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International Journal of
eISSN: 2470-9980

Vaccines & Vaccination

Correspondence:

Received: January 01, 1970 | Published: ,

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Abstract

Vaccines are being under investigation for the possible side effects they can cause. In order to supply new information, an electron-microscopy investigation method was applied to the study of vaccines, aimed at verifying the presence of solid contaminants by means of an Environmental Scanning Electron Microscope equipped with an X-ray microprobe. The results of this new investigation show the presence of micro- and nanosized particulate matter composed of inorganic elements in vaccines’ samples which is not declared among the components and whose unduly presence is, for the time being, inexplicable. A considerable part of those particulate contaminants have already been verified in other matrices and reported in literature as non biodegradable and non biocompatible. The evidence collected is suggestive of some hypotheses correlated to diseases that are mentioned and briefly discussed.

Keywords:vaccine, disease, contamination, protein corona, biocompatibility, toxicity, nanoparticles, immunogenicity, foreign body, environment, industrial process, quality control

Introduction

Vaccines are one of the most notable inventions meant to protect people from infectious diseases. The practice of variolation is century-old and is mentioned in Chinese and Indian documents dated around 1000 A.D. Over time, variolation has been replaced by vaccination, vaccines have been enhanced as to technology, and the vaccination practice is now standardized worldwide.

Side effects have always been reported but in the latest years it seems that they have increased in number and seriousness, particularly in children as the American Academy of pediatrics reports.1,2 For instance, the diphtheria-tetanus-pertussis (DTaP) vaccine was linked to cases of sudden infant death syndrome (SIDS);3 measles-mumps-rubella vaccine with autism;4,5 multiple immunizations with immune disorders;6 hepatitis B vaccines with multiple sclerosis, etc.

The notice of Tripedia DTaP by Sanofi Pasteur reports “Adverse events reported during post-approval use of Tripedia vaccine include idiopathic thrombocytopenic purpura, SIDS, anaphylactic reaction, cellulitis, autism, convulsion/grand mal convulsion, encephalopathia, hypotonia, neuropathy, somnolence and apnea”. The epidemiological studies carried out did not show a clear evidence of those associations, even if in 2011 the National Academy of Medicine (formerly, IOM) admitted: "Vaccines are not free from side effects, or adverse effects".7

Specific researches on components of the vaccines like adjuvants (in most instances, Aluminum salts) are already indicated as possible responsible of neurological symptoms8‒10 and in some cases, in-vivo tests and epidemiological studies demonstrated a possible correlation with neurological diseases.10,11 Neurological damages induced in patients under hemodialysis treated with water containing Aluminum are reported in literature.12

Recently, with the worldwide-adopted vaccines against Human Papillomavirus (HPV), the debate was reawaken due to some adverse effects reported by some young subjects.

Specific studies communicated the existence of symptoms related to never-described-before syndromes developed after the vaccine was administered. For instance, Complex Regional Pain Syndrome (CRPS), Postural Orthostatic Tachycardia Syndrome (POTS), and Chronic Fatigue Syndrome (CFS).13 The side-effects that can arise within a relatively short time can be local or systemic.

Pain at the site of injection, swelling and uncontrollable movement of the hands (though this last symptom can also be considered systemic) are described. Among the systemic effects, fever, headache, irritability, epileptic seizures, temporary speech loss, lower limbs dysaesthesia and paresis, hot flashes, sleep disorders, hypersensitivity reactions, muscle pain, recurrent syncope, constant hunger, significant gait impairment, incapacity to maintain the orthostatic posture are reported.14

It is a matter of fact that every day millions of vaccine doses are administered and nothing notable happens, but it is also irrefutable that, regardless of the amount of side effects that are not recorded and the percentage of which remains in fact unknown, in a limited number cases something wrong occurs. No satisfactory explanation or, in many cases, no explanation at all has been given and it seems that those adverse effects happen on a random and stochastic basis.

Those situations induced us to verify the safety of vaccines from a point of view which was never adopted before: not a biological, but a physical approach. So, we developed a new analysis method based on the use of a Field Emission Gun Environmental Scanning Electron Microscope investigations to detect possible physical contamination in those products.

Material and methods

44 types of vaccines coming from 2 countries (Italy and France) were analyzed. Table 1 groups them in terms of name, brand and purpose.

N

Name

Brand Name,  Country of Distribution        

Description

Production Batch, Expiry Date

1

Vivotif Berna

Berna Biotech SA, Italy

Anti-Thyphoid Vaccine  (Live), group Ty21a

3000336 [2004]

2

Typhim Vi

Aventis Pasteur MSD, Italy

Anti-Salmonella typhi Vaccine

U1510-2 [2004]

3

Typherix

GlaxoSmithKline S.p.a., Italy

Anti-Thypoid Vaccine  (polysaccharide Vi)

ATYPB061BB [2009]

4

Anatetall

Chiron (now Novartis) Italy

Adsorbed anti-Tetanus Vaccine

030106 [2004]

5

Anatetall

Novartis Vaccines and Diagnostics, Italy

Adsorbed anti-Tetanus Vaccine

060510 [2009]

6

Tetabulin

Baxter AG, Italy

Adsorbed anti-Tetanus Vaccine

VNG2G006A [2009]

7

Dif-Tet-All

Novartis Vaccines and Diagnostics, Italy

Adsorbed anti-Tetanus  and diphtheria Vaccine

070501 [2009]

8

Infanrix

GlaxoSmithKline S.p.a., Italy

Anti-Diphtheria, tetanus and pertussis vaccine

AC14B071AJ [2009]

9

Infanrix hexa

GlaxoSmithKline Biologicals s, Italy

Anti-diphtheria, tetanus, pertussis, hepatitis B, poliomyelitis
and disease caused by Haemophilus influenzae type b

A21CC512A [ 2017]

10

Infanrix hexa

GlaxoSmithKline Biologicals s. a.  France

Anti-diphtheria, tetanus, pertussis, hepatitis B, poliomyelitis
and disease caused by Haemophilus influenzae type b

A21CC421A [ 2017]

11

M-M-R vaxPro

Sanofi Pasteur MSD, Italy

M-M-R vaxPro  (measles, mumps, and rubella)
analyzed in Cambridge        

L012437 [ 2017]

12

Repevax

Sanofi Pasteur MSD, France

Anti-diphtheria-tetanus-pertussis-polio-vaccine

L0362-1 [2017]

13

Repevax

Sanofi Pasteur MSD SNC France

Anti-diphtheria-tetanus-pertussis-polio-vaccine

L0033-1 [2016]

14

Priorix

GlaxoSmithKline S.p.a., Italy

Anti--measles-mumps, and rubella (MMR) vaccine

A69CB550A [2009]

15

Morupar

Chiron (now Novartis, ), Italy

Anti-measles- mumps, and rubella (MMR) vaccine

7601 [2004]

16

Varilrix

GlaxoSmithKline S.p.a., Italy

Anti-Chicken pox vaccine (group OKA)

A70CA567A [2009]

17

Stamaril Pasteur

Sanofi Pasteur MSD, Italy

anti-yellow fever  vaccine

A5329-6 [2009]

18

Allergoid-Adsorbat 6-Graser Starke B.    

Allergopharma, Germany

Antiallergic vaccine

Ch-B.:30005999-B [2006]

19

Engerix-B

GlaxoSmithKline S.p.a., Italy

Adsorbed  anti-hepatitis B vaccine

AHBVB468BD [2009]

20

Prenevar 13

Pfizer, Italy

Antipneumococcal vaccine

G79324  [2013]

21

Prevenar 13

Pfizer, France

Antipneumococcal vaccine

N27430 [ 2018]

22

Mencevax Acwy

GlaxoSmithKline, Italy

anti-Neisseria meningococcal group A, C, W135 and Y vaccine

N402A47B 12 [2004]

23

Meningitec

Pfizer, Italy

(group C 10) (adsorbed on Al-Phosphate)

H92709 [2015]

24

Meningitec

Pfizer-Italy

Anti-meningococcus (group C 10) vaccine (adsorbed on Al-Phosphate        )

H20500 [2014]

25

Meningitec

Pfizer-Italy

Anti-meningococcus vaccine sequestred by Procura della Repubblica

G76673 [2014]

26

Meningitec

Pfizer-Italy

Anti-meningococcus vaccine sequestred by Procura della Repubblica

H99459 [2015]

27

Meningitec

Pfizer-Italy

Anti-meningococcus vaccine sequestred by Procura della Repubblica

H52269 [2015]

28

Menjugate

Novartis Vaccines and Diagnostics

Anti-meningococcus group  C

YA0163AB [2010]

29

Menveo

Novartis Vaccines and Diagnostics

Antimeningococcus groups A, C, W135, Y

A15083 [2017]

30

Meningitec

Wyeth Pharmaceutical - France

Anti-meningococcus group C vaccine

E83920 [2011]

31

Inflexal V

Berna Biotech

Anti-flu vaccine  2008/2009

3001463-01 [2009]

32

Vaxigrip

Sanofi Pasteur MSD

Anti-flu vaccine  2008/2009

D9703-1 [2009]

33

Vaxigrip

Sanofi Pasteur

Anti-flu vaccine 2012/2013

J8401-1 [2013]

34

Vaxigrip

Sanofi Pasteur, Italy

Anti-flu vaccine, with inactivated and split virus

M7319-1 [2016]

35

Focetria

Novartis Vaccines and Diagnostics

Anti-pandemic flu H1N1 vaccine

0902401 [2010]

36

Agrippal

Novartis

Anti-flu vaccine 2012/2013

127002A [2013]

37

Agrippal

Novartis vaccines, Italy

Anti-flu vaccine with inactivated and split virus 2015/2016 -

152803 [2016]

38

Agrippal S1

Novartis Vaccines and Diagnostics

Anti-flu inactivated/superficial antigene v -  2014/2015

147302A [2015]

39

Fluarix

GlaxoSmithKline - GSK

Anti-flu vaccine  2013

AFLUA789AA [2014]

40

Fluad

Novartis Vaccines and Diagnostics

Anti-flu inactivated/superficial antigene vaccine -  2014/2015

142502 [2015]

41

Gardasil

Sanofi Pasteur MSD, Italy

Anti-HPV types 6,11,16,18 vaccine

NP01250 [2012]

42

Gardasil

Sanofi Pasteur MSD, Italy

Anti-HPV (types 6,11,16,18) vaccine

K023804 [2016]

43

Cervarix

GlaxoSmithKline Biological, Italy

Anti-HPV (type 16,18)

AHPVA238AX [2017]

44

Feligen CRP

Virbac S.A. - Carros - Italy

anti-panleucopenia, infectious rhinotracheitis and infections
by Calcivirus, veterinary Vaccine for cats

3R4R [2013]

Table 1 List of vaccines analyzed, according to their purpose

Some vaccines, in fact a minority, are meant to deal with a single bacterium or virus, while others are multi-valent. The list of vaccines we analyzed may contain repeated names, because we considered different batches and years of production of the same vaccine: the ones against influenza in particular.

The study was aimed at verifying a possible physical contamination. To do that, we performed a new kind of investigation based on observations under a Field Emission Gun Environmental Electron Scanning Microscope (FEG-ESEM, Quanta 200, FEI, The Netherlands) equipped with the X-ray microprobe of an Energy Dispersive Spectroscope (EDS, EDAX, Mahwah, NJ, USA) to detect the possible presence of inorganic, particulate contaminants and identify their chemical composition.

A drop of about 20microliter of vaccine is released from the syringe on a 25-mm-diameter cellulose filter (Millipore, USA), inside a flow cabinet. The filter is then deposited on an Aluminum stub covered with an adhesive carbon disc. The sample is immediately put inside a clean box in order to avoid any contamination and the box is re-opened only for the sample to be inserted inside the FEG-ESEM chamber. We selected that particular type of microscope as it allows to analyse watery and oily samples in low vacuum (from 10 to 130 Pa) at a high sensitivity.

When the water and saline the vaccine contains are evaporated, the biological/physical components emerge on the filter and it is then possible to observe them. This type of microscope (low-vacuum observations) prevents the possible sample contamination and the creation of artefacts. The observations are made with different sensors (SE: secondary-electron sensor and BSE: backscattered-electron sensor), and are performed at a pressure of 8.9 e-1 mbar, at energies ranging from 10 to 30kV to detect the particulate matter’s size, morphology and its elemental composition. The method identifies clearly inorganic bodies with a higher atomic density (looking whiter) than the biological substrate. So, organic entities are visible and easy to distinguish from inorganic ones. The method cannot distinguish between proteins and organic adjuvants (e.g. squalene, glutamate, proteins, etc.) or viruses, bacteria, bacteria’s DNA, endo-toxins and bacteria’s waste, but their comparatively low atomic density allows us to identify these entities as organic matter. In some vaccines, the organic matter contains white-looking debris named aggregates, while a high concentration or inorganic debris is called a cluster.

Single inorganic particles or organic-inorganic aggregates are identified, evaluated and counted. The counting procedure is repeated three times by three different operators, with an error lower than 10%. When a layer of salts (Sodium chloride or Aluminum) is detected, we record the situation but we do not do body count.

Results

The investigations verified the physical-chemical composition of the vaccines considered according to the inorganic component as declared by the Producer. In detail, we verified the presence of saline and Aluminum salts, but further presence of micro-, sub-micro- and nanosized, inorganic, foreign bodies (ranging from 100nm to about ten microns) was identified in all cases, whose presence was not declared in the leaflets delivered in the package of the product (Table 2).

N

Company

Name

Alluminum

Elements Identified

1

Allergopharma - Germany

Allergoid

yes

Al

2

Aventis Pasteur MSD Lyon - Francie    

Typhim Vi

no

BrKP, PbSi, FeCr, PbClSiTi

3

Baxter AG

Tetabulin

no

SiMg, Fe, SiTiAl, SBa, Zn

4

Berna Biotech

Vivotif Berna

no

FeAl, ZrAlHf, SrAl, BiAlCl

5

Berna Biotech

Inflexal V

no

CuSnPbZn, Fe, CaSiAl, SiAl, NaPZn, ZnP, AlSiTi

6

Chiron

Anatetall

Al(OH)3

FeAl, SZnBaAl

7

Chiron

Morupar

no

/

8

GlaxoSmithKline- Belgium

Mencevax ACWY    

no

FeCrNi, ZrAl, FeCrNiZrAlSi

9

GlaxoSmithKline

Infanrix

Al(OH)3

Al, AlTi, AlSi

10

GlaxoSmithKline Biologicals

Infanrix hexa

Al(OH)3

SBa, FeCu, SiAl, FeSi, CaMgSi, AlCaSi, Ti, Au, SCa, SiAlFeSnCuCrZn, CaAlSi

11

GlaxoSmithKline Biologicals

Infanrix hexa

Al(OH)3 ,AlPO4. 2H2O    

W, FeCrNi, Ti

12

GlaxoSmithKline

Typherix

no

Ti, TiW, AlSiTiWCr, SBa, W, SiAl, AlSiTi

13

GlaxoSmithKline

Priorix

no

WCa, WFeCu, SiAl, SiMg, PbFe, Ti, WNiFe

14

GlaxoSmithKline

Engerix-B

no

Al (precipitates)

15

GlaxoSmithKline

Varilrix

no

FeZn, FeSi, AlSiFe, SiAlTiFe, MgSi, Ti, Zr, Bi

16

GlaxoSmithKline

Fluarix

no

AlCu, Fe, AlBi, Si, SiZn, AlCuFe, SiMg, SBa, AlCuBi, FeCrNi, SPZn

17

GlaxoSmithKline Biologicals

Cervarix

Al(OH)3

AlSi,FeAl, SiMg,CaSiAl, CaZn, FeAlSi, FeCr, CuSnPb

18

Novartis Vaccines and Diagnostics

Anatetall

Al(OH)3

Al, FeCrNi, AlCr, AlFe, BaS, ZnAl

19

Novartis Vaccines and Diagnostics

Dif-Tet-All

Al(OH)3

Fe,SBa, SiSBa, AlZnCu, AlZnFeCr

20

Novartis Vaccines and Diagnostics

Menjugate kit

Al(OH)3

SiAl,Ti,FeZn, Fe, Sb, SiAlFeTi, W, Zr

21

Novartis Vaccines and Diagnostics

Focetria

no

Fe, FeCrNiCu, FeCrNi, SiFeCrNi, Cr, SiAlFe, AlSiTiFe, AlSi, SiMgFe, Si, FeZn

22

Novartis

Agrippal S1

no

Ca, Fe, SBa, SBaZn, Cr, Si, Pb, Bi, e FeSiAlCr, SiAlSBaFe, CaAlSi, Zn, CeFeTiNi, FeCrNi

23

Novartis Vaccines and Diagnostics

Agrippal S1

no

SiAlK, Si, SiMgFe, CaSiAl, SBaZn

24

Novartis vaccines

Agrippal

no

Cr, Ca, SiCaAl, ZrSi, SBa, CuZn, SCa

25

Novartis Vaccines and Diagnostics S

Fluad

no

CaSiAl, FeSiTi,SiMgAlFe, SBa

26

Novartis Vaccines and Diagnostics

Menveo

no

CaSiAl, SiAlFe, FeCrNi, Fe, Al, SBa

27

Pfizer

Prenevar 13

no

FeCr

28

Pfizer

Prevenar 13

no

W, CaAlSi, Al, CaSiAlFe, FeS, FeCr, FeCrNi, Fe, , CaP, FeTiMn, Ba, SiMgAlFe

29

Pfizer

Meningitec - ctrl

no

Cr, Si

30

Pfizer

Meningitec - ctrl

no

FeCrNi, W

31

Pfizer

Meningitec

no

CaSiAl, CaSi, SiAlFeTi, FeCrNi, W, Fe, Pb

32

Pfizer

Meningitec

no

Cr (precipitates), Ca, AlSi

33

Pfizer

Meningitec

no

W, SiCa, CaSi, Pb, FeCrNi, Cr

34

Wyeth Pharmaceutical - UK

Meningitec

no

SiAlFe, SiAlTi, SiMgFe, W, Fe, Zr, Pb, Ca, Zn, FeCrNi

35

Sanofi Pasteur MSD-France

Vaxigrip

no

Fe, FeCrNi, SiAlFe, AlSi, SiAlFeCr

36

Sanofi Pasteur MSD

Stamaril Pasteur

no

CaSiAl, AlSi, Fe, SiMgFe, SiMgAlFe, CrSiFeCr, CrSiCuFe

37

Sanofi Pasteur MSD

Gardasil

AlPO4. 2H2O

AlCuFe, PbBi, Pb, Bi, Fe

38

Sanifi Pasteur MSD

Gardasil

AlPO4. 2H2O

CaAlSi, AlSi, SiMgFe, Al,Fe, AlCuFe, FeSiAl, BiBaS, Ti, TiAlSi

39

Sanofi Pasteur

Vaxigrip

no

Ca, CrFe, FeCrNi, CaSZn, CaSiAlTiFe, Ag, Fe

40

Sanofi Pasteur

Vaxigrip

no

SiMgFe, CaSiAl, AlSiFe, AlSi,FeCr, FeZn, Fe

41

Sanofi Pasteur MSD

Repevax

AlPO4 .2H2O

Bi, Fe, AlSiFe, SiMg, SBa, Ca

42

Sanofi Pasteur MSD S

Repevax

AlPO4.2H2O

Ti, Br, AuCuZn, Ca, SiZn, SiAuAgCu, SiMgFe,FeCrNi.AlSiMgTiMnCrFe, SiFeCrNi, FeAl

43

Sanofi Pasteur MSD

M-M-R vaxPro

no

Si, SiFeCrNi, FeCrNi,FeNi, Fe, SCa, AlSiCa, CaAlSiFeV, SBa, Pt, PtAgBiFeCr

44

Virbac S.A. - Carros - France

Feligen CRP

no

Ca,SiAl

Table 2 List of the vaccines according to their manufacturers with the chemical composition of the debris identified in each sample. The elements most represented are reported

Play Video

Figure 1a shows a layer of crystals of Sodium chloride (NaCl) embedding salts of Aluminum phosphate (AlPO4) in a drop of Gardasil (anti-HPV vaccine by Merck) as the EDS spectrum (Figure 1b) shows. Saline is the fluid base to any vaccine preparation and Aluminum salts or Aluminum hydroxide Al(OH)3 are the adjuvants which are usually added.

Figure 1 Crystals of saline solution and Aluminum Phosphate and corresponding EDS spectra.

Looking at the area outside these precipitates but inside the liquid drop, we identified other things: single particles, clusters of particles and aggregates (organic-inorganic composites) that are due to an interaction of the inorganic particulate matter with the organic part of the vaccine.

Figure 2a-2f shows the different typology of entities identified in the vaccines (Repevax, Prevenar and Gardasil); single particles, cluster of micro- and nanoparticles (<100nm) and aggregates with their EDS spectra (Figure 2d-2f). The images (Figure 2a & 2d) show debris of Aluminum, Silicon, Magnesium and Titanium; of Iron, Chromium, Silicon and Calcium particles (Figure 2b & 2e) arranged in a cluster, and Aluminum -Copper debris (Figure 2c & 2f) in an aggregate.

Figure 2 Images of single particles, cluster of micro- and nanoparticles (<100nm) andaggregates with their EDS spectra. They are respectively composed of (a,b) Aluminum, Silicon, Magnesium, Titanium, Chromium, Manganese, Iron, (c,d) Iron, Silicon, Calcium Titanium, Chromium, (e,f) Aluminum, Copper. The arrows show the points where EDS spectra were taken.

As can be seen, the particles are surrounded and embedded in a biological substrate. In all the samples analyzed, we identified particles containing: Lead (Typhym, Cervarix, Agrippal S1, Meningitec, Gardasil) or stainless steel (Mencevax, Infarix Hexa, Cervarix. Anatetall, Focetria, Agrippal S1, Menveo, Prevenar 13, Meningitec, Vaxigrip, Stamaril Pasteur, Repevax and MMRvaxPro).

Figure 3a-3d show particles of Tungsten identified in drops of Prevenar and Infarix (Aluminum, Tungsten, Calcium chloride).

Figure 3 Images of Tungsten particles identified in drops of Prevenar and Infarix. They are composed respectively of Tungsten, Aluminum, Iron but in different concentrations. The arrows show the points where EDS spectra were taken.

Figure 4a-4d present singular debris found in Repevax (Silicon, Gold, Silver) and Gardasil (Zirconium).

Figure 4 Images show examples of nano biointeraction. The aggregate (a,b) identified in Gardasil contains nanoparticles of Chlorine, Silicon, Aluminum, Zirconium, while the debris found in Repevax contains Silicon, Gold, Silver (c,d). The arrows show the points where EDS spectra were taken.

Some metallic particles made of Tungsten or stainless steel were also identified. Other particles containing Zirconium, Hafnium, Strontium and Aluminum (Vivotif, Meningetec); Tungsten, Nickel, Iron (Priorix, Meningetec); Antimony (Menjugate kit); Chromium (Meningetec); Gold or Gold, Zinc (Infarix Hexa, Repevax), or Platinum, Silver, Bismuth, Iron, Chromium (MMRvaxPro) or Lead,Bismuth (Gardasil) or Cerium (Agrippal S1) were also found. The only Tungsten appears in 8/44 vaccines, while Chromium (alone or in alloy with Iron and Nickel) in 25/44. The investigations revealed that some particles are embedded in a biological substrate, probably proteins, endo-toxins and residues of bacteria. As soon as a particle comes in contact with proteic fluids, a nano-bio-interaction6 occurs and a "protein corona" is formed.7‒10 The nano-bio-interaction generates a bigger-sized compound that is not biodegradable and can induce adverse effects, since it is not recognized as self by the body.

Figure 5a-5f show examples of these nano-bio-interactions. Aggregates can be seen (stable composite entities) containing particles of Lead in Meningitec, (Figure 5a & 5b) of stainless steel (Iron, Chromium and Nickel, Figure 5c & 5d) and of Copper, Zinc and Lead in Cervarix (Figure 5e & 5f). Similar aggregates, though in different situations (patients suffering from leukemia or cryoglobulinemia), have already been described in literature.

Figure 5 Show particles surrounded by an organic compound. They are composed of Lead (a,b), Iron, Chromium, Nickel (stainless steel; c,d), Copper, Tin, Lead (e,f). The arrows show the points where EDS spectra were taken.

The link between these two entities generates an unfolding of the proteins that can induce an autoimmune effect once those proteins are injected into humans.

Figure 6a & 6b show one of the foreign bodies identified in Agrippal. The particle is composed of Cerium, Iron, Titanium and Nickel. (Figure 7a & 7b) present an area of Repevax where the morphology of red cells - we cannot tell whether they are human or animal- is clearly visible.

Figure 6 Show an organic aggregate containing a debris made of Cerium, Iron, Nickel, Titanium. The red arrow indicates the organic layer (less atomically dense) that covers the Cerium particle.

Figure 7 Image of an area in a Repevax drop where the morphology of red cells (red arrows) were identified. It is impossible to know whether they are human or animal origin. Among the debris of saline and Aluminum phosphate, there is the presence of debris (white arrows) composed of Aluminum, Bromine, Silicon, Potassium, Titanium.

Table 3 summarizes the number and morphology of the debris identified, in term of single particles, clusters of particles or aggregates (organic-inorganic compounds), while Figure 8 shows the graph obtained calculating the total number of particles (particles plus clusters plus aggregates) identified for 20microl of every vaccine.

Name

Total Debris n.

Size Range in mm

Cluster n.

Size Range in mm

Aggregate n.(Range of Particles)

Size Range mm

Allergoid

NaCl precipitates

/

/

/

/

/

Typhim Vi

394

0,1-2,5

3[9-350]

Feb-35

Tetabulin

519

0,1-15

3[100-180]

25-60

Vivotif Berna

4

1,5-15

Inflexal V

103

0,1-17

1

20

3[35-45]

25-Oct

Anatetall

2

3-Jan

Morupar

/

/

/

Mencevax ACWY

13

0,2-5

Infanrix

3

5-Jan

1

25

Infanrix hexa

1821

0,1-15

15[1820]

20-140

Infanrix hexa

162

0,3-7

12

60

2[7 debris]

3.5-44

Typherix

8

0,2-8

1

15

Priorix

641

0,05-30

1

10

3[600]

20-70

Engerix-B

precipitates

/

Varilrix

2723

0,1-4

36 [120-2000]

15-40

Fluarix

1317

0,1-40

3[83]

30-Jul

Cervarix

1569

0,2-3

2

10-May

4[1400]

30-Aug

Anatetall

47

0,05-40

Dif-Tet-All

111

0,2-3

Menjugate

73

0,1-5

Focetria

35

0,7-10

Agrippal S1

430

0,2-6

13

0.2-80

5[410]

20

Agrippal S1

1029

0,1-12

9[1025]

35-80

Agrippal

480

0,1-6

11[ 460]

Feb-80

Fluad

605

0,2-15

4

25-Dec

6[ 600]

70

Menveo

452

0,1-13

4[430 ]

30-110

Prenevar 13

precipitates + 5 debris

7-Jan

Prevenar 13

precipitates + 81 debris

0,2-50

3

May-40

1 [60]

25

Meningitec

3

20-Oct

Meningitec

24

Aug-60

Meningitec

673

0,1-20

1

7

9[624]

5-110

Meningitec

precipitates + 40

0,1-3,5

2[40]

25-70

Meningitec

177

0,2-10

3[165]

15-100

Meningitec

241

0,1-15

1

50

2[230]

50

Vaxigrip

86

0,1-7

2[50]

2-2,5

Stamaril Pasteur

152

0,1-7

2

7-May

3[145]

20-Apr

Gardasil

304

0,05-3

1[300]

15

Gardasil

454

0.1-30

2

20-Jul

9[445]

May-60

Vaxigrip

304

0,1-10

1

13

2[300]

35

Vaxigrip

674

0,3-25

2

12-Feb

10[660]

9-150

Repevax

137

0,1-20

2[130]

40-50

Repevax

214

0,1-10

6[150]

30-May

M-M-R vaxPro

93

0,1-15

2[50]

15-Oct

Feligen CRP

92

0,1-12

1

12

1 (40 debris)

25

Table 3 List of the debris’ number identified in each vaccine as single particle, clusters and aggregates.
Characterization is made by shape, size range and variability of the number of particles counted in each aggregate [in brackets]

Figure 8 Graph of the debris’ quantities identified in a 20 microl drop of every vaccine.

Similar aggregates were already described by other scientists who identified them in the blood e.g. in leukemic patients15 and in subjects affected by cryoglobulinemia.16

Not all the vaccines analyzed contain the same contamination, though the same vaccine belonging to different batches and, in some cases, coming from different countries can contain a similar contamination (e.g. the vaccines by Glaxo Infarix, Typherix and Priorix contain Tungsten. Tungsten was also identified in Menjugate kit by Novartis, and Prevenar, Meningitec by Pfizer and Meningitec by Wyeth).

Feligen, the only veterinary vaccine tested, proved to be the only sample free from inorganic contamination, while Allergoid generates a layer of inorganic salts so thick that it does not allow to detect other particulate contaminants.

Discussion

The quantity of foreign bodies detected and, in some cases, their unusual chemical compositions baffled us. The inorganic particles identified are neither biocompatible nor biodegradable, that means that they are biopersistent and can induce effects that can become evident either immediately close to injection time or after a certain time from administration. It is important to remember that particles (crystals and not molecules) are bodies foreign to the organism and they behave as such. More in particular, their toxicity is in some respects different from that of the chemical elements composing them, adding to that toxicity which, in any case, is still there, that typical of foreign bodies. For that reason, they induce an inflammatory reaction.

After being injected, those microparticles, nanoparticles and aggregates can stay around the injection site forming swellings and granulomas.17 But they can also be carried by the blood circulation, escaping any attempt to guess what will be their final destination. We believe that in many cases they get distributed throughout the body without causing any visible reaction, but it is also likely that, in some circumstances, they reach some organ, none excluded and including the microbiota, in a fair quantity. As happens with all foreign bodies, particularly that small, they induce an inflammatory reaction that is chronic because most of those particles cannot be degraded. Furthermore, the protein-corona effect (due to a nano-bio-interaction18 can produce organic/inorganic composite particles capable of stimulating the immune system in an undesirable way.19‒22 It is impossible not to add that particles the size often observed in vaccines can enter cell nuclei and interact with the DNA.23

In some cases, e.g. as occurs with Iron and some Iron alloys, they can corrode and the corrosion products exert a toxicity affecting the tissues.24‒26

The detection of presence of Aluminum and NaCl salts is obvious as they are substances used by the Producers and declared as components, but other materials are not supposed to be in the vaccine or in any other injectable drug, at that, and, in any case, Aluminum has already been linked with neurological diseases.27‒29

Given the contaminations we observed in all samples of human-use vaccines, adverse effects after the injection of those vaccines are possible and credible and have the character of randomness, since they depend on where the contaminants are carried by the blood circulation. It is only obvious that similar quantities of these foreign bodies can have a more serious impact on very small organisms like those of children. Their presence in the muscles, due an extravasation from the blood, could heavily impair the muscle functionality.30,31

We come across particles with chemical compositions, similar to those found in the vaccines we analyzed, when we study cases of environmental contamination caused by different pollution sources. In most circumstances, the combinations detected are very odd as they have no technical use, cannot be found in any material handbook and look like the result of the random formation occurring, for example, when waste is burnt. In any case, whatever their origin, they should not be present in any injectable medicament, let alone in vaccines, more in particular those meant for infants.

Other forms of so-far unknown contaminations have recently been observed and, in any case, vaccines contain components that could themselves be the cause of adverse effects. It is a well-known fact in toxicology that contaminants exert a mutual, synergic effect, and as the number of contaminants increases, the effects grow less and less predictable. The more so when some substances are unknown.

As a matter of fact, no exhaustive and reliable official data exist on the side-effects induced by vaccines. The episodic evidence reported by people allegedly damaged by vaccines is twofold: some say the damage occurred and became visible within a few hours from administration, and some maintain that it was a matter of some weeks. Though we have no indisputable evidence as to the reliability of those attestations, we can put forward a hypothesis to explain the different phenomena. In the former case, the pollutants contained in the drug have reached the brain and, depending on the anatomical site interested, have induced a reaction. If that is the case, the whole phenomenon is very rapid. In the latter circumstance, the pollutants reached the microbiota, thus interfering with the production of enzymes necessary to carry out neurological functions.32‒35 That possibility takes time, as it involves the production of chemical compounds in a sufficient quantity, and an elapse of some weeks between injection and clinical evidence is reasonable. Of course, ours is no more than a hypothesis open to discussion and in need of proof, hoping that a chance of further investigation is allowed.

Conclusion

The analyses carried out show that in all samples checked vaccines contain non biocompatible and bio-persistent foreign bodies which are not declared by the Producers, against which the body reacts in any case. This new investigation represents a new quality control that can be adopted to assess the safety of a vaccine. Our hypothesis is that this contamination is unintentional, since it is probably due to polluted components or procedures of industrial processes (e.g. filtrations) used to produce vaccines, not investigated and not detected by the Producers. If our hypothesis is actually the case, a close inspection of the working places and the full knowledge of the whole procedure of vaccine preparation would probably allow to eliminate the problem.

A further purification of the vaccines could improve their quality and could probably decrease the number and seriousness of the adverse incidental effects.

Acknowledgments

The Authors are indebted to Dr. Federico Capitani, Dr. Laura Valentini and Ms. Lavinia Nitu for their technical assistance. The opinions and conclusions are not necessarily those of the Institution.

Conflicts of interest

Author declares there are no conflicts of interest.

Funding

None.

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