move closer together
- attach to bone via TENDONS
- attach to bone via APONEUROSES
TENDON LIGAMENT
→ Dense fibrous connective tissue (organised → Similar materials
collagen bundles) – don’t contract → deep in the body
→ attach muscles to BONE → attach BONE to BONE
→ rounded/strap-like cords → surrounds bone joints

TYPES OF MUSCLES
INTRINSIC EXTRINSIC
Both attachment points within one area of the One has one attachment within one body
body structure, one beyond it

MUSCLE SHAPE: MUSCLE SHAPE: pennate
Flat - feather-like
- parallel - unipennate (muscle fibres insert
fibres at angle to one side of tendon)
- may be wide - bipennate (muscle fibres insert
- may have at angle to both sides of tendon)
aponeurosis - multipennate (collection of
- may be thin bipennates)

Can be longer - can
contract more
MUSCLE SHAPE:
Fusiform
- spindle
shaped

Can pack many (most) short angled
fibres into a smaller region
→ pennation = less contraction, but
more fibres contracting simultaneously =
stronger
MUSCLE SHAPE: MUSCLE SHAPE: Circular
Convergent - Form a sphincter
- possess
broad and
narrow
attachment
at either end

MUSCLE SHAPE: MUSCLE SHAPE: multiheaded /
quadrate multibellied
- 4 equal sides - More than one attachment at
one end

-
TENDONS AND LIGAMENTS
= attach to bones via Sharpey’s fibres (perforating fibres)
= parallel collagen fibres extend into the periosteum and embed
into the bone matrix
= periosteum is the dense connective tissue layer immediately
surrounding bone

JOINTS… caused by skeletal muscle
Mechanical advantages:
1. Effectiveness of muscle effect on joint varies
2. Length of tendons effects
3. Joint positioning can maximise muscle fibre contractions

EXAMPLES OF MUSCLE ACTIONS ON JOINTS
FLEXION EXTENSION
Bending (decrease angle at joint) Straitening (increase angle at joint)

ABDUCTION ADDUCTION
Moving away from the midline of the body Moving towards the midline of the body (coronal
(coronal plane) plane)
EG spreading fingers EG bringing fingers back together
 Nerves activate muscle
Motor unit= motor neuron (nerve cell) and the muscle fibres it controls
Nerves typically activate the muscles they pass through (usually from the deeper side)
Wide muscles → nerves stimulate parts individually to alter muscle action

TYPES OF CONTRACTION
ISOTONIC ISOMETRIC
▪ Muscle changes ▪ Muscle length
length unchanged
▪ Movement produced ▪ No movement
▪ Resists gravity and
force
CONCENTRIC ECCENTRIC
▪ Muscle shortens ▪ Muscle contracting
▪ Movement produced but lengthening
▪ Controlled movement
MUSCLE TONE
NOTE: muscles are almost always slightly contracted, even
when relaxed
▪ Contraction = no movement
▪ Muscles slightly stiff
▪ Maintains posture/stability

MUSCLE FUNCTIONS
FIXATOR SYNERGIST/S
▪ Steadies’ proximal limb segments ▪ Helps the prime mover
▪ Isometric contraction ▪ Does similar action / steadies joint
PRIME MOVER ANTAGONIST
▪ Produces a specific movement ▪ Opposes action of prime mover
▪ Concentric contraction ▪ Eccentric contraction

HOW ARE MUSCLES FED
FIXATOR SYNERGIST/S
Supplied by arteries bringing blood Multiple arteries contracting within muscles
PRIME MOVER ANTAGONIST
Tendons supplied by blood from muscle bellies ▪ Endurance (isotonic movement) increases
and from the bone they are attached to number of blood vessels
▪ Strength training (isometric movement)
increases mass of muscle fibres

Nerves and Vessels Lectures

MUSCLE FUNCTIONS
ARTERIES VEINS
▪ Carries oxygenated blood ▪ Carries deoxygenated blood
▪ Blood flow: heart → body ▪ Blood flow: body → heart
▪ Thick elastic walls ▪ Less thick and elastic walls
▪ High pressure ▪ Low pressure
▪ No valves ▪ Valves
▪ Branching

LYMPH VESSELS NERVES
▪ Carries excess fluid/plasma proteins/cell ▪ Superficial nerves form networks with
debris: interstitial space → venous system vessels
(drains from spaces between cells ▪ Deep nerves collect with vessels in
▪ Fluid flow: tissues → heart bundles under deep fascia
▪ Fine, thin walled ▪ Large nerves/vessels may be enclosed in
▪ Needs pressure from vessels and muscles fascial sheaths
to pump
▪ Abundance: where body contracts
exterior skin/mucosa/submucosa of
respiratory/GI systems/membranes
▪ Limited: muscles/bone/fascia
▪ Absent: CNS
▪ Drainage: Drain into lymphatic ducts
(lymph vessels that merge together):
lymph → blood

TYPES OF CIRCULATION
PULMONARY SYSTEMIC
Heart → lung, heart → lung Blood begins deoxygenated → supplied to heart
Blood begins deoxygenated (from body) → → lungs → oxygenated
reoxygenated when pumped to lungs Blood begins oxygenated → supplied to body →
deoxygenated
General order: artery → arteriole → capillary → venule → vein

JOURNEY OF BLOOD FROM DEOXYGENATION TO OXYGENATION

^^ general systematic circulation ^^
 RIGHT VENTRICLE→ PULONARY ARTERIES → CAPILLARY BEDS (IN LUNGS)
→ GAS EXCHANGE → OXYGENATED BLOOD (FROM VENULES) → LEFT
VENTRICLE (VIA VEIN)

THE HEART
MECHANISMS
= 2 sided
= 2 pumps
= 4 chambers
= 2 atria receive blood from veins
= 2 ventricles pump blood to arteries
RIGHT SIDE receives deoxygenated blood (loss
pressure pump = thinner walls)
LEFT SIDE receives oxygenated blood (higher
pressure pump = thicker walls)

Venous plexuses = intercommunicating networks of veins
- Cushioning effect around nervous tissue (spinal cord)
- Wick heat off hot blooded artery (spermatic cord

Venous plexuses =
intercommunicating
networks of veins
- Cushioning
effect around
nervous tissue
(spinal cord)
- Wick heat off
hot blooded
artery
(spermatic
cord
Venous sinuses =
endothelial-lined
spaces with cranial
cavity (drainage)

LYMPHATIC SYSTEM
ROLE: drains excess tissue fluid, cleans up debris
→ lymph: when fluid enters a lymphatic vessel
→ lymph is typically clear/colourless
→ GI lymph’s carry lipids = can have milky appearance
 FACTORS AFFECTING LYMPH FLOW
→ Filtration pressure in tissue space

→ Vessel compression

→ Gravity and pressure

→ valves create unidirectional flow

→ No pump

Lymphatic organs…
◼ produce lymphocytes (type of white blood cells) → consists of thymus gland, bone marrow
◼ initiate immune response against antigens
 NERVOUS SYSTEM
CNS ROLE
Make sense of stimulation (sensory input)
Initiates responses (motor output)
Facilitates response to internal and external
environments
PNS ROLE
Collects and transports sensory input
External → internal environments (CNS)
Collects and transports motor output
Internal (CNS) → external environments

Nerves in the
head
= optic
= trigeminal
Spinal nerve
= intercostal
nerve
= vagus
= phenic
= sympathetic
trunk
PNS
= radial
= ulnar

Bone Lectures
BONE FUNCTION
◼ enables movement
 ◼ provides support
◼ protects organs
◼ store/release minerals
◼ production of red blood cells

Cells involved in remodelling
Remodelling consequential of altered muscle use
Osteoclasts (cells removing bone)
Osteoblasts (cells adding bone)

TYPES OF BONE
CANCELLOUS CORTICAL
- porous - outside
- spongy - dense/heavy
- light - outside of bone
- inner bone and at the ends of long bone - less porous

MADE OF…
HYDROXYAPATITE: mineral component mainly Ca and P → provides strength and rigidity
COLLAGEN: provides elasticity/flexibility (organic)

Periosteum definition: fibrous sheath covering bone, containing blood vessels and nerves, providing
nourishment and sensation

VASCULAR SUPPLY
→ blood supply to and from bone
Principal arterial sources (central arteries):
1. Periosteal
2. Nutrient
Both contribute to CENTRAL ARTERIES
Venous drainage occurs through corresponding
veins
1. Periosteal
2. Venous
3. Central

BONE DEVELOPMENT
 BONE CLASSIFICATION
LONG – TUBULAR

SHORT – CUBOIDAL

FLAT = USUALLY
PROTECTIVE
IRREGULAR

SESEAMOID – FORMS
WITHIN A TENDON, GIVES
MUSCLE GREATER FORCE
FOR FUNCTION (INCREASED
DISTANCE TO EXTEND OVER
= GREATER POWER)
 MARKINGS AND FEATURES ON BONE
CREST (ridge) FORAMEN (opening/hole) – NUTRIENT
FORAMEN (takes artery into bone)

FOSSA (depression/hollow) TUBEROSITY (roughened prominence for
attachment)
Forensic lecture
Forensic workers
- Coroners
- Pathologists
- Dentists
- Anthropologists
- mortuary technicians
- radiographers
- social workers
- molecular biologists

BIOLOGICAL PROFILING
ANCESTRY/RACE SEX
→ bone structure (bone prominence, face → almost impossible in children
projection, nose, mandible) (underdeveloped sex characteristics)
→ DNA (groups of people sharing same series of → adults – pelvis development and muscle
mutations on mitochondrial genome) attachments (overlapping with long bones)
→ Phenotyping (appearance): issues = hair/eye
colour change, skin colour change

AGE STATURE/HEIGHT
→ Children = dental eruption
 → Adolescence = dental and bone fusion
→ Adults (difficult post-40) = growth stopped,
degree of osteoarthritis

TYPES OF TRAUMA
1. blunt Antemortem trauma: Perimortem trauma: Postmortem trauma:
2. sharp force injury occurring before injury occurring around injury occurring after
3. ballistic/projectil death time of death death
e - useful in child - fresh bone = Causes:
abuse significant → dogs
cases/identificatio collagen → rodents
n - fractures are →
shape/jagged weathering/erosion
- bone bending → plants
→ burning

Estimating postmortem interval
IMPORTANCE identify the person, witnesses and suspects
PROBLEMS weathering of bone dependent on environment (temperature, humidity, pH, exposure, soil
type) which vary enormously
METHODS
- Cultural associations
- Taphonomic factors
- Radioactive decay methods

Cultural associations in estimating postmortem intervals
ABORIGINALS EUROPEAN POSITIONING
Exhibit severe tooth wear Restorations/fillings, Prehistoric: flexed/foetal
without decay (no sugar, tough crowns/root canal treatment, position
diet) implants, orthodontics, veneers Forensic: shallow burial, odd
positioning
Historic: extended on back

RADIOACTIVE DECAY METHODS
RADIOCARBON DATING BOMB PULSE C14 DATING
 - Uses C-13/14 Testing nuclear weapons of WW2 = significant
- Useful from 300-60,000 years atmospheric C-14 concentrations
Suitable post 1950s
Not useful as time progresses (levels stabilising)

Joints Lecture

“anthrology” = study of joints
“anthroscopy” = scoping of a joint
“anthroplasty” = joint replacement
“arthritis” = inflammation of joint
“articulation” = two bones meeting
(eg articulation between the two
bones in the forearm)

Joint definition: known as an articulation – the site where 2+ bones meet to facilitate movement/support

FIBROUS CARTILAGINOUS SYNOVIAL
- Bones joined by fibrous Bones joined by: Features:
connective tissue a) cartilage - joint capsule
- Little to no movement b) cartilage and fibrous tissue - ligaments
i) cartilage type = hyaline - synovial membrane and fluid
ii) some joins may have pad of - articular cartilage
fibrocartilage - sometimes: fat pad, articular
iii) slight → no movement discs
- freely movable

OSTEOARTHRITUS
WHAT IS IT? FACTORS AFFECTING
Bone-joint inflammation, occurring due to - Mechanical
imbalanced joint tissue - Inflammatory
repair/destruction/remodelling - Metabolic
Comparative Anatomy Lecture
LEARNING OUTCOME: identify bones, bony features, and tooth types of the human skull

Human teeth = unspecialised
Bony pelvis = hip bones and sacrum
 COMPARING HUMAN LIMBS

LOWER LIMB
- Similarities across species = usually used for locomotion
- In quadrupedal mammals weight bearing on lower limbs
ANIMALS
BASIC VERTEBRATE LOWER LIMB - For animals dependent on running
PLAN → increasing length of distal limb segments
increases the distance covered with stride
→ longer distal segments cover more ground for
same energy expended
→ reduced animal digits and slender bones reduces
energy required to swing limb

→ more digits increase manoeuvrability for
short energetic bursts
→ long distance = less toes
→ JUMPING ANIMALS: lower limbs highly
flexed – muscle levelrage, large feet
increase locomotion
→ SWIMMING AND FLYING ANIMALS:
lower limbs = flippers, not weight bearing
Histology lecture

HISTOLOGY VS PATHOLOGY
HISTOLOGY PATHOLOGY
study of body’s cells and tissues / how tissues are study of abnormal / diseased tissue
organised into organs

STEPS INVOLVED IN TISSUE PROCESSING
1. SPECIMEN ACQUISITION
2. FIXATION to preserve structure
3. DEHYDRATION to remove water
4. EMBEDDING stiffen to cut
5. SECTION improves resolution
6. STAIN produces contrast, specific identification of structures
STEPS INVOLVED IN TISSUE PROCESSING
1. SPECIMEN ACQUISITION fresh tissue
2. FIXATION to preserve structure
3. DEHYDRATION to remove water
4. EMBEDDING stiffen to cut
5. SECTION improves resolution
6. STAIN produces contrast, specific identification of structures
Magnification: enlarging the size of an object through optimal instrument
Resolution: ability to distinguish between two closely spaced objects / images
→ Low resolution = blurry / less distinct
Viscera Lecture
Viscera means ‘internal organ’ → typically protected by superficial bone,
muscles, or fat
 BODY SYSTEMS

SYSTEMIC ANATOMY REGIONAL ANATOMY
→ structures that work together → structures located together
→ various locations → PRO: focus on one ‘body area’ at a time
→ PRO: focus on one body function at a time → CON: sometimes unrelated functions
→ CON: hard to draw correlations with other
systems
 VISCERA OF CRANIAL CAVITY (+ VERTEBRAL)
- Brain – cerebral hemisphere
- Brain – cerebellum
- Brain stem
- Spinal cord

VISCERA OF THORACIC CAVITY
VISCERA OF ABDOMINAL CAVITY

VISCERA OF PELVIC CAVITY
Viscera 2 lecture
Viscera of the cranial cavity and their relationships

Cerebral hemisphere: controls voluntary motor actions,
sensory processing, emotional control, higher thought
processes
Cerebellum: controls physical movements, regulates
balance learned movements, controls motor coordination - VOLUNTARY
Brain stem: connects brain and spinal cord, controls INVOLUNTARY
Spinal cord: communicates sensory, motor and autonomic messages between brain and body (interacts
with external environment, controlling internal environment)

Viscera of the thoracic cavity

Right lung Lateral to heart, great
vessels, trachea, bronchi,
and oesophagus
Heart and great vessels Medial to lungs, anterior to
trachea and oesophagus
Left lung Lateral to heart, great
vessels, trachea, bronchi,
and oesophagus
Trachea and bronchi Posterior to heart, anterior
(passage for air in and out of to oesophagus, medial to
lungs) lungs

Oesophagus (passage for Posterior to heart, trachea
food and drink into stomach) and bronchi, medial to
lungs
Thyroid gland (makes Superior to heart and lungs,
thyroid hormone – gets oxygen anterior to trachea and
into cells from metabolism) oesophagus

Viscera of the abdominal cavity

Liver (makes bile, processes blood to removes Small intestine (absorption of nutrients)
waste, breakdowns harmful GI substances)
Stomach Spleen (filters/stores blood, produces white
blood cells/antibodies, destroys old red blood cells)
Gall bladder (stores bile) Right kidney (filters blood, eliminating excess
fluids and salts, removes wastes)
Large intestine (removes water from digested Left kidney
food)
Duodenum (chemical digestion of partially
digested food, site for bile and pancreatic enzyme,
absorbs water, electrolytes, and nutrients)
Pancreas (makes enzymes to digest protein, fat,
sugar, controls BGL, makes endocrine hormones
(insulin/glucagon))

Viscera of the pelvic cavity

Urinary Stores urine made by kidneys
bladder
Ureter Passage for urine from kidney →
bladder
Ovary Produces female gametes,
secretes hormones
Uterus Space for protection, supply of
oxygen/nutrition, removal of
metabolic waste for offspring
Vagina Passage in/out of uterus for sperm

Prostate Secretes fluid to protect/nourish
male gametes, allows ejaculation
gland of semen/secretes hormones
Urethra Passage for urine from bladder to
outside body, for males passage of
sperm outside body
Large Removes water from faeces
intestine
Rectum Stores faeces from colon
Fertilisation to Neurulation
Cellular processes during embryonic development

PROLIFERATION DIFFERENTIATION INTERACTION MOVEMENT
Rapid divisions of cells One cell turns into Cell communication
diving to form different another cell type (many interactions and
structures movement)

CELL IDENTITY GUIDE CELLS TO DEVELOPMENT TYPES OF CELL SIGNALS
a) Gene expression AUTOCRINE SIGNALLING: one cell secretes, acts on
b) Protein expression itself
c) MicroRNA PARACRINE SIGNALLING: signal released by one
d) Epigenetics cell, affecting surrounding cells

MORPHOGEN / MORPHOGEN GRADIENTS
Crucial for inductive signals
Morphogen: instructing molecule for development (come in the embryo) important in establishing
signals and gradients
Organising organ: structure signalling and affecting surrounding cells (secretes signal) that move across
embryo with concentration gradient (high conc. to low conc.)

Organising structures resulting in gradient across tube = green and purple (roof plate) = patterning of
spinal cord
 EMBRYONIC DEVELOPMENT
▪ Female gamete = oocyte (released and travels down fallopian tube)
▪ Haploid cell (23 chromosomes) forms in ovaries
▪ Fertilisation (embryo implantation) occurs in uterus
▪ Hormones prep uterine lining for embryo implant = oestrogen, progesterone
▪ Hormones prep oocyte for ovulation = luteinizing hormone (LH) and follicle stimulating hormone
(FSH)
▪ DAY 14 = ovulation
▪ 7 DAYS LATER = embryo formation, uterus ready to receive embryo for implantation
▪ Zygote (single cell pronuclei, diploid 46 chromosomes) formation post-fertilisation

THE ZYGOTE
Zygote:
→ single cell pronuclei (2 – 1 from oocyte, one from sperm)
→ surrounded by zona pellucida (protection and maintains
development)
→ outside = polar bodies (excess)

EARLY STAGES OF DEVELOPMENT
 SERIES OF MITOTIC DIVISIONS AS IT TRAVELS DOWN THE FALLOPIAN TUBE

STAGE 1: Zygote Cleavage = single cell splits
STAGE 2: Series of cleavages (cell division)
STAGE 3: Cells get smaller with each division
STAGE 4: Day 5 Morula formation, compacts and cavitates (cells compacting 16-32 cells)
- Cell polarity established: different inside/outside environments (receive different signals)
- Cavity formation: cavity forms as fluids rush into embryo
- Differentiation: cells evolve to more developed cells (totipotent) → can turn into any embryonic
cell → excess cells produce embryonic tissue (yolk or amniotic sac)
STAGE 5: Blastocyst formation… main cell populations
- Inner cell mass: contain cells that turn into embryo, making nerve/heart cells, supportive tissues
(yolk sac) (pluripotency – multiple cell types)
- Trophectoderm: outer population of cells (differentiate into the placenta)

STAGE 6: DAY 6/7 Blastocyst hatches from zona pellucida
- Inner cell mass segregates into two populations of
cells
- Primitive endoderm (Hypoblast) differentiates into
extra embryonic tissue
- Primitive ectoderm (Epiblast) forms embryo/foetus
STAGE 7: Blastocyst must escape protective structure to penetrate/attach to the endometrium
STAGE 8: 8/9 days embryo implants into uterine wall
STAGE 9: proliferation of uterus, embryo adheres, attaches, and invades to uterine wall (endometrium)
- Invasion of endometrium using trophoblast cells (eventually form placenta)
- Epiblast and hypoblast from bilaminar disc
- Amniotic cavity formation

PREGNANCY TEST OPERATION = trophoblast cells secrete human chorionic gonadotpin
(Hcg) hormone
Detection ~ 2 weeks post-implantation
Tests must be sensitive and specific via urine samples
Present hCG binds to antibodies

Bilaminar disc formation
Epiblast = pluripotent
Hypoblast becomes multipotent → differentiates into different cell population
Visceral endoderm → forms yolk sac
Hypoblast cells migrate and form a cavity (yolk sac)
 GASTRULATION
BEGINS WITH THE FORMATION OF THE PRIMITIVE STREAK AT THE CAUDAL END OF THE
PRIMITIVE ECTODERM

Epiblast → primitive ectoderm → germ layer formation
Beneath yolk sac supplies nutrients to embryo
Primitive streak: site of gastrulation
Initial: primitive ectoderm proliferation (cell division)
3 germ layers:
1. Ectoderm: nervous system, skin, hair, nails
2. Mesoderm: forms bone, blood vessels/blood, heart, muscles
3. Endoderm: form epithelial lining of glands/respiratory/GI tracts

During development: embryo will turn and fold where endoderm will form inside structures

Cells of the node establish embryonic left-right axis
➔ Primitive node/pit: consists of cells (made of cilia) – motile cell specialisation, embryo rotates
clockwise distributing signals forming left-right axis
➔ Signal movement in specific direction = structures are unilateral
 NEURULATION (DAY 20)
Neural plate undergoes neurulation
Neural tube formation
◼ Neural plate folding forms neural tube
◼ Primitive ectoderm thickens, elevates, folds
◼ Neural folds converge at the mid line
◼ Neural tube closes
◼ Patterning (different neurons – motor/sensory – at different regions)
◼ Upon neural tube closing:
→ notochord: organiser, instructs bottom half of neural tube
→ anterior/dorsal components: different, specific neuron types
◼ Upon closure = two sides = caudal and cranial neuropore

Neural tube function
o Cells of CNS
Neural crest cells
o Forms PNS
o Melanocytes (skin pigmentation)

BODY PLAN FOR ORGANOGENESIS
 During embryonic development, primary BRAIN vesicles formed → differentiate to produce secondary
brain vesicles

^^ Neural tube patterning ^^

BASIC STAGES OF DEVELOPMENT
1. PREIMPLANTATION
2. GASTRULATION / EARLY ORGANOGENESIS
3. ORGANOGENESIS
4. FOETAL GROWTH AND DEVELOPMENT

DEFINITIONS
Somatic cells: highly specialised body cells Differentiation: is the process of turning into
Progenitor cells: less mature cells: another cell
differentiate/replicate Potency: ability to differentiate
Stem cells: undifferentiated (cannot turn into Terminally differentiated: cannot differentiate
another cell type) = unspecialised
 TYPES OF STEM CELLS
EMBRYONIC ADULT INDUCED PLURIPOTENT
→ derived from inner cell mass of → derived from developed → somatic body cells ‘reverted’
the blastocyst organs backwards to pluripotent
→ pluripotent – differentiate into → multipotent – lineage embryonic stem cell-like cells
~200 body cells restricted (genetic reprogramming)

EG BLOOD STEM CELLS
- Cells turn into multipotent cell types
- Form various blood components
o RBC
o WBC
o Platelets
- Highly differentiable
- Highly specialised
- Aids understanding blood development / factors affecting

USES OF STEM CELLS
 MOLECULAR REGULATION OF CELL IDENTITY

Growth factor: differentiation and proliferation stimulating molecule
- Useful for studying cell behaviour
- Changes molecular identity of cell
- Various growth factors alter concentrations/timings/gradients/affects
IDENTIFYING IF YOU HAVE THE RIGHT CELL TYPE
PHENOTYPE MOLECULAR MARKERS
Not the optimal way (stomach/liver cells look the Proteins and genes
same) Cells have molecular identity

Example in development: How does the neural plate form the neural tube?
Cannot access neural tube in the embryo: invasive/dynamic
Use stem cells to help isolate particular events during embryogenesis -> proliferation,
differentiation, interaction and movement.
Take stem cells -> add growth factors to turn them into neurons
o Want to look at neural plate differentiation-> definitive ectoderm, proliferating and forming lots and
lots of layers, add growth factors to stem cells that are known to cause proliferation -> can study
those process
o Can look at signalling pathways that happen, what cells do how they migrate
o Can look at how the nervous system gets patterned -> dorsal patterning growth factors and turn
them into sensory neurons
▪ Can understand not just how neurons develop but how sensory neurons develop
▪ If there were problems with sensation, that information can help understand some of the
pathological occurring
▪ Same thing can be done for dorsal patterning turning them into motor neurons, motor neuron
development and disease.
Workshop Notes
 Bilateral = paired structured (on body’s left/right)
Unilateral = one on one side of the body
Ipsilateral = two structures being compared on the same side of the body
Contralateral = two structures compared on opposite sides of the body

Practical Notes
General, identifiable descriptions of organs
Heart: size of a large apple/fist, shaped like a pear or upside down egg (rounder top and pointier bottom),
marbled texture like a steak
Brain: looks like a wrinkled walnut, soft pinkish cauliflower, consistency like jelly/tofu
Lung: spongy balloon, pinkish-grey, tree branches with leaves = bronchial tree
Stomach: deflated ballon, bagpipe, rubber hot water, soft wrinkled leather pouch
Kidney: beans, size of a smartphone, rubbery
Large intestine: long bumpy tube (coiled garden hose), upside down horseshoe, series of linked sausages,
bumpy accordion
Small intestine: long tightly coiled garden hose, bundle of cooked spaghetti
Pancreas: lumpy banana, fish fillet (wider head, narrow tail), long pine cone
Gallbladder: small green pear, deflated balloon

Muscles, nerves, and vessels
 ARTERY
Description - Firm and elastic
- Thick muscular walls
- Thick rubber hose / springy thick rubber cord
- Larger than veins and nerves
- Red appearance
Location in relation to Close to tissues and organs (to supply oxygen).
other nearby structures
VEIN
Description - Softer, thinner, flexible
- Blue appearance
- Rubber tube, soft cord, flexible straw
Location in relation to Carry deoxygenated blood to the heart, located running parallel to arteries,
other nearby structures typically closer to skins surface and sometimes bile ducts.
NERVE
Description - Smooth
 - Rope-like
Location in relation to Transmit signals between brain, spinal cord, and body, often running
other nearby structures alongside structures including muscles, blood vessels, and bones.

Muscles
Nerves
Bone

Joints